TY - JOUR A1 - Nanadikar, Maithily S. A1 - Vergel Leon, Ana M. A1 - Borowik, Sergej A1 - Hillemann, Annette A1 - Zieseniss, Anke A1 - Belousov, Vsevolod V. A1 - Bogeski, Ivan A1 - Rehling, Peter A1 - Dudek, Jan A1 - Katschinski, Dörthe M. T1 - O2 affects mitochondrial functionality ex vivo JF - Redox Biology N2 - Mitochondria have originated in eukaryotic cells by endosymbiosis of a specialized prokaryote approximately 2 billion years ago. They are essential for normal cell function by providing energy through their role in oxidizing carbon substrates. Glutathione (GSH) is a major thiol-disulfide redox buffer of the cell including the mitochondrial matrix and intermembrane space. We have generated cardiomyocyte-specific Grx1-roGFP2 GSH redox potential (EGSH) biosensor mice in the past, in which the sensor is targeted to the mitochondrial matrix. Using this mouse model a distinct EGSH of the mitochondrial matrix (−278.9 ± 0.4 mV) in isolated cardiomyocytes is observed. When analyzing the EGSH in isolated mitochondria from the transgenic hearts, however, the EGSH in the mitochondrial matrix is significantly oxidized (−247.7 ± 8.7 mV). This is prevented by adding N-Ethylmaleimide during the mitochondria isolation procedure, which precludes disulfide bond formation. A similar reducing effect is observed by isolating mitochondria in hypoxic (0.1–3% O2) conditions that mimics mitochondrial pO2 levels in cellulo. The reduced EGSH is accompanied by lower ROS production, reduced complex III activity but increased ATP levels produced at baseline and after stimulation with succinate/ADP. Altogether, we demonstrate that oxygenation is an essential factor that needs to be considered when analyzing mitochondrial function ex vivo. KW - glutathione redox potential KW - hypoxia KW - mitochondrial matrix KW - Grx1-roGFP Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-232217 VL - 22 ER - TY - JOUR A1 - Kiser, Dominik P. A1 - Popp, Sandy A1 - Schmitt-Böhrer, Angelika G. A1 - Strekalova, Tatyana A1 - van den Hove, Daniel L. A1 - Lesch, Klaus-Peter A1 - Rivero, Olga T1 - Early-life stress impairs developmental programming in Cadherin 13 (CDH13)-deficient mice JF - Progress in Neuropsychopharmacology & Biological Psychiatry N2 - Objective Cadherin-13 (CDH13), a member of the calcium-dependent cell adhesion molecule family, has been linked to neurodevelopmental disorders, including autism spectrum (ASD) and attention-deficit/hyperactivity (ADHD) disorders, but also to depression. In the adult brain, CDH13 expression is restricted e.g. to the presynaptic compartment of inhibitory GABAergic synapses in the hippocampus and Cdh13 knockout mice show an increased inhibitory drive onto hippocampal CA1 pyramidal neurons, leading to a shift in excitatory/inhibitory balance. CDH13 is also moderating migration of serotonergic neurons in the dorsal raphe nucleus, establishing projections preferentially to the thalamus and cerebellum during brain development. Furthermore, CDH13 is upregulated by chronic stress as well as in depression, suggesting a role in early-life adaptation to stressful experience. Here, we therefore investigated the interaction between Cdh13 variation and neonatal maternal separation (MS) in mice. Methods Male and female wild-type (Cdh13+/+), heterozygous (Cdh13+/−) and homozygous (Cdh13−/−) knockout mice exposed to MS, or daily handling as control, were subjected to a battery of behavioural tests to assess motor activity, learning and memory as well as anxiety-like behaviour. A transcriptome analysis of the hippocampus was performed in an independent cohort of mice which was exposed to MS or handling, but remained naïve for behavioural testing. Results MS lead to increased anxiety-like behaviour in Cdh13−/− mice compared to the other two MS groups. Cdh13−/− mice showed a context-dependent effect on stress- and anxiety-related behaviour, impaired extinction learning following contextual fear conditioning and decreased impulsivity, as well as a mild decrease in errors in the Barnes maze and reduced risk-taking in the light-dark transition test after MS. We also show sex differences, with increased locomotor activity in female Cdh13−/− mice, but unaltered impulsivity and activity in male Cdh13−/− mice. Transcriptome analysis revealed several pathways associated with cell surface/adhesion molecules to be altered following Cdh13 deficiency, together with an influence on endoplasmic reticulum function. Conclusion MS resulted in increased stress resilience, increased exploration and an overall anxiolytic behavioural phenotype in male Cdh13+/+ and Cdh13+/− mice. Cdh13 deficiency, however, obliterated most of the effects caused by early-life stress, with Cdh13−/− mice exhibiting delayed habituation, no reduction of anxiety-like behaviour and decreased fear extinction. Our behavioural findings indicate a role of CDH13 in the programming of and adaptation to early-life stress. Finally, our transcriptomic data support the view of CDH13 as a neuroprotective factor as well as a mediator in cell-cell interactions, with an impact on synaptic plasticity. KW - Cadherin-13 (CDH13) KW - T-cadherin KW - neurodevelopment KW - autism KW - ADHD KW - depression KW - psychiatric disorders KW - early-life stress KW - mouse KW - RNA sequencing KW - endoplasmic reticulum stress KW - adhesion Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-325859 VL - 89 ER - TY - JOUR A1 - Faber, T. A1 - Hudec, M. A1 - Malinský, M. A1 - Meinzinger, P. A1 - Porod, W. A1 - Staub, F. T1 - A unified leptoquark model confronted with lepton non-universality in B-meson decays JF - Physics Letters B N2 - The anomalies in the B-meson sector, in particular R-K(*) and R-D(*), are often interpreted as hints for physics beyond the Standard Model. To this end, leptoquarks or a heavy Z' represent the most popular SM extensions which can explain the observations. However, adding these fields by hand is not very satisfactory as it does not address the big questions like a possible embedding into a unified gauge theory. On the other hand, light leptoquarks within a unified framework are challenging due to additional constraints such as lepton flavor violation. The existing accounts typically deal with this issue by providing estimates on the relevant couplings. In this letter we consider a complete model based on the SU(4)(C) circle times SU(2)(L) circle times U(1) R gauge symmetry, a subgroup of SO(10), featuring both scalar and vector leptoquarks. We demonstrate that this setup has, in principle, all the potential to accommodate R-K(*) and R-D(*) while respecting bounds from other sectors usually checked in this context. However, it turns out that K-L -> e(+/-)mu(-/+) severely constraints not only the vector but also the scalar leptoquarks and, consequently, also the room for any sizeable deviations of R-K(*) from 1. We briefly comment on the options for extending the model in order to conform this constraint. Moreover, we present a simple criterion for all-orders proton stability within this class of models. Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-227419 VL - 787 ER - TY - RPRT A1 - Geßner, Daniel T1 - Rethinking renewable energy policies for hydrogen – How the intercept of electricity and hydrogen markets can be addressed N2 - A lot of countries have recently published updated hydrogen strategies, often including more ambitious targets for hydrogen production. In parallel, accompanying ramp-up mechanisms are increasingly coming into focus with the first ones already being released. However, these proposals usually translate mechanisms from renewable energy (RE) policy without considering the specific uncertainties, spillovers, and externalities of integrating hydrogen electrolysis into electricity grids. This article details how different aspects of a policy can address the specific issues, namely funding, risk-mitigation, and the complex relation with electricity markets. It shows that, compared to RE policy, subsidies need to emphasize the input side more strongly as price risks and intermittency from electricity markets are more prominent than from hydrogen markets. Also, it proposes a targeted mechanism to capture the positive externality of mitigating excess electricity in the grid while keeping investment security high. Economic policy should consider such approaches before massively scaling support and avoid the design shortcomings experienced with early RE policy. T3 - Würzburg Economic Papers (W. E. P.) - 111 KW - Wasserstoff KW - Öffentliche Förderung KW - Contract for Difference KW - Elektrizitätsmarkt KW - Erneuerbare Energien KW - Hydrogen Policy KW - Renewable Energy Policy KW - Electricity Markets KW - Support Mechanisms KW - Contracts for Difference Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370973 ER - TY - JOUR A1 - Hauke, Jan A1 - Horvath, Judit A1 - Groß, Eva A1 - Gehrig, Andrea A1 - Honisch, Ellen A1 - Hackmann, Karl A1 - Schmidt, Gunnar A1 - Arnold, Norbert A1 - Faust, Ulrike A1 - Sutter, Christian A1 - Hentschel, Julia A1 - Wang-Gohrke, Shan A1 - Smogavec, Mateja A1 - Weber, Bernhard H. F. A1 - Weber-Lassalle, Nana A1 - Weber-Lassalle, Konstantin A1 - Borde, Julika A1 - Ernst, Corinna A1 - Altmüller, Janine A1 - Volk, Alexander E. A1 - Thiele, Holger A1 - Hübbel, Verena A1 - Nürnberg, Peter A1 - Keupp, Katharina A1 - Versmold, Beatrix A1 - Pohl, Esther A1 - Kubisch, Christian A1 - Grill, Sabine A1 - Paul, Victoria A1 - Herold, Natalie A1 - Lichey, Nadine A1 - Rhiem, Kerstin A1 - Ditsch, Nina A1 - Ruckert, Christian A1 - Wappenschmidt, Barbara A1 - Auber, Bernd A1 - Rump, Andreas A1 - Niederacher, Dieter A1 - Haaf, Thomas A1 - Ramser, Juliane A1 - Dworniczak, Bernd A1 - Engel, Christoph A1 - Meindl, Alfons A1 - Schmutzler, Rita K. A1 - Hahnen, Eric T1 - Gene panel testing of 5589 BRCA1/2-negative index patients with breast cancer in a routine diagnostic setting: results of the German Consortium for Hereditary Breast and Ovarian Cancer JF - Cancer Medicine N2 - The prevalence of germ line mutations in non-BRCA1/2 genes associated with hereditary breast cancer (BC) is low, and the role of some of these genes in BC predisposition and pathogenesis is conflicting. In this study, 5589 consecutive BC index patients negative for pathogenic BRCA1/2 mutations and 2189 female controls were screened for germ line mutations in eight cancer predisposition genes (ATM, CDH1, CHEK2, NBN, PALB2, RAD51C, RAD51D, and TP53). All patients met the inclusion criteria of the German Consortium for Hereditary Breast and Ovarian Cancer for germ line testing. The highest mutation prevalence was observed in the CHEK2 gene (2.5%), followed by ATM (1.5%) and PALB2 (1.2%). The mutation prevalence in each of the remaining genes was 0.3% or lower. Using Exome Aggregation Consortium control data, we confirm significant associations of heterozygous germ line mutations with BC for ATM (OR: 3.63, 95%CI: 2.67–4.94), CDH1 (OR: 17.04, 95%CI: 3.54–82), CHEK2 (OR: 2.93, 95%CI: 2.29–3.75), PALB2 (OR: 9.53, 95%CI: 6.25–14.51), and TP53 (OR: 7.30, 95%CI: 1.22–43.68). NBN germ line mutations were not significantly associated with BC risk (OR:1.39, 95%CI: 0.73–2.64). Due to their low mutation prevalence, the RAD51C and RAD51D genes require further investigation. Compared with control datasets, predicted damaging rare missense variants were significantly more prevalent in CHEK2 and TP53 in BC index patients. Compared with the overall sample, only TP53 mutation carriers show a significantly younger age at first BC diagnosis. We demonstrate a significant association of deleterious variants in the CHEK2, PALB2, and TP53 genes with bilateral BC. Both, ATM and CHEK2, were negatively associated with triple-negative breast cancer (TNBC) and estrogen receptor (ER)-negative tumor phenotypes. A particularly high CHEK2 mutation prevalence (5.2%) was observed in patients with human epidermal growth factor receptor 2 (HER2)-positive tumors. KW - breast cancer predisposition KW - hereditary breast cancer Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-227902 ER - TY - JOUR A1 - Lumma, Anna-Lena A1 - Valk, Sofie L. A1 - Böckler, Anne A1 - Vrtička, Pascal A1 - Singer, Tania T1 - Change in emotional self-concept following socio-cognitive training relates to structural plasticity of the prefrontal cortex JF - Brain and Behavior N2 - Introduction Self-referential processing is a key component of the emotional self-concept. Previous studies have shown that emotional self-referential processing is related to structure and function of cortical midline areas such as medial prefrontal cortex (mPFC), and that it can be altered on a behavioral level by specific mental training practices. However, it remains unknown how behavioral training-related change in emotional self-concept content relates to structural plasticity. Methods To address this issue, we examined the relationship between training-induced change in participant's emotional self-concept measured through emotional word use in the Twenty Statement Test and change in cortical thickness in the context of a large-scale longitudinal mental training study called the ReSource Project. Results Based on prior behavioral findings showing increased emotional word use particularly after socio-cognitive training targeting perspective-taking capacities, this study extended these results by revealing that individual differences in the degree to which participants changed their emotional self-concept after training was positively related to cortical thickness change in right mPFC extending to dorsolateral PFC (dlPFC). Furthermore, increased self-related negative emotional word use after training was positively associated with cortical thickness change in left pars orbitalis and bilateral dlPFC. Conclusions Our findings reveal training-related structural brain change in regions known to be involved in self-referential processing and cognitive control, and could indicate a relationship between restructuring of the emotional self-concept content as well as reappraisal of negative aspects and cortical thickness change. As such, our findings can guide the development of psychological interventions targeted to alter specific facets of the self-concept. KW - cortical thickness KW - emotional word use KW - meditation KW - mental training KW - neuroplasticity KW - self-concept content KW - self-descriptions Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-237395 VL - 8 ER - TY - JOUR A1 - Bäumer, Nils A1 - Kartha, Kalathil K. A1 - Kumar Allampally, Naveen A1 - Yagai, Shiki A1 - Albuquerque, Rodrigo Q. A1 - Fernández, Gustavo T1 - Exploiting Coordination Isomerism for Controlled Self-Assembly JF - Angewandte Chemie International Edition N2 - We exploited the inherent geometrical isomerism of a PtII complex as a new tool to control supramolecular assembly processes. UV irradiation and careful selection of solvent, temperature, and concentration leads to tunable coordination isomerism, which in turn allows fully reversible switching between two distinct aggregate species (1D fibers↔2D lamellae) with different photoresponsive behavior. Our findings not only broaden the scope of coordination isomerism, but also open up exciting possibilities for the development of novel stimuli-responsive nanomaterials. KW - coordination isomerism KW - photoresponsive behavior KW - self-assembly KW - supramolecular polymers KW - p-conjugated systems Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-221362 VL - 58 ER - TY - JOUR A1 - Sol, Jeroen A. H. P. A1 - Dehm, Volker A1 - Hecht, Reinhard A1 - Würthner, Frank A1 - Schenning, Albertus P. H. J. A1 - Debije, Michael G. T1 - Temperature-Responsive Luminescent Solar Concentrators: Tuning Energy Transfer in a Liquid Crystalline Matrix JF - Angewandte Chemie International Edition N2 - Temperature-responsive luminescent solar concentrators (LSCs) have been fabricated in which the Förster resonance energy transfer (FRET) between a donor–acceptor pair in a liquid crystalline solvent can be tuned. At room temperatures, the perylene bisimide (PBI) acceptor is aggregated and FRET is inactive; while after heating to a temperature above the isotropic phase of the liquid crystal solvent, the acceptor PBI completely dissolves and FRET is activated. This unusual temperature control over FRET was used to design a color-tunable LSC. The device has been shown to be highly stable towards consecutive heating and cooling cycles, making it an appealing device for harvesting otherwise unused solar energy. KW - energy transfer KW - fluorescence KW - liquid crystals KW - luminescent solar concentrators KW - perylene dyes Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-238778 VL - 57 ER - TY - JOUR A1 - Gole, Bappaditya A1 - Stepanenko, Vladimir A1 - Rager, Sabrina A1 - Grüne, Matthias A1 - Medina, Dana D. A1 - Bein, Thomas A1 - Würthner, Frank A1 - Beuerle, Florian T1 - Microtubular Self-Assembly of Covalent Organic Frameworks JF - Angewandte Chemie International Edition N2 - Despite significant progress in the synthesis of covalent organic frameworks (COFs), reports on the precise construction of template-free nano- and microstructures of such materials have been rare. In the quest for dye-containing porous materials, a novel conjugated framework DPP-TAPP-COF with an enhanced absorption capability up to λ=800 nm has been synthesized by utilizing reversible imine condensations between 5,10,15,20-tetrakis(4-aminophenyl)porphyrin (TAPP) and a diketopyrrolopyrrole (DPP) dialdehyde derivative. Surprisingly, the obtained COF exhibited spontaneous aggregation into hollow microtubular assemblies with outer and inner tube diameters of around 300 and 90 nm, respectively. A detailed mechanistic investigation revealed the time-dependent transformation of initial sheet-like agglomerates into the tubular microstructures. KW - covalent organic frameworks KW - diketopyrrolopyrroles KW - imines KW - microtubes KW - porphyrins Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-227373 VL - 57 ER - TY - JOUR A1 - Griemert, Eva-Verena A1 - Schwarzmaier, Susanne M. A1 - Hummel, Regina A1 - Gölz, Christina A1 - Yang, Dong A1 - Neuhaus, Winfried A1 - Burek, Malgorzata A1 - Förster, Carola Y. A1 - Petkovic, Ivan A1 - Trabold, Raimund A1 - Plesnila, Nikolaus A1 - Engelhard, Kristin A1 - Schäfer, Michael K. A1 - Thal, Serge C. T1 - Plasminogen activator inhibitor-1 augments damage by impairing fibrinolysis after traumatic brain injury JF - Annals of Neurology N2 - Objective Plasminogen activator inhibitor-1 (PAI-1) is the key endogenous inhibitor of fibrinolysis, and enhances clot formation after injury. In traumatic brain injury, dysregulation of fibrinolysis may lead to sustained microthrombosis and accelerated lesion expansion. In the present study, we hypothesized that PAI-1 mediates post-traumatic malfunction of coagulation, with inhibition or genetic depletion of PAI-1 attenuating clot formation and lesion expansion after brain trauma. Methods We evaluated PAI-1 as a possible new target in a mouse controlled cortical impact (CCI) model of traumatic brain injury. We performed the pharmacological inhibition of PAI-1 with PAI-039 and stimulation by tranexamic acid, and we confirmed our results in PAI-1–deficient animals. Results PAI-1 mRNA was time-dependently upregulated, with a 305-fold peak 12 hours after CCI, which effectively counteracted the 2- to 3-fold increase in cerebral tissue-type/urokinase plasminogen activator expression. PAI-039 reduced brain lesion volume by 26% at 24 hours and 43% at 5 days after insult. This treatment also attenuated neuronal apoptosis and improved neurofunctional outcome. Moreover, intravital microscopy demonstrated reduced post-traumatic thrombus formation in the pericontusional cortical microvasculature. In PAI-1–deficient mice, the therapeutic effect of PAI-039 was absent. These mice also displayed 13% reduced brain damage compared with wild type. In contrast, inhibition of fibrinolysis with tranexamic acid increased lesion volume by 25% compared with vehicle. Interpretation This study identifies impaired fibrinolysis as a critical process in post-traumatic secondary brain damage and suggests that PAI-1 may be a central endogenous inhibitor of the fibrinolytic pathway, promoting a procoagulatory state and clot formation in the cerebral microvasculature. Ann Neurol 2019;85:667–680 Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-228682 VL - 85 ER - TY - JOUR A1 - Charbonnier, Baptiste A1 - Baradaran, Aslan A1 - Sato, Daisuke A1 - Alghamdi, Osama A1 - Zhang, Zishuai A1 - Zhang, Yu-Ling A1 - Gbureck, Uwe A1 - Gilardino, Mirko A1 - Harvey, Edward A1 - Makhoul, Nicholas A1 - Barralet, Jake T1 - Material-Induced Venosome-Supported Bone Tubes JF - Advanced Science N2 - The development of alternatives to vascular bone grafts, the current clinical standard for the surgical repair of large segmental bone defects still today represents an unmet medical need. The subcutaneous formation of transplantable bone has been successfully achieved in scaffolds axially perfused by an arteriovenous loop (AVL) and seeded with bone marrow stromal cells or loaded with inductive proteins. Although demonstrating clinical potential, AVL-based approaches involve complex microsurgical techniques and thus are not in widespread use. In this study, 3D-printed microporous bioceramics, loaded with autologous total bone marrow obtained by needle aspiration, are placed around and next to an unoperated femoral vein for 8 weeks to assess the effect of a central flow-through vein on bone formation from marrow in a subcutaneous site. A greater volume of new bone tissue is observed in scaffolds perfused by a central vein compared with the nonperfused negative control. These analyses are confirmed and supplemented by calcified and decalcified histology. This is highly significant as it indicates that transplantable vascularized bone can be grown using dispensable vein and marrow tissue only. This is the first report illustrating the capacity of an intrinsic vascularization by a single vein to support ectopic bone formation from untreated marrow. KW - angiogenesis KW - axial vascularization KW - bioceramic KW - bioinorganic KW - material-host interactions KW - osteogenesis Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-222318 VL - 6 ER - TY - JOUR A1 - Kirsch, Anna Dalal A1 - Hassin-Baer, Sharon A1 - Matthies, Cordula A1 - Volkmann, Jens A1 - Steigerwald, Frank T1 - Anodic versus cathodic neurostimulation of the subthalamic nucleus: A randomized-controlled study of acute clinical effects JF - Parkinsonism and Related Disorders N2 - Introduction Stimulation settings of deep brain stimulation (DBS) have evolved empirically within a limited parameter space dictated by first generation devices. There is a need for controlled clinical studies, which evaluate efficacy and safety of established programming practice against novel programming options provided by modern neurostimulation devices. Methods Here, we tested a polarity reversal from conventional monopolar cathodic to anodic stimulation in an acute double-blind, randomized, cross-over study in patients with PD implanted with bilateral STN DBS. The primary outcome measure was the difference between efficacy and side-effect thresholds (current amplitude, mA) in a monopolar review and the severity of motor symptoms (as assessed by MDS-UPDRS III ratings) after 30 min of continuous stimulation in the medication off-state. Results Effect and side effect thresholds were significantly higher with anodic compared to cathodic stimulation (3.36 ± 1.58 mA vs. 1.99 ± 1.37 mA; 6.05 ± 1.52 mA vs. 4.15 ± 1.13 mA; both p < 0.0001). However, using a predefined amplitude of 0.5 mA below the respective adverse effect threshold, blinded MDS-UPDRS-III-ratings were significantly lower with anodic stimulation (anodic: median 17 [min: 12, max: 25]; cathodic: 23 [12, 37]; p < 0.005). Conclusion Effective anodic stimulation requires a higher charge injection into the tissue, but may provide a better reduction of off-period motor symptoms within the individual therapeutic window. Therefore, a programming change to anodic stimulation may be considered in patients suffering from residual off-period motor symptoms of PD despite reaching the adverse effect threshold of cathodic stimulation in the subthalamic nucleus. KW - deep brain stimulation KW - subthalamic nucleus KW - Parkinson's disease KW - anodic stimulation Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-325820 VL - 55 ER - TY - JOUR A1 - Counsell, John R. A1 - Karda, Rajvinder A1 - Diaz, Juan Antiano A1 - Carey, Louise A1 - Wiktorowicz, Tatiana A1 - Buckley, Suzanne M. K. A1 - Ameri, Shima A1 - Ng, Joanne A1 - Baruteau, Julien A1 - Almeida, Filipa A1 - de Silva, Rohan A1 - Simone, Roberto A1 - Lugarà, Eleonora A1 - Lignani, Gabriele A1 - Lindemann, Dirk A1 - Rethwilm, Axel A1 - Rahim, Ahad A. A1 - Waddington, Simon N. A1 - Howe, Steven J. T1 - Foamy Virus Vectors Transduce Visceral Organs and Hippocampal Structures following In Vivo Delivery to Neonatal Mice JF - Molecular Therapy: Nucleic Acids N2 - Viral vectors are rapidly being developed for a range of applications in research and gene therapy. Prototype foamy virus (PFV) vectors have been described for gene therapy, although their use has mainly been restricted to ex vivo stem cell modification. Here we report direct in vivo transgene delivery with PFV vectors carrying reporter gene constructs. In our investigations, systemic PFV vector delivery to neonatal mice gave transgene expression in the heart, xiphisternum, liver, pancreas, and gut, whereas intracranial administration produced brain expression until animals were euthanized 49 days post-transduction. Immunostaining and confocal microscopy analysis of injected brains showed that transgene expression was highly localized to hippocampal architecture despite vector delivery being administered to the lateral ventricle. This was compared with intracranial biodistribution of lentiviral vectors and adeno-associated virus vectors, which gave a broad, non-specific spread through the neonatal mouse brain without regional localization, even when administered at lower copy numbers. Our work demonstrates that PFV can be used for neonatal gene delivery with an intracranial expression profile that localizes to hippocampal neurons, potentially because of the mitotic status of the targeted cells, which could be of use for research applications and gene therapy of neurological disorders. KW - foamy virus KW - spumavirus KW - viral vector KW - gene therapy KW - vector tropism KW - bioimaging KW - hippocampus Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-223379 VL - 12 ER - TY - JOUR A1 - Argyrousi, Elentina K. A1 - de Nijs, Laurence A1 - Lagatta, Davi C. A1 - Schlütter, Anna A1 - Weidner, Magdalena T. A1 - Zöller, Johanna A1 - van Goethem, Nick P. A1 - Joca, Sâmia R. L. A1 - van den Hove, Daniel L. A. A1 - Prickaerts, Jos T1 - Effects of DNA methyltransferase inhibition on pattern separation performance in mice JF - Neurobiology of Learning and Memory N2 - Enhancement of synaptic plasticity through changes in neuronal gene expression is a prerequisite for improved cognitive performance. Moreover, several studies have shown that DNA methylation is able to affect the expression of (e.g. plasticity) genes that are important for several cognitive functions. In this study, the effect of the DNA methyltransferase (DNMT) inhibitor RG108 was assessed on object pattern separation (OPS) task in mice. In addition, its effect on the expression of target genes was monitored. Administration of RG108 before the test led to a short-lasting, dose-dependent increase in pattern separation memory that was not present anymore after 48 h. Furthermore, treatment with RG108 did not enhance long-term memory of the animals when tested after a 24 h inter-trial interval in the same task. At the transcriptomic level, acute treatment with RG108 was accompanied by increased expression of Bdnf1, while expression of Bdnf4, Bdnf9, Gria1 and Hdac2 was not altered within 1 h after treatment. Methylation analysis of 14 loci in the promoter region of Bdnf1 revealed a counterintuitive increase in the levels of DNA methylation at three CpG sites. Taken together, these results indicate that acute administration of RG108 has a short-lasting pro-cognitive effect on object pattern separation that could be explained by increased Bdnf1 expression. The observed increase in Bdnf1 methylation suggests a complex interplay between Bdnf methylation-demethylation that promotes Bdnf1 expression and associated cognitive performance. Considering that impaired pattern separation could constitute the underlying problem of a wide range of mental and cognitive disorders, pharmacological agents including DNA methylation inhibitors that improve pattern separation could be compelling targets for the treatment of these disorders. In that respect, future studies are needed in order to determine the effect of chronic administration of such agents. KW - object pattern separation KW - DNA methyltransferase inhibitors KW - BDNF KW - CpG islands KW - epigenetics KW - hippocampal plasticity Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-221226 VL - 159 ER - TY - JOUR A1 - Figel, Benedikt A1 - Brinkmann, Leonie A1 - Buff, Christine A1 - Heitmann, Carina Y. A1 - Hofmann, David A1 - Bruchmann, Maximilian A1 - Becker, Michael P. I. A1 - Herrmann, Martin J. A1 - Straube, Thomas T1 - Phasic amygdala and BNST activation during the anticipation of temporally unpredictable social observation in social anxiety disorder patients JF - NeuroImage: Clinical N2 - Anticipation of potentially threatening social situations is a key process in social anxiety disorder (SAD). In other anxiety disorders, recent research of neural correlates of anticipation of temporally unpredictable threat suggests a temporally dissociable involvement of amygdala and bed nucleus of the stria terminalis (BNST) with phasic amygdala responses and sustained BNST activation. However, the temporal profile of amygdala and BNST responses during temporal unpredictability of threat has not been investigated in patients suffering from SAD. We used functional magnetic resonance imaging (fMRI) to investigate neural activation in the central nucleus of the amygdala (CeA) and the BNST during anticipation of temporally unpredictable aversive (video camera observation) relative to neutral (no camera observation) events in SAD patients compared to healthy controls (HC). For the analysis of fMRI data, we applied two regressors (phasic/sustained) within the same model to detect temporally dissociable brain responses. The aversive condition induced increased anxiety in patients compared to HC. SAD patients compared to HC showed increased phasic activation in the CeA and the BNST for anticipation of aversive relative to neutral events. SAD patients as well as HC showed sustained activity alterations in the BNST for aversive relative to neutral anticipation. No differential activity during sustained threat anticipation in SAD patients compared to HC was found. Taken together, our study reveals both CeA and BNST involvement during threat anticipation in SAD patients. The present results point towards potentially SAD-specific threat processing marked by elevated phasic but not sustained CeA and BNST responses when compared to HC. KW - FMRI KW - threat anticipation KW - social anxiety disorder KW - bed nucleus of stria terminalis KW - amygdala Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-228071 VL - 22 ER - TY - JOUR A1 - Godel, Tim A1 - Pham, Mirko A1 - Kele, Henrich A1 - Kronlage, Moritz A1 - Schwarz, Daniel A1 - Brunée, Merle A1 - Heiland, Sabine A1 - Bendszus, Martin A1 - Bäumer, Philipp T1 - Diffusion tensor imaging in anterior interosseous nerve syndrome – functional MR Neurography on a fascicular level JF - NeuroImage: Clinical N2 - Purpose By applying diffusor tensor imaging (DTI) in patients with anterior interosseous nerve syndrome (AINS), this proof of principle study aims to quantify the extent of structural damage of a peripheral nerve at the anatomical level of individual fascicles. Methods In this institutional review board approved prospective study 13 patients with spontaneous AINS were examined at 3 Tesla including a transversal T2-weighted turbo-spin-echo and a spin-echo echo-planar-imaging pulse sequence of the upper arm level. Calculations of quantitative DTI parameters including fractional anisotropy (FA), mean diffusivity (MD), radial diffusivity (RD), and axial diffusivity (AD) for median nerve lesion and non-lesion fascicles as well as ulnar and radial nerve were obtained. DTI values were compared to each other and to a previously published dataset of 58 healthy controls using one-way Analysis of Variance with Bonferroni correction and p-values <.05 were considered significant. Receiver operating characteristic (ROC) curves were performed to assess diagnostic accuracy. Results FA of median nerve lesion fascicles was decreased compared to median nerve non-lesion fascicles, ulnar nerve and radial nerve while MD, RD, and AD was increased (p < .001 for all parameters). Compared to median nerve values of healthy controls, lesion fascicles showed a significant decrease in FA while MD, RD, and AD was increased (p < .001 for all parameters). FA of median nerve non-lesion fascicles showed a weak significant decrease compared to healthy controls (p < .01) while there was no difference in MD, RD, and AD. ROC analyses revealed an excellent diagnostic accuracy of FA, MD and RD in the discrimination of median nerve lesion and non-lesion fascicles in AINS patients as well as in the discrimination of lesion fascicles and normative median nerve values of healthy controls. Conclusion By applying this functional MR Neurography technique in patients with AINS, this proof of principle study demonstrates that diffusion tensor imaging is feasible to quantify structural nerve injury at the anatomical level of individual fascicles. KW - anterior interosseous nerve syndrome KW - diffusion tensor imaging KW - functional MR Neurography Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-233061 VL - 21 ER - TY - JOUR A1 - Gorlova, Anna A1 - Pavlov, Dmitrii A1 - Anthony, Daniel C. A1 - Ponomarev, Eugene D. A1 - Sambon, Margaux A1 - Proshin, Andrey A1 - Shafarevich, Igor A1 - Babaevskaya, Diana A1 - Lesch, Klaus-Peter A1 - Bettendorff, Lucien A1 - Strekalova, Tatyana T1 - Thiamine and benfotiamine counteract ultrasound-induced aggression, normalize AMPA receptor expression and plasticity markers, and reduce oxidative stress in mice JF - Neuropharmacology N2 - The negative societal impacts associated with the increasing prevalence of violence and aggression is increasing, and, with this rise, is the need to understand the molecular and cellular changes that underpin ultrasound-induced aggressive behavior. In mice, stress-induced aggression is known to alter AMPA receptor subunit expression, plasticity markers, and oxidative stress within the brain. Here, we induced aggression in BALB/c mice using chronic ultrasound exposure and examined the impact of the psychoactive anti-oxidant compounds thiamine (vitamin B1), and its derivative benfotiamine, on AMPA receptor subunit expression, established plasticity markers, and oxidative stress. The administration of thiamine or benfotiamine (200 mg/kg/day) in drinking water decreased aggressive behavior following 3-weeks of ultrasound exposure and benfotiamine, reduced floating behavior in the swim test. The vehicle-treated ultrasound-exposed mice exhibited increases in protein carbonyl and total glutathione, altered AMPA receptor subunits expression, and decreased expression of plasticity markers. These ultrasound-induced effects were ameliorated by thiamine and benfotiamine treatment; in particular both antioxidants were able to reverse ultrasound-induced changes in GluA1 and GluA2 subunit expression, and, within the prefrontal cortex, significantly reversed the changes in protein carbonyl and polysialylated form of neural cell adhesion molecule (PSA-NCAM) expression levels. Benfotiamine was usually more efficacious than thiamine. Thus, the thiamine compounds were able to counteract ultrasound-induced aggression, which was accompanied by the normalization of markers that have been showed to be associated with ultrasound-induced aggression. These commonly used, orally-active compounds may have considerable potential for use in the control of aggression within the community. This article is part of the Special Issue entitled ‘Current status of the neurobiology of aggression and impulsivity’. KW - aggression KW - emotional stress KW - brain oxidative stress KW - plasticity KW - thiamine KW - mice Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-227439 VL - 156 ER - TY - JOUR A1 - Verheijen, Bert M. A1 - Stevens, Jo A. A. A1 - Gentier, Romina J. G. A1 - van't Hekke, Christian D. A1 - van den Hove, Daniel L. A. A1 - Hermes, Denise J. H. P. A1 - Steinbusch, Harry W. M. A1 - Ruijter, Jan M. A1 - Grimm, Marcus O. W. A1 - Haupenthal, Viola J. A1 - Annaert, Wim A1 - Hartmann, Tobias A1 - van Leeuwen, Fred W. T1 - Paradoxical effects of mutant ubiquitin on Aβ plaque formation in an Alzheimer mouse model JF - Neurobiology of Aging N2 - Amyloid-β (Aβ) plaques are a prominent pathological hallmark of Alzheimer's disease (AD). They consist of aggregated Aβ peptides, which are generated through sequential proteolytic processing of the transmembrane protein amyloid precursor protein (APP) and several Aβ-associated factors. Efficient clearance of Aβ from the brain is thought to be important to prevent the development and progression of AD. The ubiquitin-proteasome system (UPS) is one of the major pathways for protein breakdown in cells and it has been suggested that impaired UPS-mediated removal of protein aggregates could play an important role in the pathogenesis of AD. To study the effects of an impaired UPS on Aβ pathology in vivo, transgenic APPSwe/PS1ΔE9 mice (APPPS1) were crossed with transgenic mice expressing mutant ubiquitin (UBB+1), a protein-based inhibitor of the UPS. Surprisingly, the APPPS1/UBB+1 crossbreed showed a remarkable decrease in Aβ plaque load during aging. Further analysis showed that UBB+1 expression transiently restored PS1-NTF expression and γ-secretase activity in APPPS1 mice. Concurrently, UBB+1 decreased levels of β-APP-CTF, which is a γ-secretase substrate. Although UBB+1 reduced Aβ pathology in APPPS1 mice, it did not improve the behavioral deficits in these animals. KW - mutant ubiquitin KW - ubiquitin-proteasome system KW - γ-secretase KW - amyloid-β KW - behavior KW - Alzheimer's disease Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-233185 VL - 72 ER - TY - JOUR A1 - Hedrich, Rainer A1 - Mueller, Thomas D. A1 - Becker, Dirk A1 - Marten, Irene T1 - Structure and Function of TPC1 Vacuole SV Channel Gains Shape JF - Molecular Plant N2 - Plants and animals in endosomes operate TPC1/SV-type cation channels. All plants harbor at least one TPC1 gene. Although the encoded SV channel was firstly discovered in the plant vacuole membrane two decades ago, its biological function has remained enigmatic. Recently, the structure of a plant TPC1/SV channel protein was determined. Insights into the 3D topology has now guided site-directed mutation approaches, enabling structure–function analyses of TPC1/SV channels to shed new light on earlier findings. Fou2 plants carrying a hyperactive mutant form of TPC1 develop wounding stress phenotypes. Recent studies with fou2 and mutants that lack functional TPC1 have revealed atypical features in local and long-distance stress signaling, providing new access to the previously mysterious biology of this vacuolar cation channel type in planta. KW - Ca2+ sensors KW - TPC1/SV channel KW - vacuole membrane voltage KW - voltage sensor Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-228046 VL - 11 ER - TY - JOUR A1 - Mühlemann, Markus A1 - Zdzieblo, Daniela A1 - Friedrich, Alexandra A1 - Berger, Constantin A1 - Otto, Christoph A1 - Walles, Heike A1 - Koepsell, Hermann A1 - Metzger, Marco T1 - Altered pancreatic islet morphology and function in SGLT1 knockout mice on a glucose-deficient, fat-enriched diet JF - Molecular Metabolism N2 - Objectives Glycemic control by medical treatment represents one therapeutic strategy for diabetic patients. The Na+-d-glucose cotransporter 1 (SGLT1) is currently of high interest in this context. SGLT1 is known to mediate glucose absorption and incretin secretion in the small intestine. Recently, inhibition of SGLT1 function was shown to improve postprandial hyperglycemia. In view of the lately demonstrated SGLT1 expression in pancreatic islets, we investigated if loss of SGLT1 affects islet morphology and function. Methods Effects associated with the loss of SGLT1 on pancreatic islet (cyto) morphology and function were investigated by analyzing islets of a SGLT1 knockout mouse model, that were fed a glucose-deficient, fat-enriched diet (SGLT1−/−-GDFE) to circumvent the glucose-galactose malabsorption syndrome. To distinguish diet- and Sglt1−/−-dependent effects, wildtype mice on either standard chow (WT-SC) or the glucose-free, fat-enriched diet (WT-GDFE) were used as controls. Feeding a glucose-deficient, fat-enriched diet further required the analysis of intestinal SGLT1 expression and function under diet-conditions. Results Consistent with literature, our data provide evidence that small intestinal SGLT1 mRNA expression and function is regulated by nutrition. In contrast, pancreatic SGLT1 mRNA levels were not affected by the applied diet, suggesting different regulatory mechanisms for SGLT1 in diverse tissues. Morphological changes such as increased islet sizes and cell numbers associated with changes in proliferation and apoptosis and alterations of the β- and α-cell population are specifically observed for pancreatic islets of SGLT1−/−-GDFE mice. Glucose stimulation revealed no insulin response in SGLT1−/−-GDFE mice while WT-GDFE mice displayed only a minor increase of blood insulin. Irregular glucagon responses were observed for both, SGLT1−/−-GDFE and WT-GDFE mice. Further, both animal groups showed a sustained release of GLP-1 compared to WT-SC controls. Conclusion Loss or impairment of SGLT1 results in abnormal pancreatic islet (cyto)morphology and disturbed islet function regarding the insulin or glucagon release capacity from β- or α-cells, respectively. Consequently, our findings propose a new, additional role for SGLT1 maintaining proper islet structure and function. KW - glucose transporter SGLT1 KW - pancreatic islet cytomorphology KW - pancreatic islet function KW - β-cell KW - α-cell Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-224230 VL - 13 ER - TY - JOUR A1 - Baluapuri, Apoorva A1 - Hofstetter, Julia A1 - Dudvarski Stankovic, Nevenka A1 - Endres, Theresa A1 - Bhandare, Pranjali A1 - Vos, Seychelle Monique A1 - Adhikari, Bikash A1 - Schwarz, Jessica Denise A1 - Narain, Ashwin A1 - Vogt, Markus A1 - Wang, Shuang-Yan A1 - Düster, Robert A1 - Jung, Lisa Anna A1 - Vanselow, Jens Thorsten A1 - Wiegering, Armin A1 - Geyer, Matthias A1 - Maric, Hans Michael A1 - Gallant, Peter A1 - Walz, Susanne A1 - Schlosser, Andreas A1 - Cramer, Patrick A1 - Eilers, Martin A1 - Wolf, Elmar T1 - MYC Recruits SPT5 to RNA Polymerase II to Promote Processive Transcription Elongation JF - Molecular Cell N2 - The MYC oncoprotein binds to promoter-proximal regions of virtually all transcribed genes and enhances RNA polymerase II (Pol II) function, but its precise mode of action is poorly understood. Using mass spectrometry of both MYC and Pol II complexes, we show here that MYC controls the assembly of Pol II with a small set of transcription elongation factors that includes SPT5, a subunit of the elongation factor DSIF. MYC directly binds SPT5, recruits SPT5 to promoters, and enables the CDK7-dependent transfer of SPT5 onto Pol II. Consistent with known functions of SPT5, MYC is required for fast and processive transcription elongation. Intriguingly, the high levels of MYC that are expressed in tumors sequester SPT5 into non-functional complexes, thereby decreasing the expression of growth-suppressive genes. Altogether, these results argue that MYC controls the productive assembly of processive Pol II elongation complexes and provide insight into how oncogenic levels of MYC permit uncontrolled cellular growth. KW - MYC KW - SPT5 KW - SUPT5H KW - SPT6 KW - RNA polymerase II KW - transcription KW - elongation rate KW - processivity KW - directionality KW - tumorigenesis Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-221438 VL - 74 ER - TY - JOUR A1 - Bugai, Andrii A1 - Quaresma, Alexandre J. C. A1 - Friedel, Caroline C. A1 - Lenasi, Tina A1 - Düster, Robert A1 - Sibley, Christopher R. A1 - Fujinaga, Koh A1 - Kukanja, Petra A1 - Hennig, Thomas A1 - Blasius, Melanie A1 - Geyer, Matthias A1 - Ule, Jernej A1 - Dölken, Lars A1 - Barborič, Matjaž T1 - P-TEFb Activation by RBM7 Shapes a Pro-survival Transcriptional Response to Genotoxic Stress JF - Molecular Cell N2 - DNA damage response (DDR) involves dramatic transcriptional alterations, the mechanisms of which remain ill defined. Here, we show that following genotoxic stress, the RNA-binding motif protein 7 (RBM7) stimulates RNA polymerase II (Pol II) transcription and promotes cell viability by activating the positive transcription elongation factor b (P-TEFb) via its release from the inhibitory 7SK small nuclear ribonucleoprotein (7SK snRNP). This is mediated by activation of p38MAPK, which triggers enhanced binding of RBM7 with core subunits of 7SK snRNP. In turn, P-TEFb relocates to chromatin to induce transcription of short units, including key DDR genes and multiple classes of non-coding RNAs. Critically, interfering with the axis of RBM7 and P-TEFb provokes cellular hypersensitivity to DNA-damage-inducing agents due to activation of apoptosis. Our work uncovers the importance of stress-dependent stimulation of Pol II pause release, which enables a pro-survival transcriptional response that is crucial for cell fate upon genotoxic insult. KW - Pol II elongation KW - Pol II pause release KW - P-TEFb KW - CDK9 KW - 7SK snRNP KW - RBM7 KW - genotoxic stress KW - DNA damage response KW - p38 MAP kinase KW - apoptosis Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-221726 VL - 74 ER - TY - JOUR A1 - Žutić, Igor A1 - Matos-Abiague, Alex A1 - Scharf, Benedikt A1 - Dery, Hanan A1 - Belashchenko, Kirill T1 - Proximitized materials JF - Materials Today N2 - Advances in scaling down heterostructures and having an improved interface quality together with atomically thin two-dimensional materials suggest a novel approach to systematically design materials. A given material can be transformed through proximity effects whereby it acquires properties of its neighbors, for example, becoming superconducting, magnetic, topologically nontrivial, or with an enhanced spin–orbit coupling. Such proximity effects not only complement the conventional methods of designing materials by doping or functionalization but also can overcome their various limitations. In proximitized materials, it is possible to realize properties that are not present in any constituent region of the considered heterostructure. While the focus is on magnetic and spin–orbit proximity effects with their applications in spintronics, the outlined principles also provide a broader framework for employing other proximity effects to tailor materials and realize novel phenomena. Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-233972 VL - 22 ER - TY - JOUR A1 - McColl, Erin A1 - Groll, Jürgen A1 - Jungst, Tomasz A1 - Dalton, Paul D. T1 - Design and fabrication of melt electrowritten tubes using intuitive software JF - Materials and Design N2 - This study approaches the accurate continuous direct-writing onto a cylindrical collector from a mathematical perspective, taking into account the winding angle, cylinder diameter and length required for the final 3D printed tube. Using an additive manufacturing process termed melt electrowriting (MEW), porous tubes intended for tissue engineering applications are fabricated from medical-grade poly(ε-caprolactone) (PCL), validating the mathematically-derived method. For the fabricated tubes in this study, the pore size, winding angle and printed length can all be planned in advance and manufactured as designed. The physical dimensions of the tubes matched theoretical predictions and mechanical testing performed demonstrated that variations in the tubular morphology have a direct impact on their strength. MEWTubes, the web-based application developed and described here, is a particularly useful tool for planning the complex continuous direct writing path required for MEW onto a rotating, cylindrical build surface. KW - additive manufacturing KW - 3D printing KW - electrohydrodynamic printing KW - biomaterials KW - polycaprolactone Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-223891 VL - 155 ER - TY - JOUR A1 - Fazzini, Federica A1 - Lamina, Claudia A1 - Fendt, Liane A1 - Schultheiss, Ulla T. A1 - Kotsis, Fruzsina A1 - Hicks, Andrew A. A1 - Meiselbach, Heike A1 - Weissensteiner, Hansi A1 - Forer, Lukas A1 - Krane, Vera A1 - Eckardt, Kai-Uwe A1 - Köttgen, Anna A1 - Kronenberg, Florian T1 - Mitochondrial DNA copy number is associated with mortality and infections in a large cohort of patients with chronic kidney disease JF - Kidney International N2 - Damage of mitochondrial DNA (mtDNA) with reduction in copy number has been proposed as a biomarker for mitochondrial dysfunction and oxidative stress. Chronic kidney disease (CKD) is associated with increased mortality and risk of cardiovascular disease, but the underlying mechanisms remain incompletely understood. Here we investigated the prognostic role of mtDNA copy number for cause-specific mortality in 4812 patients from the German Chronic Kidney Disease study, an ongoing prospective observational national cohort study of patients with CKD stage G3 and A1-3 or G1-2 with overt proteinuria (A3) at enrollment. MtDNA was quantified in whole blood using a plasmid-normalized PCR-based assay. At baseline, 1235 patients had prevalent cardiovascular disease. These patients had a significantly lower mtDNA copy number than patients without cardiovascular disease (fully-adjusted model: odds ratio 1.03, 95% confidence interval [CI] 1.01-1.05 per 10 mtDNA copies decrease). After four years of follow-up, we observed a significant inverse association between mtDNA copy number and all-cause mortality, adjusted for kidney function and cardiovascular disease risk factors (hazard ratio 1.37, 95% CI 1.09-1.73 for quartile 1 compared to quartiles 2-4). When grouped by causes of death, estimates pointed in the same direction for all causes but in a fully-adjusted model decreased copy numbers were significantly lower only in infection-related death (hazard ratio 1.82, 95% CI 1.08-3.08). A similar association was observed for hospitalizations due to infections in 644 patients (hazard ratio 1.19, 95% CI 1.00-1.42 in the fully-adjusted model). Thus, our data support a role of mitochondrial dysfunction in increased cardiovascular disease and mortality risks as well as susceptibility to infections in patients with CKD. KW - chronic kidney disease KW - infections KW - mitochondrial DNA copy number KW - mortality Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-227662 VL - 96 ER - TY - THES A1 - Fuhl, Lucas T1 - Photolumineszenzmikroskopie und -spektroskopie endohedraler Farbstoffe in Bornitridnanoröhren T1 - Photoluminescence microscopy and spectroscopy of endohedral dyes in boron nitride nanotubes N2 - Im Rahmen der vorliegenden Dissertation wurde untersucht, wie die Einkapselung organischer Farbstoffmoleküle in Bornitridnanoröhren (BNNTs) die photophysikalischen Eigenschaften der Fluorophore beeinflusst. Als Farbstoffe wurden hierbei alpha-Quaterthiophen (4T), alpha-Sexithiophen (6T), alpha-Octithiophen (8T) sowie Nilrot (NR) ausgewählt. Die eingesetzten BNNTs besitzen einen nominellen Durchmesser von \(5 \pm 2\)nm. Für die Charakterisierung der reinen Farbstoffe und der hybriden Systeme aus Farbstoff und Nanoröhre kam ein Laboraufbau zum Einsatz, der neben Absorptions- und Photolumineszenz (PL)-Spektroskopie auch PL-Mikroskopie ermöglicht. Zusätzlich lässt sich damit auch eine zeitaufgelöste Untersuchung der PL (engl. time correlated single photon counting, TCSPC) im Ensemble und an einzelnen, separierten Nano-Objekten (mit Farbstoff gefüllte BNNTs) umsetzen. In Kapitel 5 wurden zunächst die freien Farbstoffe in Lösung charakterisiert. Es hat sich gezeigt, dass sowohl 4T als auch NR im verwendeten Lösemittel Dimethylformamid (DMF) löslich sind, wohingegen 6T und 8T hier eine geringere Löslichkeit zeigen. Die unterschiedlichen Verläufe der konzentrationsabhängigen PL-Spektren für 4T und 6T in DMF lassen sich vermutlich auf diesen Löslichkeitsunterschied zurückführen. Zudem wurden Extinktionskoeffizienten für 4T und NR mittels konzentrationsabhängiger Absorptionsspektren bestimmt und es zeigte sich eine gute Übereinstimmung mit der Literatur. Für 6T und 8T war eine Bestimmung aufgrund der geringen Löslichkeit nicht möglich, weshalb auf Literaturwerte zurückgegriffen wurde oder diese extrapoliert wurden (8T). In Kapitel 6 erfolgte die detaillierte Charakterisierung der mit Oligothiophenen gefüllten BNNTs. Die Befüllung wurde dabei im Wesentlichen nach einem von C. Allard publizierten Verfahren durchgeführt und auf die zusätzlichen Fluorophore 4T, 8T und NR übertragen. Für Messungen mittels UV-Vis-Spektroskopie in Lösung bzw. Dispersion hat sich beim Farbstoff 6T gezeigt, dass sich das Absorptionsmaximum von 407nm (freies 6T) hin zu 506nm (6T@BNNT) verschiebt. Ursache hierfür ist vermutlich die Bildung von J-Aggregaten im Inneren der Röhren. Die entsprechenden PL-Spektren von freiem 6T und dem Hybridsystem zeigen dabei keine signifikanten Unterschiede. Für konzentrationsabhängige PL-Spektren von 6T@BNNT ergibt sich (anders als bei freiem 6T in DMF) keine Änderung des Verlaufs der Kurven, was als ein Indiz für eine erfolgreiche Einkapselung gedeutet werden kann. Durch Kombination von Rasterkraft- und PL-Mikroskopie konnten die Außendurchmesser von einzelnen 6T@BNNT Objekten ermittelt und in direkten Zusammenhang mit deren photophysikalischen Eigenschaften gebracht werden. Bei einer Analyse der Polarisation des Emissionslichtes von 6T@BNNT in Abhängigkeit des Außendurchmessers ließ sich jedoch keine klare Korrelation zwischen Struktur und Emissionscharakteristiken erkennen. Diese Beobachtung lässt sich vermutlich dadurch erklären, dass mit Hilfe der Rasterkraftmikroskopie lediglich der Außendurchmesser der (teils mehrwandigen) BNNTs bestimmt werden kann. Die entscheidende Größe an dieser Stelle ist allerdings der innere Durchmesser der BNNTs, welcher die Ausrichtung und damit auch die Polarisation der Farbstoffmoleküle beeinflusst. Ein Vergleich des mittleren maximalen Polarisationsgrades der jeweiligen Hybridsysteme hat gezeigt, dass 4T@BNNT den geringsten und 6T@BNNT mit den höchsten Wert aufweist. Dies bestätigt die Annahme, dass mit zunehmender Moleküllänge die Polarisation, aufgrund des höheren Templat-Effektes der Röhre, zunimmt. 8T@BNNT liegt zwischen den beiden anderen Werten, was dieser Annahme widerspricht. Der mittlere Verkippungswinkel der eingekapselten Farbstoffmoleküle gegenüber der Röhrenachse liegt für 4T@BNNT bei etwa 16° und ist damit etwas größer als derjenige von 6T@BNNT. Somit zeigt sich auch hier, dass kürzere Moleküle mehr sterische Freiheitsgerade im Innern der Röhren besitzen. Für 8T@BNNT liegt der Winkel bei ca. 28° und widerspricht abermals der Annahme. TCSPC-Messungen an freien Oligothiophen-Farbstoffen sowie an den hybriden Systemen zeigten, dass die Fluoreszenzlebensdauer \(\tau\) für 4T und 6T (jeweils in DMF) infolge der Einkapselung deutlich zunimmt wenn die Hybridsysteme ebenfalls in DMF dispergiert sind. Die ermittelten Werte für \(\tau\) der separierten Nanoobjekte lagen für 4T@BNNT und 6T@BNNT unterhalb der entsprechenden in DMF. Für 8T bzw. 8T@BNNT ergab sich eine deutlich kürzerer Lebensdauer der separierten Nanoobjekte im Vergleich zum freien Farbstoff in kolloidaler Suspension. Ein erster Ansatz, um den zugrundeliegende Mechanismus aufzuklären, bestand darin, die TCSPC-Spektren (für 6T in DMF und 6T@BNNT in DMF) hinsichtlich der einzelnen Zerfallskanäle zu analysieren. Die erhaltenen Ergebnisse deuteten darauf hin, dass bei freiem 6T in DMF andere Zerfallskanäle dominieren als beim Hybridsystem 6T@BNNT (in DMF). Eine Korrelation der Fluorezenslebensdauer von 6T@BNNT vom äußeren Durchmesser der Nanoröhren zeigte keinen eindeutigen Zusammenhang. Die Charakterisierung von Nilrot bzw. NR@BNNT (analog zu den Oligothiophenen) erfolgte in Kapitel 4. Auch hier zeigte sich eine Verschiebung des PL-Spektrums des Fluorophores durch die Einkapselung in die BNNTs. Allerdings ist das PL-Spektrum des Hybridsystems (NR@BNNT) um etwa 20nm hypsochrom verschoben. Nilrot ist in der Literatur zudem als Nanosonde zur Ermittlung der Permittivität des Lösemittels bzw. der Umgebung bekannt. Dies erlaubte eine Abschätzung der relativen Permittivät im Inneren der BNNTs. Der ermittelte Wert von ca. 4 für ein isoliertes NR@BNNT Objekt deutet auf eine relativ unpolare Umgebung im Röhreninneren hin. Zum Vergleich dazu, liegt der Wert von freiem NR in DMF bei 47, was die relativ hohe Polarität von DMF bestätigt. Der ermittelte Wert für die mittlere maximale Polarisation lag leicht über dem der hybriden Systeme aus Oligothiophenen und Nanoröhren. Für die Auslenkung der NR-Moleküle gegenüber der Röhrenachse ergab sich ein Winkel von etwa 16°, was im Bereich der Werte von 4T@BNNT und 6T@BNNT liegt. Die Messung der zeitaufgelösten Fluoreszenz von freiem und eingekapseltem Nilrot hat ergeben, dass auch in diesem Fall eine Verkürzung der Lebensdauer (von 4091 ps auf 812 ps) erfolgte. Eine solche Verkürzung der Lebensdauer von Chromophoren wird in der Literatur unter anderem mit der Bildung von J-Aggregaten in Zusammenhang gebracht. N2 - This dissertation investigated how the encapsulation of organic dye molecules in boron nitride nanotubes (BNNTs) influences the photophysical properties of the fluorophores. The dyes chosen were alpha-quaterthiophene (4T), alpha-sexithiophene (6T), alpha-octithiophene (8T) and Nile red (NR). The BNNTs used have a nominal diameter of \(5 \pm 2\)nm. To characterize the pure dyes and the hybrid systems consisting of dye and nanotube, a laboratory setup was used that enables PL microscopy in addition to absorption and photoluminescence (PL) spectroscopy. In addition, a time-resolved study of PL (time correlated single photon counting, TCSPC) can be implemented in the ensemble and on individual, separated nano-objects (BNNTs filled with dye). In Chapter 5, the free dyes in solution were first characterized. It has been shown that both 4T and NR are soluble in the solvent used, dimethylformamide (DMF), whereas 6T and 8T show lower solubility. The different profiles of the concentration-dependent PL spectra for 4T and 6T in DMF can probably be attributed to this difference in solubility. In addition, extinction coefficients for 4T and NR were determined using concentration-dependent absorption spectra and there was good agreement with the literature. For 6T and 8T, a determination was not possible due to the low solubility, which is why literature values ​​were used or extrapolated (8T). Chapter 6 detailed the characterization of the BNNTs filled with oligothiophenes. The filling was essentially carried out according to a method published by C. Allard and transferred to the additional fluorophores 4T, 8T and NR. For measurements using UV-Vis spectroscopy in solution or dispersion, it has been shown that the absorption maximum for the dye 6T shifts from 407nm (free 6T) to 506nm (6T@BNNT). The reason for this is probably the formation of J-aggregates inside the tubes. The corresponding PL spectra of free 6T and the hybrid system show no significant differences. For concentration-dependent PL spectra of 6T@BNNT (unlike free 6T in DMF), there is no change in the shape of the curves, which can be interpreted as an indication of successful encapsulation. By combining atomic force and PL microscopy, the outer diameters of individual 6T@BNNT objects could be determined and directly related to their photophysical properties. However, when analyzing the polarization of the emission light from 6T@BNNT depending on the outer diameter, no clear correlation between structure and emission characteristics could be seen. This observation can probably be explained by the fact that only the outer diameter of the (some multi-walled) BNNTs can be determined using atomic force microscopy. The crucial size at this point, however, is the inner diameter of the BNNTs, which influences the alignment and thus also the polarization of the dye molecules. A comparison of the average maximum degree of polarization of the respective hybrid systems showed that 4T@BNNT has the lowest value and 6T@BNNT has the highest value. This confirms the assumption that as the molecule length increases, the polarization increases due to the higher template effect of the tube. 8T@BNNT lies between the other two values, which contradicts this assumption. The average tilt angle of the encapsulated dye molecules relative to the tube axis is about 16° for 4T@BNNT and is therefore slightly larger than that of 6T@BNNT. This also shows that shorter molecules have more steric freedom inside the tubes. For 8T@BNNT the angle is approximately 28° and again contradicts the assumption. TCSPC measurements on free oligothiophene dyes and on the hybrid systems showed that the fluorescence lifetime \(\tau\) for 4T and 6T (each in DMF) increases significantly as a result of encapsulation when the hybrid systems are also dispersed in DMF. The determined values ​​for \(\tau\) of the separated nanoobjects for 4T@BNNT and 6T@BNNT were below the corresponding ones in DMF. For 8T or 8T@BNNT, the lifespan of the separated nanoobjects was significantly shorter compared to the free dye in colloidal suspension. A first approach to elucidate the underlying mechanism was to analyze the TCSPC spectra (for 6T in DMF and 6T@BNNT in DMF) with respect to the individual decay channels. The results obtained indicated that different decay channels dominate for free 6T in DMF than for the hybrid system 6T@BNNT (in DMF). Correlating the fluorescence lifetime of 6T@BNNT with the outer diameter of the nanotubes showed no clear relationship. The characterization of Nile red or NR@BNNT (analogous to the oligothiophenes) took place in Chapter 4. Here, too, there was a shift in the PL spectrum of the fluorophore due to the encapsulation in the BNNTs. However, the PL spectrum of the hybrid system (NR@BNNT) is hypsochromically shifted by about 20 nm. Nile red is also known in the literature as a nanoprobe for determining the permittivity of the solvent or the environment. This allowed an estimation of the relative permittivity inside the BNNTs. The determined value of approx. 4 for an isolated NR@BNNT object indicates a relatively non-polar environment inside the tube. For comparison, the value of free NR in DMF is 47, confirming the relatively high polarity of DMF. The value determined for the average maximum polarization was slightly higher than that of the hybrid systems made of oligothiophenes and nanotubes. The deflection of the NR molecules relative to the tube axis resulted in an angle of approximately 16°, which is in the range of the values ​​for 4T@BNNT and 6T@BNNT. The measurement of the time-resolved fluorescence of free and encapsulated Nile Red showed that in this case too there was a shortening of the lifespan (from 4091 ps to 812 ps). In the literature, such a shortening of the lifespan of chromophores is associated, among other things, with the formation of J-aggregates. KW - Fluoreszenzmikroskopie KW - Spektroskopie KW - Oligothiophene KW - Nanoröhre KW - Nanomaterialien KW - Endohedrale Farbstoffe KW - Nanomaterials KW - Endohedral dyes Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-371150 ER - TY - THES A1 - Adolf, Jonas Michael T1 - Die Zusammenarbeit zwischen der stationären beziehungsweise teilstationären psychotherapeutischen Behandlung und niedergelassenen Psychotherapeut:innen T1 - The Collaboration between inpatient and semi-inpatient psychotherapeutic treatment and outpatient psychotherapists N2 - Das Ziel der vorliegenden Arbeit war es die aktuelle Versorgungskontinuität in der psychotherapeutischen Versorgung hinsichtlich der Zusammenarbeit des (teil-)stationären und des ambulanten Sektors aus Sicht der niedergelassenen Psychotherapeut:innen zu untersuchen, diese in den wissenschaftlichen Kontext einzuordnen und – falls möglich – erste Möglichkeiten zur Verbesserung der derzeitigen Versorgungskontinuität aufzuzeigen. In Zusammenarbeit mit dem Arbeitsbereich für Medizinische Psychologie und Psychotherapie im Zentrum für psychische Gesundheit des Universitätsklinikums Würzburg wurde hierzu ein Fragebogen entwickelt und acht ausgewählten psychotherapeutischen Fachgesellschaften beziehungsweise Psychotherapeutenkammern mit der Bitte um Weiterleitung an deren Mitglieder zugesandt. In der vorliegenden Studie wurden – neben einer Globalbeurteilung – im Speziellen die Teil-aspekte des Austauschs, der entsprechenden Rahmenbedingungen und die Bereitstellung des poststationären ambulanten Psychotherapieplatzes betrachtet. Die Studienergebnisse bilden den derzeitigen Status Quo der psychotherapeutischen Versorgungslage aus Sicht der niedergelassenen Psychotherapeut:innen ab und weisen im Zuge dessen auf einige Defizite in den untersuchten Teilaspekten hin. Die aufgestellten Nebenfragestellungen zeigen gleichsam aber auch Ansatzunkte für Lösungen auf. Aufgrund der besonderen Relevanz der aufgezeigten Ergebnisse, gilt es – zur Ermöglichung einer adäquaten kontinuierlichen psychotherapeutischen Versorgung – eine weitergehende Betrach-tung der aufgezeigten Defizite vorzunehmen. Für ein umfassendes Bild sind zudem kongruente Folgearbeiten mit dem Augenmerk auf der Sichtweise der (teil-)stationären Behandlungseinrichtungen und der Patient:innen notwendig. Insbesondere vor dem Hintergrund der limitierten Möglichkeiten der vorliegenden Arbeit gilt es große repräsentative und nationale Studien anzustreben. Hierzu wäre die Etablierung zentral verwalteter Register zur Bündelung der bisherigen und zukünftigen Forschungsarbeiten im Bereich der Psychotherapie wünschenswert. Vor allem vor dem Hintergrund zahlreicher Modellprojekte erscheint dies sinnvoll und könnte einen wichtigen Beitrag zur Optimierung der derzeitigen psychotherapeutischen Forschungs- und Versorgungslage beitragen. N2 - The aim of the study was to identify the current continuity of care regarding psychotherapeutic care and the collaboration of the (semi-)inpatient and outpatient field from point of view of the outpatient psychotherapists. Furthermore, the study wants to integrate the findings in the recent scientific context and wants to reveal improvements regarding the continuity of care in the field of psychotherapy. An explorative survey was created in collaboration with the working group of medical psychology and psychotherapy at the centre for mental health of the university hospital of Würzburg. Eight selected psychotherapeutic organisations (psychotherapy chambers and societies) were invited to conduct the survey to their members. Apart from a general assessment the study took a closer look at the framework conditions, the field of exchange and the care of outpatient psychotherapy to patients after (semi-)inpatient care. The study results describe the current situation of the psychotherapy care in Germany from the point of view of the outpatient psychotherapists and demonstrate on the one hand deficits regarding the analysed aspects and – as part of the side questions – on the other hand possible approaches for improvements. To facilitate a better continuity of psychotherapeutic care, it is important to take a closer look at the demonstrated deficits reported by the study. Moreover further studies are necessary treating the point of view of (semi-)inpatient psychotherapists as well as to conduct large national-wide representative studies, especially against the backdrop of the limited possibilities of the present study. For this purpose, it is helpful to establish a central-managed register to collect all studies in the field of psychotherapy. That could contribute to improve the current situation of research and care in the field of psychotherapy, in particular against the backdrop of the numerous pilot projects. KW - Psychotherapie KW - Medizinische Versorgung KW - Versorgungskontinuität KW - Sektoren KW - Versorgung KW - Psychiatrie Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-371098 ER - TY - THES A1 - Schuhmair, Leah Sophia T1 - Etablierung eines in-situ-Immunfluoreszenzfärbeverfahrens zur dreidimensionalen Darstellung und Quantifizierung der Immunzellinfiltration in experimentellen Tumoren T1 - Establishment of an in-situ immunofluorescence staining method for three-dimensional imaging and quantification of immune cell infiltration in experimental tumours N2 - Brustkrebs ist die häufigste diagnostizierte Krebserkrankung weltweit. Trotz der vielfältigen Behandlungsmöglichkeiten endet die Diagnose Brustkrebs in vielen Fällen noch immer tödlich. Aus diesem Grund ist die Entwicklung neuer Therapieansätze wichtig. Ein Therapieansatz, der in den letzten zehn Jahren immer mehr an Bedeutung gewonnen hat, ist die Immuntherapie. Allerdings konnte sie bei Brustkrebs noch keine großen Erfolge erzielen. Ursache hierfür ist die geringe Immunzellinfiltration in Brusttumoren. Um Brustkrebs für Immuntherapie empfänglicher zu machen, müssten Immuntherapeutika in Kombination mit Medikamenten angewendet werden, die die Immunzellinfiltration steigern. Um die Wirksamkeit solcher Medikamente in präklinischen Studien zu testen, braucht es eine Methode, mit der man die T-Zellverteilung innerhalb des Tumors darstellen kann. Für umfassendes Verständnis ist dreidimensionale Darstellung der Zellen im Tumor notwendig, da es einen großen Unterschied macht, ob sich die T-Zellen im Tumorstroma oder in unmittelbarer Nähe zu den Tumorzellen befinden. Die starke Fibrotisierung der Extrazellulären Matrix, die typisch für Brusttumoren ist, erschwert nicht nur die Immunzellinfiltration, sondern auch die Diffusion der fluoreszierenden Antikörper ins Gewebe. Im Zuge dieser Arbeit wurde eine Methode entwickelt, um im dreidimensionalen CD4 und CD8-positive T-Zellen in Brusttumoren darzustellen. Dies gelang mittels Immunfluoreszenzfärbung und anschließender dreidimensionaler Aufnahme mithilfe optischer Sektionierung am Lichtblattmikroskop. Erreicht wurde dies durch deutliche Erhöhung der Inkubationszeiten, aggressive Permeabilisierung des Gewebes, Testen unterschiedlicher Antikörper bzw. Antikörperkombinationen und Entfärbung sowie Klärung des Tumorgewebes. Darüber hinaus konnten erste Schritte in der nachträglichen Bearbeitung der Aufnahmen inklusive Rekonstruktion der Zellen gemacht werden. Für die Anwendung des Verfahrens in Studien zur Medikamentenwirksamkeit ist noch weitere Optimierung notwendig. N2 - Breast cancer is the most frequently diagnosed cancer worldwide. Despite the wide range of treatment options available, the diagnosis of breast cancer is still fatal in many cases. For this reason, the development of new therapeutic approaches is important. One therapeutic approach that has become increasingly important in the last ten years is immunotherapy. However has not yet been very successful in breast cancer. The reason for this is the low level of immune cell infiltration in breast tumours. To make breast cancer more receptive to immunotherapy, immunotherapeutics could be used in combination with drugs that increase immune cell infiltration. In order to test the efficacy of such drugs in preclinical studies, a method is needed that can be used to visualise the T cell distribution within the tumour. For a comprehensive understanding, three-dimensional visualisation of the cells in the tumour is necessary, as it makes a big difference whether the T cells are located in the tumour stroma or in close proximity to the tumour cells. The strong fibrotisation of the extracellular matrix, which is typical of breast tumours, not only makes T cell infiltration, but also the diffusion of the fluorescent antibodies into the tissue difficult. In the course of this work, a method was developed to visualise CD4 and CD8-positive T cells in breast tumours in three dimensions. This was achieved by significantly increasing incubation times, aggressive permeabilisation of the tissue, testing different antibodies and antibody combinations and decolourisation as well as clarification of the tumour tissue. In addition, the first steps were taken in the subsequent processing of the images, including reconstruction of the cells. However further optimisation is still required before the method can be used in drug efficacy studies. KW - Immunfluoreszenz KW - Brustkrebs KW - Dreidimensionales Bild KW - T-Lymphozyt KW - Immuntherapie KW - 3D imaging KW - Tumormikroumgebung KW - immun escape mechanism Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370945 ER - TY - THES A1 - Wanner, Maren T1 - Längsschnittanalyse von Stimmparametern bei gesunden Säuglingen im zweiten Lebenshalbjahr T1 - Systematic longitudinal analysis: Development of melodic structure in the second half of the first year of life N2 - In der vorliegenden Arbeit wurde die Melodiestrukturentwicklung im zweiten Lebenshalbjahr, exemplarisch an zehn gesunden Säuglingen mit deutscher Umgebungssprache, untersucht. Zusammen mit den zuvor erhobenen und vorliegenden Ergebnissen der ersten sechs Lebensmonate (Kottmann, 2023) war erstmalig eine systematische Längsschnittanalyse über das gesamte erste Lebensjahr möglich. Mithilfe des Lautanalyseprogramms CDAP wurden für die vorliegende Arbeit 4686 frühkindliche Lautaufahmen bezüglich ihres Melodiekonturverlaufs sowie ihrer auditiv und visuell wahrnehmbaren Feinstrukturmerkmale detailliert analysiert und ausgewertet. Der Datensatz spiegelt repräsentativ das typische Lautrepertoire von Säuglingen im zweiten Lebenshalbjahr mit den hier untersuchten Komfort-Vokalisationstypen wider: Übergangslaute, marginale und kanonische Babbellaute. In Übereinstimmung mit dem von Wermke und Mende postulierten MD-Modell, das eine vokalisationstyp-übergreifende Komplexitätszunahme frühkindlicher Lautäußerungen beschreibt, konnten erstmals die regelhaften Entwicklungsverläufe im zweiten Lebenshalbjahr gezeigt und ausführlich benannt werden. Dabei scheint die Zunahme der Komplexität vor allem im Zusammenhang mit artikulatorischen Reifeprozessen zu stehen. In der Melodie selbst fiel diesbezüglich vor allem der Einbau von Segmentierungen auf. Diese innermelodischen Unterbrechungen können wiederum als Vorläufer linguistischer Strukturen, wie beispielsweise Silben, angesehen werden. Der Übergang von einfachen zu fortgeschritteneren Vokalisationen, bis hin zu den ersten Wörtern, ist fließend. Zukünftig wäre für weitere empirische Untersuchungen interessant, inwiefern sich der Grundfrequenzverlauf zunehmend zur suprasegmentalen Intonationskurve entwickelt, was sich bereits in den durchgeführten Analysen angedeutet hat. Die kontinuierlich wachsende Kontrolle des Säuglings über den Vokaltrakt mit zunehmend gezielter Reproduktion erlernter Lautstrukturen wird durch die Ergebnisse der vorliegenden Arbeit belegt. Sie liefert einen wichtigen Beitrag zum Verständnis der Sprachentwicklung von Säuglingen und ermöglicht durch die Erkenntnisse der physiologisch ablaufenden Prozesse eine vorsprachliche Diagnostik, eine frühzeitige Intervention und Förderung der Sprache. Vor allem der Beginn des Babbelns scheint hierbei eine wichtige Evaluationsgröße zu sein. N2 - The present study investigated the development of melodic structure in the second half of their first year of life in ten healthy native German infants. Together with previously collected and published results of the first six months of life (Kottmann, 2023), a systematic longitudinal analysis of the entire first year of life was possible for the first time. Using the sound analysis programme CDAP, 4686 sound recordings from early childhood were analyzed and evaluated in detail with regard to their melodic contours as well as their auditorily and visually perceived fine structure features. The data set is representative of the typical sound repertoire of infants in the second half of their first year of life with the types of comfort vocalizations studied here: transitional, marginal and canonical baby sounds. Consistent with the MD model postulated by Wermke and Mende, which describes an increase in complexity of early infant vocalizations across vocalization types, the regular developmental trajectories in the second half of their first year of life could be shown and named in detail for the first time. The increase in complexity seems to be mainly related to articulatory maturation processes. In the melody itself, the integration of segmentations was particularly noticeable. These intra-melodic breaks can be seen as precursors of linguistic structures such as syllables. The transition from simple to more advanced vocalizations up to the first words is a smooth one. It would be interesting for future empirical studies to determine the extent to which the baseline frequency curve increasingly develops into the suprasegmental intonation curve that has already been suggested in the analyses conducted. The continuously increasing control of the vocal tract by infants with an increasingly specific reproduction of learned phonetic structures is supported by the results of the present study. The study makes an important contribution to the understanding of infant language development and, by providing insights into the physiological processes involved, enables pre-linguistic diagnostics, early intervention and language promotion. In particular, the onset of babbling appears to be an important assessment variable in this context. KW - Sprachentwicklung KW - vorsprachliche Entwicklung KW - MD-Modell Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370962 ER - TY - THES A1 - Liu, Yang T1 - Predictions for Composite Higgs Models Using Gauge/Gravity Duality T1 - Vorhersagen für zusammengesetzte Higgs-Modelle unter Verwendung der Eich-/Gravitationsdualität N2 - This thesis is dedicated to construct a non-abelian holographic dynamical minimal composite Higgs model. We first build a non-abelian bottom-up AdS/YM model that can explain the QCD meson spectrum well. The model is made non-abelian by considering non-abelian DBI action in the top-down model. We then change the dual theory from the QCD to the minimal composite Higgs model U (4)/Sp(4). By adding a second explicit U (4) → Sp(4) breaking through the NJL interaction at the boundary, we managed to construct a composite Higgs phase and a technicolor phase in this model. The transition between the two phases is also realized, which is controlled by the NJL coupling. This thesis is based on the works [1, 2]. N2 - Diese Arbeit konstruiert ein nicht-abelsches holographisches dynamisches minimales Composite-Higgs-Modell. Wir erstellen zunächst ein nicht-abelsches Bottom-up-AdS/YM-Modell, das das QCD-Mesonenspektrum gut erklären kann. Das Modell ist nicht-abelsch, da die nicht-abelsche DBI-Wirkung im Top-Down-Modell berücksichtigt wird. Anschließend ändern wir die duale Theorie von der QCD auf das minimale Composite-Higgs-Modell U (4)/Sp(4). Durch das Hinzufügen einer zweiten expliziten Brechung U (4) → Sp(4), das die NJL-Wechselwirkung an der Grenze durchbricht, konstruierten wir in diesem Modell eine Composite-Higgs-Phase und eine Technicolor-Phase. Auch der Übergang zwischen den beiden Phasen wird realisiert, welcher durch die NJL-Kopplung gesteuert wird. Diese Arbeit basiert auf den Arbeiten [1, 2]. KW - Composite Higgs KW - Gauge/gravity duality KW - holographic model KW - Higgs-Modell Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370833 ER - TY - THES A1 - Müller, Nicole T1 - Modellierung klonaler Evolution beim Multiplen Myelom T1 - Modeling Clonal Evolution in Multiple Myeloma N2 - In dieser Arbeit wurde ein modulares Zelllinienmodell zur Visualisierung klonaler Evolutionsmechanismen etabliert. Hierfür wurden unterschiedlich fluoreszierende Proteine (LSSmKate2, EGFP, mTagBFP2) durch Anwendung eines Sleeping Beauty basierten Vektorsystems in unterschiedliche Sublinien der Myelom Zelllinie L363 eingebracht. Diese vier Sublinien beinhalten jeweils eine von drei aus primären Patientenproben gewonnenen Mutationen in IKZF1 (A152T, E170D, R439H) oder den IKZF1 WT. Die Anwendung von immunmodulatorischen Medikamenten (IMiDs) führt zu einer Ubiquitinierung des Transkriptionsfaktors IKZF1 durch die E3-Ubiquitin-Protein-Ligase (CRBN-CUL4). Durch Mutationen in IKZF1 kommt es zu Störungen in diesem Prozess und damit zu einer Überexpression von IKZF1. Dies wirkt sich wachstumsfördert auf die Myelomzellen aus. Die Auswirkungen der einzelnen Mutationen in IKZF1 ist aufgrund dessen ein klinisch relevantes Forschungsthema. In dieser Arbeit wurden jeweils zwei Sublinien mit Zellen des IKZF1 WT und Zellen mit einer IKZF1 Mutation mit jeweils unterschiedlich fluoreszierenden Proteinen markiert. Diese wurden gemeinsam unter Behandlung mit verschiedenen Konzentrationen von Lenalidomid inkubiert. Somit konnte das Selektionsverhalten mittels Durchflusszytometrie-Auswertungen visualisiert werden. Es konnte gezeigt werden, dass die IKZF1 Mutation A152T einen deutlichen Selektionsvorteil für die Myelomzellen darstellt. Bei den IKZF1 Mutationen E170D und R439H konnte kein Selektionsvorteil gegenüber dem IKZF1 WT beobachtet werden. N2 - In this work, a modular cell line model was established to visualize clonal evolutionary mechanisms. Different fluorescent proteins (LSSmKate2, EGFP, mTagBFP2) were introduced into various sublines of the myeloma cell line L363 using a Sleeping Beauty-based vector system. These four sublines each contain one of three mutations in IKZF1 (A152T, E170D, R439H) derived from primary patient samples or the IKZF1 wild type (WT). The application of immunomodulatory drugs (IMiDs) leads to the ubiquitination of the transcription factor IKZF1 by the E3 ubiquitin-protein ligase (CRBN-CUL4). Mutations in IKZF1 disrupt this process, resulting in the overexpression of IKZF1, which promotes the growth of myeloma cells. The effects of individual mutations in IKZF1 are therefore a clinically relevant research topic. In this study, two sublines each with IKZF1 WT cells and cells with an IKZF1 mutation were labeled with different fluorescent proteins. These were incubated together under treatment with various concentrations of lenalidomide. Thus, the selection behavior could be visualized using flow cytometry analyses. It was shown that the IKZF1 mutation A152T provides a clear selective advantage for the myeloma cells. No selective advantage was observed for the IKZF1 E170D and R439H mutations compared to IKZF1 WT. KW - Lenalidomid KW - Plasmozytom KW - IKZF1 KW - klonale Evolution KW - Vektormodell KW - Multiples Myelom Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370818 ER - TY - THES A1 - Rode, Stefan T1 - Automated resummation of electroweak Sudakov logarithms in diboson production T1 - Automatisierte Resummierung elektroschwacher Sudakov-Logarithmen in Vektorboson-Paarproduktion N2 - The present thesis is concerned with the automated computation of integrated and differential cross sections of diboson production in proton–proton and electron–positron collisions at very high energies, including a resummation of electroweak Sudakov logarithms to all orders in the fine-structure constant using soft–collinear effective theory. The search for new physics at future colliders such as the FCC–hh or the CLIC requires precise predictions for scattering cross sections from the theoretical high-energy physics com- munity. Electroweak Sudakov logarithms, which currently limit the accuracy of predictions in the high-energy tails of differential distributions for LHC-like energies, are known to destroy the convergence behaviour of the fixed-order perturbative series, once sufficiently high energies are considered. To resum these large corrections, soft–collinear effective theory has been applied to simple processes, which permits analytic calculations. Within this work, we present an automated computation within a Monte Carlo integration framework, thus facilitating the computation of fully differential cross section to complicated processes. This requires the use of the Catani– Seymour subtraction algorithm to treat the occurring infrared divergences. The machinery is applied to all diboson processes with intermediate weak gauge bosons, including the photon- induced W+ W− -production channel. To this end we carefully study the validity of the necessary assumptions such as the double- pole approximation and estimate the order of magnitude of neglected effects. Especially the non-doubly-resonant contributions turn out to be sizeable in several interesting phase-space regions. For lepton collisions at 3 TeV we obtain the integrated cross sections of W-pair and Z-pair production to be shifted by more than 20% with respect to the Born value, owing to the resum- mation of the leading-logarithmic corrections These effects are partly cancelled by subleading effects. For proton–proton collisions at √ s = 100 TeV we observe sizeable resummation effects in the high-energy tails, while the integrated cross sections are dominated by interactions, for which soft–collinear effective theory is not applicable. N2 - Das Thema ist der vorliegenen Arbeit ist die automatisierte Berechnung differenzieller und integrierter Wirkungsquerschnitte der Paarerzeugung schwerer Eichbosonen bei sehr hohen Streuenergien mit Resummierung der auftretenden elektroschwachen Sudakov-Logarithmen zu allen Ordnungen in der Feinstrukturkonstanten mittels Soft-Collinear Effective Theory. Die Suche nach Physik jenseits des Standardmodells an zukunftigen Teilchenbeschleunigern wie dem FCC oder dem CLIC erfordert hochpräzise Voraussagen fur Streuquerschnitte seitens der theoretischen Physik. Es ist seit langem bekannt, dass elektroschwache Sudakov-Logarithmen, die bereits gegenwärtig die Genauigkeit der Voraussagen in den Hochenergieschwänzen von Verteilungen limitieren, die Konvergenz der konventionellen Störungsreihen vollkommen zunichte machen, wenn hinreichend hohe Energien erreicht werden. Mittels Soft-Collinear Effective Theory wurden diese Logarithmen bereits in der Vergangenheit in einfachen Prozessen, die eine analytische Behandlung erlauben, resummiert. Im Rahmen dieser Arbeit wurden diese Methoden in ein Monte-Carlo-Integrationsprogramm implementiert, um somit vollständig differenzielle Vorhersagen präsentieren zu können. Dies erfordert die Behandlung von Infrarotdivergenzen mit Hilfe des Catani-Seymour-Algorithmus. Mit diesen Werkzeugen wurden resummierte Streuquerschnitte fur verschiedene Vektorboson-Paarproduktionsprozesse berechnet, u.a. fur den Photon-Photon-induzierten Produktionskanal zur W-Boson-Paarproduktion. Auf dem Weg dorthin sind verschiedene vereinfachende Annahmen notwendig, deren Gultigkeit im Rahmen dieser Arbeit ebenfalls getestet wurde, so z.B. die Qualität der Doppelpolnäherung. Des weiteren wurden Größenordnungen vernachlässigter Effekte abgeschätzt. Dabei haben sich vor allem nicht doppelt resonante Beiträge in bestimmten Phasenraumregionen als beträchtlich herausgestellt. Der Resummationseffekt der fuhrend logarithmischen Korrekturen verschiebt die integrierten Paarproduktionsstreuquerschnitte um mehr als 20% bezogen auf den Bornstreuquerschnitt im Falle von Leptonkollisionen bei einer Schwerpunktsenergie von 3 TeV. Diese Effekte werden allerdings teilweise von nicht-führenden Beiträgen kompensiert. Fur Proton-Proton-Kollisionen bei √ s = 100 TeV finden wir deutliche Resummationseffekte in allen Hochenergieschwänzen, während die integrierten Wirkungsquerschnitte von Phasenraumregionen dominiert werden, in denen Soft-Collinear Effective Theory nicht anwendbar ist. KW - High-energy physics Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-371060 ER - TY - THES A1 - Aljasem, Anwar T1 - Der Einfluss des Hepatocyte growth factors auf die PD-L1-Expression in Kopf-Hals-Karzinomen: Die Bedeutung des MAPK-, AKT- und STAT3-Signalwegs T1 - The impact of Hepatocyte growth factor (HGF) on PD-L1 expression in HNSCC: The meaning of MAPK, AKT, and STAT3 signaling pathways N2 - Die zielgerichtete Therapie und die Immuncheckpoint-Inhibitoren haben die Tumortherapie revolutioniert. Während erstere die Tumorzellen gezielt angreift, verhindern letztere die Hemmung des Immunsystems durch Immuncheckpoints, um eine robuste Immunantwort zu erreichen. Zusätzlich ist das Nebenwirkungsprofil bei direktem Vergleich mit der konventionellen Chemotherapie günstiger. Beim HNSCC werden beide Ansätze angewendet. Cetuximab ist ein monoklonaler Antikörper, der sich gegen EGFR, welcher bei HNSCC überexprimiert ist, richtet. Nivolumab und Pembrolizumab richten sich gegen das Immuncheckpoint-Protein PD-1. Nach wie vor sind die Resistenzen, sowohl die initialen als auch die erworbenen, die größte zu überwindende Herausforderung. Aufbauend auf dem Ergebnis vorangegangener Arbeiten, die zeigen konnten, dass HGF über c-MET die Expression des Immuncheckpointliganden PD-L1 steigert, setzt sich diese Arbeit weiter mit den intrazellulären nachgeschalteten Signalwegen nach c-MET Aktivierung auseinander. Dies ist von besonderem Interesse, weil diese Signalwege ebenfalls für die Resistenzentwicklung verantwortlich sein können, zeitgleich können diese im Rahmen der zielgerichteten Therapie gezielt inhibiert werden. Um den HGF-Einfluss auf die intrazellulären Signalwege zu prüfen, wurden vier etablierte HNSCC-Zelllinien herangezogen. Im ersten Teil der Arbeit wurden die 4 HNSCC-abgeleitete Zelllinien mit HGF stimuliert und mittels Western Blot der PD-L1-Anstieg und die Phosphorylierungsänderung der Schlüsselproteine der einzelnen Signalwege nachgewiesen. Daraus ergab sich, dass HGF die MAPK- und PIK3/AKT-Signalwege aktiviert. Während eine kombinierte Blockade des MAPK-Signalwegs den PD-L1-Anstieg vollständig verhindern konnte, hemmte die PIK3/AKT-Blockade den PD-L1-Anstieg nur partiell. Im zweiten Teil wurde mit siRNA der hauptsächlich für den PD-L1-Anstieg zuständige MAPK-Signalweg unterbunden, was mittels quantitativer PCR auf der mRNA-Ebene nachgewiesen werden konnte. Mittels Western Blot konnte entsprechend gezeigt werden, dass der PD-L1-Anstieg trotz HGF-Stimulation bei nicht funktionsfähigem MAPK-Signalweg eingeschränkt war. Weiter wurde der Effekt mit dem Medikament Trametinib, das im Rahmen der zielgerichteten Therapie bei malignem Melanom und NSCLC für die MAPK-Signalweg-Hemmung zugelassen ist, evaluiert. Sowohl im Western Blot als auch in der Durchflusszytometrie konnte bestätigt werden, dass Trametinib den HGF-induzierten Anstieg von PD-L1 signifikant blockiert. Darüber hinaus konnte im Rahmen der Western Blot-Versuche gezeigt werden, dass die Signalwege und die PD-L1-Expression in den Zelllinien unterschiedlich aktiv bzw. hoch waren. Unter den vier Zelllinien zeigte die FaDu-Zelllinie eine erhöhte PI3K/AKT-Aktivität, Detroit562 und SCC9 eine erhöhte MAPK-Aktivität. Die PD-L1- Expression war in der SCC9-Zelllinie am höchsten. Die Arbeit zeigt eine einheitliche Reaktion der HNSCC-Zelllinien auf den Wachstumsfaktor HGF, welcher im Tumormilieu von HNSCC oft in hoher Konzentration vorhanden ist. Neben dem EGFR-Antikörper (Cetuximab) kann eine kombinierte Hemmung entweder von c-MET oder von den nachgeschalteten Signalwegen MAPK und PI3K/AKT bei Resistenzen, Progression oder Unverträglichkeiten eine Möglichkeit für eine wirksamere Therapie von HNSCC darstellen. Ein Screening der Signalwege und deren Aktivierungsmechanismen könnte bei Resistenzen oder bei einem Rezidiv/Progress dazu beitragen, gezielt die alternative Aktivierung zu hemmen und möglicherweise die Wirksamkeit einer Immuncheckpointblockade zu verbessern. N2 - Targeted therapy and immune checkpoint inhibitors have revolutionized tumor therapy. While the former specifically targets tumor cells, the latter prevents inhibitory immune responses via immune checkpoints to achieve a robust immune response. Additionally, the side effect profile is more favorable when directly compared to conventional chemotherapy. Both approaches are approved for the treatment of Head and Neck Squamous Cell Carcinoma (HNSCC). Cetuximab is a monoclonal antibody that targets EGFR, which is overexpressed in HNSCC. Nivolumab and Pembrolizumab target the immune checkpoint protein PD-1. Resistances, both initial and acquired, however, remain significant challenges to overcome. Building on a previous report that HGF upregulates the immune checkpoint ligand PD-L1 expression via the c-MET pathway, this study investigates the intracellular downstream signaling pathways activated by HGF. This is of particular interest because these signaling pathways contribute to resistance development, while at the same time, they can be specifically inhibited in the context of targeted therapy. To examine the influence of HGF on intracellular signaling pathways, four established HNSCC cell lines were utilized. In the first part of the study, the four HNSCC-derived cell lines were stimulated with HGF, and the increase in PD-L1 expression and changes in phosphorylation levels of key proteins in the individual signaling pathways were analyzed using Western Blots. It was found that HGF activates the MAPK and PI3K/AKT pathways. While MAPK inhibition completely blocked the PD-L1 increase, PI3K/AKT inhibition only partially did so after HGF stimulation. In the second part, the MAPK pathway, mainly responsible for the increase in PD-L1, was inhibited using siRNA. Quantitative PCR validated corresponding mRNA levels. Western Blots further showed that the increase in PD-L1 was reduced despite HGF stimulation when the MAPK pathway was non-functional. In line with previous results, inhibiting MAPKs with the drug Trametinib, which is approved as a targeted therapy for malignant melanoma and NSCLC, significantly blocks HGF-induced PD-L1 expression based on Western Blot and flow cytometry analysis. Notably, the activity of the different signaling pathways and the expression levels of PD-L1 vary among the different cell lines, as Western Blot analyses reveal. For instance, while the FaDu cell line manifested high activity in the PI3K/AKT pathway, Detroit562 and SCC9 showed increased MAPK activity. Nonetheless, the SCC9 cell line showed the highest PD-L1 expression level. This study demonstrated that HNSCC cell lines similarly respond to the growth factor HGF, which is frequently present in high concentrations in the tumor microenvironment of HNSCC. Additionally, the inhibition of c-MET and its downstream MAPK or PI3K/AKT pathways in combination with EGFR blockade by Cetuximab may offer a more effective treatment strategy for HNSCC patients in cases of therapeutic resistance, disease progression, or drug intolerance. Screening of the signaling pathways and their activation mechanisms could, in cases of resistance, recurrence, or progression, contribute to the specific inhibition of alternative activation and potentially improve the efficacy of immune checkpoint blockade. KW - Hepatozyten-Wachstumsfaktor KW - MAP-Kinase KW - Plattenepithelcarcinom KW - PD-L1 Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370358 ER - TY - THES A1 - Lechermeier, Carina T1 - Neuroanatomical and functional evaluation of ADHD candidate genes in the model organism zebrafish (\(Danio\) \(rerio\)) T1 - Neuroanatomische und funktionelle Auswertung von ADHS Kandidatengenen im Modellorganismus Zebrafisch (\(Danio\) \(rerio\)) N2 - Attention deficit hyperactivity disorder (ADHD) is one of the most prevalent developmental disorders, affecting 5.9% children and adolescents and 2.5% adults worldwide. The core characteristics are age-inappropriate levels of hyperactivity, impulsivity and inattention, often accompanied by co-morbidities such as mood and conduct disorders as wells as learning deficits. In the majority of cases, ADHD is caused by an interplay of accumulated genetic and environmental risk factors. Twin studies report a very high heritability of 70–80%, however, common genetic variants in the population only explain a third of the heritability. The rest of the genetic predisposition is composed of rare copy number variations (CNVs) and gene x environment interactions including epigenetic alterations. Through genome wide association (GWAS) and linkage studies a number of likely candidate genes were identified. A handful of them play a role in dopamine or noradrenaline neurotransmitter systems, simultaneously those systems are the main targets of common drug treatment approaches. However, for the majority of candidates the biological function in relation to ADHD is unknown. It is crucial to identify those functions in order to gain a deeper understanding of the pathomechanism and genetic networks potentially responsible for the disorder. This work focuses on the three candidate genes GFOD1, SLC2A3 and LBX1 and their role in the healthy organism as well as in case of ADHD. The neuroanatomy was regarded through expression analysis and various behavioural assays of activity were performed to link alterations on the transcript level to phenotypes associated with the neurodevelopmental disorder. Zebrafish orthologues of the human risk genes were identified and extensive temporal and spacial expression characterisation performed via RNA in situ hybridisation. Through morpholino derived knock-down and mRNA overexpression zebrafish models with subsequent behavioural analysis, both hyper- and hypoactive phenotypes were discovered. Additional expression analysis through double in situ hybridisation revealed a co-localisation during zebrafish neurodevelopment of each gfod1 and slc2a3a together with gad1b, a marker for GABAergic neurons. Interestingly, both risk genes have previously been associated with glucose homeostasis and energy metabolism, which when disrupted could lead to alterations in signal transduction and neuron survival. Likewise, Lbx1 plays a pivotal role in GABAergic versus glutamatergic neuron specification during spinal cord and hindbrain development in mice and chicken. Preliminary results of this work suggest a similar role in zebrafish. Taken together, those findings on the one hand represent a sturdy basis to con- tinue studies of the function of the genes and on the other hand open up the opportunity to investigate novel aspects of ADHD research by exploring the role of the GABAergic neurotransmitter system or the connection between energy metabolism and psychiatric disorders. N2 - Die Aufmerksamkeitsdefizit-/Hyperaktivitätsstörung (ADHS) ist eine der am weitesten verbreiteten Entwicklungsstörungen, davon sind 5,9% Kinder und Jugendliche und 2,5% Erwachsene weltweit betroffen. Die Kernsymptome sind altersunangemessene Hyperaktivität, Impulsivität und Unaufmerksamkeit, oft begleitet von Begleiterkrankungen wie emotionale Dysregulation oder Verhal- tensauffälligkeiten sowie Lerndefiziten. In den meisten Fällen wird ADHS durch ein Zusammenspiel von angehäuften genetischen und umweltbedingten Risikofaktoren verursacht. Durch Zwillingsstudien gelang man zu einer errechneten Erblichkeit von 70–80%, jedoch erklären häufig auftretende genetische Varianten in der Bevölkerung nur ein Drittel der Erblichkeit. Der Rest der genetischen Veranlagung setzt sich aus seltenen Kopienzahlvariationen (CNV) und Interaktionen von Gen x Umwelt, einschließlich epigenetischer Veränderungen, zusammen. Durch genomweite Assoziationsstudien (GWAS) und Kopplungsanalysen wurden eine Reihe von wahrscheinlichen Kandidatengenen identifiziert. Eine Handvoll von ihnen spielen eine Rolle in den Dopamin oder Noradrenalin Neurotransmittersystemen. Diese Systeme sind gleichzeitig die Hauptangriffspunkte der gängigsten Medikamente, die zur Behandlung von ADHS eingesetzt werden. Allerdings ist für die Mehrheit der Kandidatengene die biologische Funktion in Bezug auf ADHS unbekannt. Es ist essentiell diese Funktionen zu identifizieren um ein tieferes Verständnis der Ätiopathogenese und der genetische Netzwerke, die möglicherweise für die Störung verantwortlich sind, zu erlangen. Diese Arbeit konzentriert sich auf die drei Kandidatengene GFOD1, SLC2A3 und LBX1 und ihre Rolle im gesunden Organismus sowie während ADHS. Die Neuroanatomie wurde durch Expressionsanalyse betrachtet und verschiedene aktivitätsbasierte Verhaltensessays wurden durchgeführt, um Veränderungen auf Transkriptebene mit den zugehörigen Phänotypen der neurologischen Entwick- lungsstörung in Verbindung zu bringen. Zebrafischorthologe der menschlichen Kandidatengene wurden identifiziert und umfangreiche zeitliche und räumli- che Expressionsanalysen via RNA in situ Hybridisierung durchgeführt. Durch Morpholino-Knockdown und mRNA-Überexpressions Zebrafischmodelle mit anschließender Verhaltensanalyse wurden sowohl hyper- als auch hypoaktive Phänotypen entdeckt. Eine zusätzliche Expressionsanalyse durch doppelte in situ Hybridisierung ergab eine Kolokalisierung während der Zebrafischneuroentwicklung von jeweils gfod1 und slc2a3a zusammen mit gad1b, einem Marker für GABAerge Neuronen. Interessanterweise wurden beide Risikogene zuvor mit der Glukosehomöostase und dem Energiestoffwechsel in Verbindung gebracht, die, wenn sie gestört werden, zu Veränderungen der Signalübertragung und der Lebensdauer von Neuronen führen können. Desgleichen spielt Lbx1 eine entscheidende Rolle bei der Spezifikation von GABAergen versus glutamatergenen Neuronen während der Entwicklung des Rückenmarks in der Wirbelsäule und im Hinterhirn von Mäusen und Hühnern. Vorläufige Ergebnisse dieser Arbeit deuten auf eine ähnliche Rolle beim Zebrafisch hin. Zusammengenommen stellen diese Erkenntnisse einerseits eine solide Grundlage für weitere Untersuchungen zur Funktion der Gene dar, andererseits eröffnet sich daraus die Möglichkeit neue Aspekte der ADHS-Forschung zu untersuchen, bei denen der Fokus auf der Rolle des GABAergen Neurotransmittersystems oder der Beziehung zwischen Energiestoffwechsel und psychiatrischen Erkrankungen liegt. KW - Aufmerksamkeitsdefizit-Syndrom KW - Zebrabärbling KW - ADHD KW - zebrafish KW - genes KW - behaviour KW - ADHS Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-371084 ER - TY - JOUR A1 - Zhang, Zishuai A1 - Ye, Siyu A1 - Gbureck, Uwe A1 - Barralet, Jake E. A1 - Merle, Géraldine T1 - Cavitation Mediated 3D Microstructured Architectures from Nanocarbon JF - Advanced Functional Materials N2 - Here, the formation of high surface area microscale assemblies of nanocarbon through phosphate and ultrasound cavitation treatment is reported. Despite high conductivity and large surface area, potential health and safety concerns limit the use of nanocarbon and add challenges to handling. Previously, it is shown that phosphate ultrasonic bonding is ineffective for organic materials but in this study, it is found that by a preliminary oxidizing treatment, several carbons can be readily assembled from xerogels. Assembling nanocarbon into microparticles can usually require a binder or surfactants, which can reduce surface area or conductivity and generate a low microsphere yield. Carbon nanotube microspheres are nitrogen-doped and flower-like nanostructured Pt deposited on their surface, and finally showcased as efficient cathode electrocatalysts for the oxygen reduction reaction (half-wave potential 0.78 V vs reversible hydrogen electrode) and methanol oxidation (417 mA mg−1). In particular, no significant degradation of the catalysts is detected after 12 000 cycles (26.6 h). These results indicate the potential of this multimaterial assembly method and open a new way to improve handling of nanoscale materials. KW - carbon nanotube microspheres KW - cavitation KW - oxygen reduction reaction KW - platinum nanostructures Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-233926 VL - 28 ER - TY - JOUR A1 - McMaster, Rebecca A1 - Hoefner, Christiane A1 - Hrynevich, Andrei A1 - Blum, Carina A1 - Wiesner, Miriam A1 - Wittmann, Katharina A1 - Dargaville, Tim R. A1 - Bauer-Kreisel, Petra A1 - Groll, Jürgen A1 - Dalton, Paul D. A1 - Blunk, Torsten T1 - Tailored Melt Electrowritten Scaffolds for the Generation of Sheet-Like Tissue Constructs from Multicellular Spheroids JF - Advanced Healthcare Materials N2 - Melt electrowriting (MEW) is an additive manufacturing technology that is recently used to fabricate voluminous scaffolds for biomedical applications. In this study, MEW is adapted for the seeding of multicellular spheroids, which permits the easy handling as a single sheet-like tissue-scaffold construct. Spheroids are made from adipose-derived stromal cells (ASCs). Poly(ε-caprolactone) is processed via MEW into scaffolds with box-structured pores, readily tailorable to spheroid size, using 13–15 µm diameter fibers. Two 7–8 µm diameter “catching fibers” near the bottom of the scaffold are threaded through each pore (360 and 380 µm) to prevent loss of spheroids during seeding. Cell viability remains high during the two week culture period, while the differentiation of ASCs into the adipogenic lineage is induced. Subsequent sectioning and staining of the spheroid-scaffold construct can be readily performed and accumulated lipid droplets are observed, while upregulation of molecular markers associated with successful differentiation is demonstrated. Tailoring MEW scaffolds with pores allows the simultaneous seeding of high numbers of spheroids at a time into a construct that can be handled in culture and may be readily transferred to other sites for use as implants or tissue models. KW - 3D printing KW - additive manufacturing KW - adipose tissue engineering Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-223921 VL - 8 ER - TY - JOUR A1 - Selcuk, Nalan Alan A1 - Toklu, Turkay A1 - Beykan, Seval A1 - Karaaslan, Serife Ipek T1 - Evaluation of the dosimetry approaches in ablation treatment of thyroid cancer JF - Journal of Applied Clinical Medical Physics N2 - In this study, we aimed to evaluate dosimetric approaches in ablation treatment of Differentiated Thyroid Carcinoma (DTC) without interrupting the clinical routine. Prior to therapy, 10.7 MBq 131I in average was orally given to 24 patients suffering from DTC. MIRD formalism was used for dosimetric calculations. For blood and bone marrow dosimetry, blood samples and whole-body counts were collected at 2, 24, 72, and 120 h after I-131 administration. For remnant tissue dosimetry, uptake measurements were performed at the same time intervals. To estimate the remnant volume, anterior and lateral planar gamma camera images were acquired with a reference source within the field of view at 24 h after I-131 administration. Ultrasound imaging was also performed. Treatment activities determined with the fixed activity method were administered to the patients. Secondary cancer risk relative to applied therapy was evaluated for dosimetric approaches. The average dose to blood and bone marrow were determined as 0.15 ± 0.04 and 0.11 ± 0.04 Gy/GBq, respectively. The average remnant tissue dose was 0.58 ± 0.52 Gy/MBq and the corresponding required activity to ablate the remnant was approximately 1.3 GBq of 131I. A strong correlation between 24th-hour uptake and time-integrated activity coefficient values was obtained. Compared to fixed activity method, approximately five times higher secondary cancer risk was determined in bone marrow dosimetry, while the risk was about three times lower in lesion-based dosimetry. KW - bone marrow dosimetry KW - remnant tissue dosimetry KW - thyroid ablation treatment Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-235882 VL - 19 ER - TY - JOUR A1 - Göttlich, Claudia A1 - Kunz, Meik A1 - Zapp, Cornelia A1 - Nietzer, Sarah L. A1 - Walles, Heike A1 - Dandekar, Thomas A1 - Dandekar, Gudrun T1 - A combined tissue-engineered/in silico signature tool patient stratification in lung cancer JF - Molecular Oncology N2 - Patient-tailored therapy based on tumor drivers is promising for lung cancer treatment. For this, we combined in vitro tissue models with in silico analyses. Using individual cell lines with specific mutations, we demonstrate a generic and rapid stratification pipeline for targeted tumor therapy. We improve in vitro models of tissue conditions by a biological matrix-based three-dimensional (3D) tissue culture that allows in vitro drug testing: It correctly shows a strong drug response upon gefitinib (Gef) treatment in a cell line harboring an EGFR-activating mutation (HCC827), but no clear drug response upon treatment with the HSP90 inhibitor 17AAG in two cell lines with KRAS mutations (H441, A549). In contrast, 2D testing implies wrongly KRAS as a biomarker for HSP90 inhibitor treatment, although this fails in clinical studies. Signaling analysis by phospho-arrays showed similar effects of EGFR inhibition by Gef in HCC827 cells, under both 2D and 3D conditions. Western blot analysis confirmed that for 3D conditions, HSP90 inhibitor treatment implies different p53 regulation and decreased MET inhibition in HCC827 and H441 cells. Using in vitro data (western, phospho-kinase array, proliferation, and apoptosis), we generated cell line-specific in silico topologies and condition-specific (2D, 3D) simulations of signaling correctly mirroring in vitro treatment responses. Networks predict drug targets considering key interactions and individual cell line mutations using the Human Protein Reference Database and the COSMIC database. A signature of potential biomarkers and matching drugs improve stratification and treatment in KRAS-mutated tumors. In silico screening and dynamic simulation of drug actions resulted in individual therapeutic suggestions, that is, targeting HIF1A in H441 and LKB1 in A549 cells. In conclusion, our in vitro tumor tissue model combined with an in silico tool improves drug effect prediction and patient stratification. Our tool is used in our comprehensive cancer center and is made now publicly available for targeted therapy decisions. KW - 3D lung tumor model KW - Boolean signaling network KW - chemoresistance KW - HSP90 inhibitor KW - insilico drug screening too KW - KRAS mutation signature Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-233137 VL - 12 ER - TY - JOUR A1 - Stromecki, Margaret A1 - Tatari, Nazanin A1 - Coudière Morrison, Ludivine A1 - Kaur, Ravinder A1 - Zagozewski, Jamie A1 - Palidwor, Gareth A1 - Ramaswamy, Vijay A1 - Skowron, Patryk A1 - Wölfl, Matthias A1 - Milde, Till A1 - Del Bigio, Marc R. A1 - Taylor, Michael D. A1 - Werbowetski-Ogilvie, Tamra E. T1 - Characterization of a novel OTX2-driven stem cell program in Group 3 and Group 4 medulloblastoma JF - Molecular Oncology N2 - Medulloblastoma (MB) is the most common malignant primary pediatric brain cancer. Among the most aggressive subtypes, Group 3 and Group 4 originate from stem/progenitor cells, frequently metastasize, and often display the worst prognosis, yet we know the least about the molecular mechanisms driving their progression. Here, we show that the transcription factor orthodenticle homeobox 2 (OTX2) promotes self-renewal while inhibiting differentiation in vitro and increases tumor initiation from MB stem/progenitor cells in vivo. To determine how OTX2 contributes to these processes, we employed complementary bioinformatic approaches to characterize the OTX2 regulatory network and identified novel relationships between OTX2 and genes associated with neuronal differentiation and axon guidance signaling in Group 3 and Group 4 MB stem/progenitor cells. In particular, OTX2 levels were negatively correlated with semaphorin (SEMA) signaling, as expression of 9 SEMA pathway genes is upregulated following OTX2 knockdown with some being potential direct OTX2 targets. Importantly, this negative correlation was also observed in patient samples, with lower expression of SEMA4D associated with poor outcome specifically in Group 4 tumors. Functional proof-of-principle studies demonstrated that increased levels of select SEMA pathway genes are associated with decreased self-renewal and growth in vitro and in vivo and that RHO signaling, known to mediate the effects of SEMA genes, is contributing to the OTX2 KD phenotype. Our study provides mechanistic insight into the networks controlled by OTX2 in MB stem/progenitor cells and reveals novel roles for axon guidance genes and their downstream effectors as putative tumor suppressors in MB. KW - axon guidance genes KW - medulloblastoma KW - orthodenticle homeobox 2 KW - RHO KW - semaphorin KW - stem cells Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-240089 VL - 12 ER - TY - JOUR A1 - Storey, Benjamin C. A1 - Staplin, Natalie A1 - Haynes, Richard A1 - Reith, Christina A1 - Emberson, Jonathan A1 - Herrington, William G. A1 - Wheeler, David C. A1 - Walker, Robert A1 - Fellström, Bengt A1 - Wanner, Christoph A1 - Landray, Martin J. A1 - Baigent, Colin T1 - Lowering LDL cholesterol reduces cardiovascular risk independently of presence of inflammation JF - Kidney International N2 - Markers of inflammation, including plasma C-reactive protein (CRP), are associated with an increased risk of cardiovascular disease, and it has been suggested that this association is causal. However, the relationship between inflammation and cardiovascular disease has not been extensively studied in patients with chronic kidney disease. To evaluate this, we used data from the Study of Heart and Renal Protection (SHARP) to assess associations between circulating CRP and LDL cholesterol levels and the risk of vascular and non-vascular outcomes. Major vascular events were defined as nonfatal myocardial infarction, cardiac death, stroke or arterial revascularization, with an expanded outcome of vascular events of any type. Higher baseline CRP was associated with an increased risk of major vascular events (hazard ratio per 3x increase 1.28; 95% confidence interval 1.19-1.38). Higher baseline LDL cholesterol was also associated with an increased risk of major vascular events (hazard ratio per 0.6 mmol/L higher LDL cholesterol; 1.14, 1.06-1.22). Higher baseline CRP was associated with an increased risk of a range of non-vascular events (1.16, 1.12-1.21), but there was a weak inverse association between baseline LDL cholesterol and non-vascular events (0.96, 0.92-0.99). The efficacy of lowering LDL cholesterol with simvastatin/ezetimibe on major vascular events, in the randomized comparison, was similar irrespective of CRP concentration at baseline. Thus, decisions to offer statin-based therapy to patients with chronic kidney disease should continue to be guided by their absolute risk of atherosclerotic events. Estimation of such risk may include plasma biomarkers of inflammation, but there is no evidence that the relative beneficial effects of reducing LDL cholesterol depends on plasma CRP concentration. KW - C-reactive protein KW - inflammation KW - LDL cholesterol KW - randomized trials KW - vascular disease Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-240067 VL - 93 ER - TY - JOUR A1 - Hoenigl, Martin A1 - Orasch, Thomas A1 - Faserl, Klaus A1 - Prattes, Juergen A1 - Loeffler, Juergen A1 - Springer, Jan A1 - Gsaller, Fabio A1 - Reischies, Frederike A1 - Duettmann, Wiebke A1 - Raggam, Reinhard B. A1 - Lindner, Herbert A1 - Haas, Hubertus T1 - Triacetylfusarinine C: A urine biomarker for diagnosis of invasive aspergillosis JF - Journal of Infection N2 - Objectives Early diagnosis of invasive aspergillosis (IA) remains challenging, with available diagnostics being limited by inadequate sensitivities and specificities. Triacetylfusarinine C, a fungal siderophore that has been shown to accumulate in urine in animal models, is a potential new biomarker for diagnosis of IA. Methods We developed a method allowing absolute and matrix-independent mass spectrometric quantification of TAFC. Urine TAFC, normalized to creatinine, was determined in 44 samples from 24 patients with underlying hematologic malignancies and probable, possible or no IA according to current EORTC/MSG criteria and compared to other established biomarkers measured in urine and same-day blood samples. Results TAFC/creatinine sensitivity, specificity, positive and negative likelihood ratio for probable versus no IA (cut-off ≥ 3) were 0.86, 0.88, 6.86, 0.16 per patient. Conclusion For the first time, we provide proof for the occurrence of TAFC in human urine. TAFC/creatinine index determination in urine showed promising results for diagnosis of IA offering the advantages of non-invasive sampling. Sensitivity and specificity were similar as reported for GM determination in serum and bronchoalveolar lavage, the gold standard mycological criterion for IA diagnosis. KW - aspergillosis KW - biomarker KW - diagnosis KW - siderophore KW - urine Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-320939 VL - 78 ER - TY - JOUR A1 - Estes, Chris A1 - Anstee, Quentin M. A1 - Arias-Loste, Maria Teresa A1 - Bantel, Heike A1 - Bellentani, Stefano A1 - Caballeria, Joan A1 - Colombo, Massimo A1 - Craxi, Antonio A1 - Crespo, Javier A1 - Day, Christopher P. A1 - Eguchi, Yuichiro A1 - Geier, Andreas A1 - Kondili, Loreta A. A1 - Kroy, Daniela C. A1 - Lazarus, Jeffrey V. A1 - Loomba, Rohit A1 - Manns, Michael P. A1 - Marchesini, Giulio A1 - Nakajima, Atsushi A1 - Negro, Francesco A1 - Petta, Salvatore A1 - Ratziu, Vlad A1 - Romero-Gomez, Manuel A1 - Sanyal, Arun A1 - Schattenberg, Jörn M. A1 - Tacke, Frank A1 - Tanaka, Junko A1 - Trautwein, Christian A1 - Wei, Lai A1 - Zeuzem, Stefan A1 - Ravazi, Homie T1 - Modeling NAFLD disease burden in China, France, Germany, Italy, Japan, Spain, United Kingdom, and United States for the period 2016–2030 JF - Journal of Hepatology N2 - Background & Aims Non-alcoholic fatty liver disease (NAFLD) and non-alcoholic steatohepatitis (NASH) are increasingly a cause of cirrhosis and hepatocellular carcinoma globally. This burden is expected to increase as epidemics of obesity, diabetes and metabolic syndrome continue to grow. The goal of this analysis was to use a Markov model to forecast NAFLD disease burden using currently available data. Methods A model was used to estimate NAFLD and NASH disease progression in eight countries based on data for adult prevalence of obesity and type 2 diabetes mellitus (DM). Published estimates and expert consensus were used to build and validate the model projections. Results If obesity and DM level off in the future, we project a modest growth in total NAFLD cases (0–30%), between 2016–2030, with the highest growth in China as a result of urbanization and the lowest growth in Japan as a result of a shrinking population. However, at the same time, NASH prevalence will increase 15–56%, while liver mortality and advanced liver disease will more than double as a result of an aging/increasing population. Conclusions NAFLD and NASH represent a large and growing public health problem and efforts to understand this epidemic and to mitigate the disease burden are needed. If obesity and DM continue to increase at current and historical rates, both NAFLD and NASH prevalence are expected to increase. Since both are reversible, public health campaigns to increase awareness and diagnosis, and to promote diet and exercise can help manage the growth in future disease burden. Lay summary Non-alcoholic fatty liver disease and non-alcoholic steatohepatitis can lead to advanced liver disease. Both conditions are becoming increasingly prevalent as the epidemics of obesity and diabetes continue to increase. A mathematical model was built to understand how the disease burden associated with non-alcoholic fatty liver disease and non-alcoholic steatohepatitis will change over time. Results suggest increasing cases of advanced liver disease and liver-related mortality in the coming years. KW - burden of disease KW - cardiovascular disease KW - health care resource utilization KW - metabolic syndrome KW - NAFLD KW - NASH KW - cirrhosis KW - HCC KW - diabetes mellitus KW - obesity Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-227286 VL - 69 ER - TY - JOUR A1 - Tappenbeck, Nils A1 - Schröder, Hannes M. A1 - Niebergall-Roth, Elke A1 - Hassinger, Fathema A1 - Dehio, Ulf A1 - Dieter, Kathrin A1 - Kraft, Korinna A1 - Kerstan, Andreas A1 - Esterlechner, Jasmina A1 - Frank, Natasha Y. A1 - Scharffetter-Kochanek, Karin A1 - Murphy, George F. A1 - Orgill, Dennis P. A1 - Beck, Joachim A1 - Frank, Markus H. A1 - Ganss, Christoph A1 - Kluth, Mark A. T1 - In vivo safety profile and biodistribution of GMP-manufactured human skin-derived ABCB5-positive mesenchymal stromal cells for use in clinical trials JF - Cytotherapy N2 - Background aims Human dermal ABCB5-expressing mesenchymal stromal cells (ABCB5+ MSCs) represent a promising candidate for stem cell–based therapy of various currently uncurable diseases in several fields of regenerative medicine. We have developed and validated a method to isolate, from human skin samples, and expand ABCB5+ MSCs that meet the guideline criteria of the International Society for Cellular Therapy. We are able to process these cells into a Good Manufacturing Practice–conforming, MSC-based advanced-therapy medicinal product. Methods To support the development of ABCB5+ MSCs for potential therapeutic topical, intramuscular and intravenous administration, we have tested our product in a series of Good Laboratory Practice–compliant nonclinical in-vivo studies addressing all relevant aspects of biosafety, including potential long-term persistence and proliferation, distribution to nontarget tissues, differentiation into undesired cell types, ectopic tissue formation, tumor formation and local tissue reaction. Results (i) Subcutaneous application of 1 × 107 ABCB5+ MSCs/animal and intravenous application of 2 × 106 ABCB5+ MSCs/animal, respectively, to immunocompromised mice did not result in safety-relevant biodistribution, persistence or proliferation of the cells; (ii) three monthly subcutaneous injections of ABCB5+ MSCs at doses ranging from 1 × 105 to 1 × 107 cells/animal and three biweekly intravenous injections of 2 × 106 ABCB5+ MSCs/animal, respectively, to immunocompromised mice were nontoxic and revealed no tumorigenic potential; and (iii) intramuscular injection of 5 × 106 ABCB5+ MSCs/animal to immunocompromised mice was locally well tolerated. Discussion The present preclinical in vivo data demonstrate the local and systemic safety and tolerability of a novel advanced-therapy medicinal product based on human skin-derived ABCB5+ MSCs. KW - stromal cells KW - stem cells KW - MSC KW - biodistribution KW - safety KW - ABCB5 KW - GMP KW - tumorigenicity KW - toxicity KW - persistence Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-240456 VL - 21 ER - TY - JOUR A1 - Wurm, Michael A1 - Stark, Thomas A1 - Zhu, Xiao Xiang A1 - Weigand, Matthias A1 - Taubenböck, Hannes T1 - Semantic segmentation of slums in satellite images using transfer learning on fully convolutional neural networks JF - ISPRS Journal of Photogrammetry and Remote Sensing N2 - Unprecedented urbanization in particular in countries of the global south result in informal urban development processes, especially in mega cities. With an estimated 1 billion slum dwellers globally, the United Nations have made the fight against poverty the number one sustainable development goal. To provide better infrastructure and thus a better life to slum dwellers, detailed information on the spatial location and size of slums is of crucial importance. In the past, remote sensing has proven to be an extremely valuable and effective tool for mapping slums. The nature of used mapping approaches by machine learning, however, made it necessary to invest a lot of effort in training the models. Recent advances in deep learning allow for transferring trained fully convolutional networks (FCN) from one data set to another. Thus, in our study we aim at analyzing transfer learning capabilities of FCNs to slum mapping in various satellite images. A model trained on very high resolution optical satellite imagery from QuickBird is transferred to Sentinel-2 and TerraSAR-X data. While free-of-charge Sentinel-2 data is widely available, its comparably lower resolution makes slum mapping a challenging task. TerraSAR-X data on the other hand, has a higher resolution and is considered a powerful data source for intra-urban structure analysis. Due to the different image characteristics of SAR compared to optical data, however, transferring the model could not improve the performance of semantic segmentation but we observe very high accuracies for mapped slums in the optical data: QuickBird image obtains 86–88% (positive prediction value and sensitivity) and a significant increase for Sentinel-2 applying transfer learning can be observed (from 38 to 55% and from 79 to 85% for PPV and sensitivity, respectively). Using transfer learning proofs extremely valuable in retrieving information on small-scaled urban structures such as slum patches even in satellite images of decametric resolution. KW - slums KW - FCN KW - convolutional neural networks KW - deep learning KW - transfer learning Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-233799 VL - 150 ER - TY - JOUR A1 - Czimmerer, Zsolt A1 - Daniel, Bence A1 - Horvath, Attila A1 - Rückerl, Dominik A1 - Nagy, Gergely A1 - Kiss, Mate A1 - Peloquin, Matthew A1 - Budai, Marietta M. A1 - Cuaranta-Monroy, Ixchelt A1 - Simandi, Zoltan A1 - Steiner, Laszlo A1 - Nagy Jr., Bela A1 - Poliska, Szilard A1 - Banko, Csaba A1 - Bacso, Zsolt A1 - Schulman, Ira G. A1 - Sauer, Sascha A1 - Deleuze, Jean-Francois A1 - Allen, Judith E. A1 - Benko, Szilvia A1 - Nagy, Laszlo T1 - The Transcription Factor STAT6 Mediates Direct Repression of Inflammatory Enhancers and Limits Activation of Alternatively Polarized Macrophages JF - Immunity N2 - The molecular basis of signal-dependent transcriptional activation has been extensively studied in macrophage polarization, but our understanding remains limited regarding the molecular determinants of repression. Here we show that IL-4-activated STAT6 transcription factor is required for the direct transcriptional repression of a large number of genes during in vitro and in vivo alternative macrophage polarization. Repression results in decreased lineage-determining transcription factor, p300, and RNA polymerase II binding followed by reduced enhancer RNA expression, H3K27 acetylation, and chromatin accessibility. The repressor function of STAT6 is HDAC3 dependent on a subset of IL-4-repressed genes. In addition, STAT6-repressed enhancers show extensive overlap with the NF-κB p65 cistrome and exhibit decreased responsiveness to lipopolysaccharide after IL-4 stimulus on a subset of genes. As a consequence, macrophages exhibit diminished inflammasome activation, decreased IL-1β production, and pyroptosis. Thus, the IL-4-STAT6 signaling pathway establishes an alternative polarization-specific epigenenomic signature resulting in dampened macrophage responsiveness to inflammatory stimuli. KW - IL-4 KW - STAT6 KW - alternative macrophage polarization KW - transcription KW - repression KW - inflammation KW - inflammasome activation KW - pyroptosis KW - IL-1β KW - macrophage epigenomics Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-223380 VL - 48 ER - TY - JOUR A1 - Trübe, Patricia A1 - Hertlein, Tobias A1 - Mrochen, Daniel M. A1 - Schulz, Daniel A1 - Jorde, Ilka A1 - Krause, Bettina A1 - Zeun, Julia A1 - Fischer, Stefan A1 - Wolf, Silver A. A1 - Walther, Birgit A1 - Semmler, Torsten A1 - Bröker, Barbara M. A1 - Ulrich, Rainer G. A1 - Ohlsen, Knut A1 - Holtfreter, Silva T1 - Bringing together what belongs together: Optimizing murine infection models by using mouse-adapted Staphylococcus aureus strains JF - International Journal of Medical Microbiology N2 - Staphylococcus (S.) aureus is a leading cause of bacterial infection world-wide, and currently no vaccine is available for humans. Vaccine development relies heavily on clinically relevant infection models. However, the suitability of mice for S. aureus infection models has often been questioned, because experimental infection of mice with human-adapted S. aureus requires very high infection doses. Moreover, mice were not considered to be natural hosts of S. aureus. The latter has been disproven by our recent findings, showing that both laboratory mice, as well as wild small mammals including mice, voles, and shrews, are naturally colonized with S. aureus. Here, we investigated whether mouse-and vole-derived S. aureus strains show an enhanced virulence in mice as compared to the human-adapted strain Newman. Using a step-wise approach based on the bacterial genotype and in vitro assays for host adaptation, we selected the most promising candidates for murine infection models out of a total of 254 S. aureus isolates from laboratory mice as well as wild rodents and shrews. Four strains representing the clonal complexes (CC) 8, 49, and 88 (n = 2) were selected and compared to the human-adapted S. aureus strain Newman (CC8) in murine pneumonia and bacteremia models. Notably, a bank vole-derived CC49 strain, named DIP, was highly virulent in BALB/c mice in pneumonia and bacteremia models, whereas the other murine and vole strains showed virulence similar to or lower than that of Newman. At one tenth of the standard infection dose DIP induced disease severity, bacterial load and host cytokine and chemokine responses in the murine bacteremia model similar to that of Newman. In the pneumonia model, DIP was also more virulent than Newman but the effect was less pronounced. Whole genome sequencing data analysis identified a pore-forming toxin gene, lukF-PV(P83)/lukM, in DIP but not in the other tested S. aureus isolates. To conclude, the mouse-adapted S. aureus strain DIP allows a significant reduction of the inoculation dose in mice and is hence a promising tool to develop clinically more relevant infection models. KW - Staphylococcus aureus KW - host-adapted KW - infection model KW - mouse KW - vole KW - CC49 Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-229081 VL - 309 ER - TY - JOUR A1 - Heimann, Sebastian M. A1 - Penack, Olaf A1 - Heinz, Werner J. A1 - Rachow, Tobias A1 - Egerer, Gerlinde A1 - Kessel, Johanna A1 - Claßen, Annika Y. A1 - Vehreschild, Jörg Janne T1 - Intravenous and tablet formulation of posaconazole in antifungal therapy and prophylaxis: A retrospective, non-interventional, multicenter analysis of hematological patients treated in tertiary-care hospitals JF - International Journal of Infectious Diseases N2 - Objectives Novel formulations (gastro-resistant tablet and intravenous solution) of posaconazole (POS) have been approved in prophylaxis and therapy of invasive fungal diseases (IFDs). Study aim was to analyze treatment strategies and clinical effectiveness. Methods We set up a web-based registry on www.ClinicalSurveys.net for documentation of comprehensive data of patients who received novel POS formulations. Data analysis was split into two groups of patients who received novel POS formulations for antifungal prophylaxis (posaconazole prophylaxis group) and antifungal therapy (posaconazole therapy group), respectively. Results Overall, 180 patients (151 in the posaconazole prophylaxis group and 29 in the posaconazole therapy group) from six German tertiary care centers and hospitalized between 05/2014 – 03/2016 were observed. Median age was 58 years (range: 19 – 77 years) and the most common risk factor for IFD was chemotherapy (n = 136; 76%). In the posaconazole prophylaxis group and posaconazole therapy group, median POS serum levels at steady-state were 1,068 μg/L (IQR 573–1,498 μg/L) and 904 μg/L (IQR 728–1,550 μg/L), respectively (P = 0.776). During antifungal prophylaxis with POS, nine (6%) probable/proven fungal breakthroughs were reported and overall survival rate of hospitalization was 86%. The median overall duration of POS therapy was 18 days (IQR: 7 – 23 days). Fourteen patients (48%) had progressive IFD under POS therapy, of these five patients (36%) died related to or likely related to IFD. Conclusions Our study demonstrates clinical effectiveness of antifungal prophylaxis with novel POS formulations. In patients treated for possible/probable/proven IFD, we observed considerable mortality in patients receiving salvage treatment and with infections due to rare fungal species. KW - invasive fungal infection KW - neutropenia KW - posaconazole serum level KW - clinical effectiveness KW - high-risk patient Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-319567 VL - 83 ER - TY - JOUR A1 - Dietz, Maximilian A1 - Johnson, Alice A1 - Martínez-Martínez, Antonio A1 - Weller, Andrew S. T1 - The [Rh(Xantphos)]+ catalyzed hydroboration of diphenylacetylene using trimethylamine-borane JF - Inorganica Chimica Acta N2 - The rhodium(I) complex [Rh(κ3-P,O,P-Xantphos)(η2-PhC≡CPh)][BArF4] (ArF = 3,5-(CF3)2C6H4) is an effective catalyst for the cis-selective hydroboration of the alkyne diphenylacetylene using the amine-borane H3B·NMe3. Detailed mechanistic studies, that include initial rate measurements, full simulation of temporal profiles for a variety of catalyst and substrate concentrations, and speciation experiments, suggest a mechanism that involves initial coordination of alkyne and a saturation kinetics regime for amine-borane binding. The solid-state molecular structure of a model complex that probes the proposed resting state is also reported, [Rh(κ3-P,O,P-Xantphos)(NCMe)(η2-PhC≡CPh)][BArF4]. KW - rhodium KW - hydroboration KW - amine borane KW - mechanism Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-225352 VL - 491 ER - TY - JOUR A1 - Seitz, Nicola A1 - vanEngelsdorp, Dennis A1 - Leonhardt, Sara D. T1 - Conserving bees in destroyed landscapes: The potentials of reclaimed sand mines JF - Global Ecology and Conservation N2 - Sand mines represent anthropogenically impacted habitats found worldwide, which bear potential for bee conservation. Although floral resources can be limited at these habitats, vegetation free patches of open sandy soils and embankments may offer good nesting possibilities for sand restricted and other bees. We compared bee communities as found in three reclaimed sand mines and at adjacent roadside meadows in Maryland, USA, over two years. Both sand mines and roadsides hosted diverse bee communities with 111 and 88 bee species, respectively. Bee abundances as well as richness and Shannon diversity of bee species were higher in sand mines than at roadsides and negatively correlated with the percentage of vegetational ground cover. Species composition also differed significantly between habitats. Sand mines hosted a higher proportion of ground nesters, more uncommon and more ‘sand loving’ bees similar to natural sandy areas of Maryland. Despite the destruction of the original pre-mining habitat, sand mines thus appear to represent a unique habitat for wild bees, particularly when natural vegetation and open sand spots are encouraged. Considering habitat loss, the lack of natural disturbance regimes, and ongoing declines of wild bees, sand mines could add promising opportunities for bee conservation which has hitherto mainly focused on agricultural and urban habitats. KW - bee conservation KW - bee decline KW - habitat restoration KW - land use KW - wild bees KW - ground nesters Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-235877 VL - 19 ER - TY - JOUR A1 - van de Peppel, L. J. J. A1 - Aanen, D. K. A1 - Biedermann, P. H. W. T1 - Low intraspecific genetic diversity indicates asexuality and vertical transmission in the fungal cultivars of ambrosia beetles JF - Fungal Ecology N2 - Ambrosia beetles farm ascomycetous fungi in tunnels within wood. These ambrosia fungi are regarded asexual, although population genetic proof is missing. Here we explored the intraspecific genetic diversity of Ambrosiella grosmanniae and Ambrosiella hartigii (Ascomycota: Microascales), the mutualists of the beetles Xylosandrus germanus and Anisandrus dispar. By sequencing five markers (ITS, LSU, TEF1α, RPB2, β-tubulin) from several fungal strains, we show that X. germanus cultivates the same two clones of A. grosmanniae in the USA and in Europe, whereas A. dispar is associated with a single A. hartigii clone across Europe. This low genetic diversity is consistent with predominantly asexual vertical transmission of Ambrosiella cultivars between beetle generations. This clonal agriculture is a remarkable case of convergence with fungus-farming ants, given that both groups have a completely different ecology and evolutionary history. KW - clonal fungiculture KW - ambrosia fungus KW - Ambrosiella KW - vertical transmission KW - symbiosis KW - Xylosandrus KW - Anisandrus KW - asexuality KW - genetic diversity Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-232161 VL - 32 ER - TY - JOUR A1 - Grebinyk, Anna A1 - Grebinyk, Sergii A1 - Prylutska, Svitlana A1 - Ritter, Uwe A1 - Matyshevska, Olga A1 - Dandekar, Thomas A1 - Frohme, Marcus T1 - C60 fullerene accumulation in human leukemic cells and perspectives of LED-mediated photodynamic therapy JF - Free Radical Biology and Medicine N2 - Recent progress in nanobiotechnology has attracted interest to a biomedical application of the carbon nanostructure C60 fullerene since it possesses a unique structure and versatile biological activity. C60 fullerene potential application in the frame of cancer photodynamic therapy (PDT) relies on rapid development of new light sources as well as on better understanding of the fullerene interaction with cells. The aim of this study was to analyze C60 fullerene effects on human leukemic cells (CCRF-CEM) in combination with high power single chip light-emitting diodes (LEDs) light irradiation of different wavelengths: ultraviolet (UV, 365 nm), violet (405 nm), green (515 nm) and red (632 nm). The time-dependent accumulation of fullerene C60 in CCRF-CEM cells up to 250 ng/106 cells at 24 h with predominant localization within mitochondria was demonstrated with immunocytochemical staining and liquid chromatography mass spectrometry. In a cell viability assay we studied photoexcitation of the accumulated C60 nanostructures with ultraviolet or violet LEDs and could prove that significant phototoxic effects did arise. A less pronounced C60 fullerene phototoxic effect was observed after irradiation with green, and no effect was detected with red light. A C60 fullerene photoactivation with violet light induced substantial ROS generation and apoptotic cell death, confirmed by caspase3/7 activation and plasma membrane phosphatidylserine externalization. Our work proved C60 fullerene ability to induce apoptosis of leukemic cells after photoexcitation with high power single chip 405 nm LED as a light source. This underlined the potential for application of C60 nanostructure as a photosensitizer for anticancer therapy. KW - C-60 fullerene KW - photodanamic therapy KW - LEDs KW - leukemic cells KW - immunocytochemistry KW - HPLC-ESI-MS KW - apoptosis Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-228245 VL - 124 ER - TY - JOUR A1 - Mueller, Dolores A1 - Jung, Kathrin A1 - Winter, Manuel A1 - Rogoll, Dorothee A1 - Melcher, Ralph A1 - Kulozik, Ulrich A1 - Schwarz, Karin A1 - Richling, Elke T1 - Encapsulation of anthocyanins from bilberries – Effects on bioavailability and intestinal accessibility in humans JF - Food Chemistry N2 - Anthocyanins are flavonoids that have been suggested to provide beneficial health effects. The biological activity of anthocyanins is influenced by their pharmacokinetic properties, but anthocyanins are associated with limited bioavailability in humans. In the presented study, we investigated how the encapsulation of bilberry extract (BE), a source of anthocyanins, with either whey protein or citrus pectin influences the bioavailability and intestinal accessibility of anthocyanins in humans. We performed an intervention study that analyzed anthocyanins and their degradation products in the urine, plasma, and ileal effluent of healthy volunteers and ileostomists (subjects without an intact colon). We were able to show, that whey protein encapsulation modulated short-term bioavailability and that citrus pectin encapsulation increased intestinal accessibility during passage through the small intestine and modulated the formation of the degradation product phloroglucinol aldehyde (PGAL) in human plasma. KW - anthocyanins KW - encapsulation KW - human intervention KW - bioavailability KW - phloroglucinol aldehyde Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-224247 VL - 248 ER - TY - JOUR A1 - Franke, Barbara A1 - Michelini, Giorgia A1 - Asherson, Philip A1 - Banaschewski, Tobias A1 - Bilbow, Andrea A1 - Buitelaar, Jan K. A1 - Cormand, Bru A1 - Faraone, Stephen V. A1 - Ginsberg, Ylva A1 - Haavik, Jan A1 - Kuntsi, Jonna A1 - Larsson, Henrik A1 - Lesch, Klaus-Peter A1 - Ramos-Quiroga, J. Antoni A1 - Réthelyi, János M. A1 - Ribases, Marta A1 - Reif, Andreas T1 - Live fast, die young? A review on the developmental trajectories of ADHD across the lifespan JF - European Neuropsychopharmacology N2 - Attention-deficit/hyperactivity disorder (ADHD) is highly heritable and the most common neurodevelopmental disorder in childhood. In recent decades, it has been appreciated that in a substantial number of cases the disorder does not remit in puberty, but persists into adulthood. Both in childhood and adulthood, ADHD is characterised by substantial comorbidity including substance use, depression, anxiety, and accidents. However, course and symptoms of the disorder and the comorbidities may fluctuate and change over time, and even age of onset in childhood has recently been questioned. Available evidence to date is poor and largely inconsistent with regard to the predictors of persistence versus remittance. Likewise, the development of comorbid disorders cannot be foreseen early on, hampering preventive measures. These facts call for a lifespan perspective on ADHD from childhood to old age. In this selective review, we summarise current knowledge of the long-term course of ADHD, with an emphasis on clinical symptom and cognitive trajectories, treatment effects over the lifespan, and the development of comorbidities. Also, we summarise current knowledge and important unresolved issues on biological factors underlying different ADHD trajectories. We conclude that a severe lack of knowledge on lifespan aspects in ADHD still exists for nearly every aspect reviewed. We encourage large-scale research efforts to overcome those knowledge gaps through appropriately granular longitudinal studies. KW - developmental trajectory KW - treatment KW - comorbidity KW - cognitive impairment KW - genetics KW - adult-onset ADHD Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-228407 VL - 28 ER - TY - JOUR A1 - Hofrichter, Michaela A. H. A1 - Doll, Julia A1 - Habibi, Haleh A1 - Enayati, Samaneh A1 - Mehrjardi, Mohammad Yahya Vahidi A1 - Müller, Tobias A1 - Dittrich, Marcus A1 - Haaf, Thomas A1 - Vona, Barbara T1 - Exome-wide copy number variation analysis identifies a COL9A1 in frame deletion that is associated with hearing loss JF - European Journal of Medical Genetics N2 - Pathogenic variants in COL9A1 are primarily associated with autosomal recessive Stickler syndrome. Patients with COL9A1-associated Stickler syndrome (STL) present hearing loss (HL), ophthalmic manifestations and skeletal abnormalities. However, the clinical spectrum of patients with COL9A1 variants can also include multiple epiphyseal dysplasia, as well as non-syndromic HL that was observed in one previously reported proband. Exome sequencing was performed on the genomic DNA of an Iranian patient and his affected brother who both report non-syndromic HL. A 44.6 kb homozygous in-frame deletion spanning exons 6 to 33 of COL9A1 was detected via exome-based copy number variation analysis. The deleted exons were confirmed by PCR in the patient and his affected brother, who both have non-syndromic HL. Segregation analysis via qPCR confirmed the parents as heterozygous deletion carriers. Breakpoint analysis mapped the homozygous deletion spanning introns 5 to 33 (g.70,948,188_70,997,277del, NM_001851.4(COL9A1):c.697–3754_2112+769del, p.(Phe233_Ser704del), with an additional 67 bp of inserted intronic sequence that may have originated due to a fork stalling and template switching/microhomology-mediated break-induced replication (FoSTeS/MMBIR) mechanism. This mechanism has not been previously implicated in HL or STL. This is also the first reported copy number variation in COL9A1 that was identified through an exome data set in an Iranian family with apparent non-syndromic HL. The present study emphasizes the importance of exome-wide copy number variation analysis in molecular diagnosis and provides supporting evidence to associate COL9A1 with autosomal recessive non-syndromic HL. KW - COL9A1 KW - copy number variation KW - FoSTeS/MMBIR mechanism KW - non-syndromic hearing loss KW - Stickler syndrome Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-322008 VL - 62 ER - TY - JOUR A1 - Elliot, Perry M. A1 - Germain, Dominique P. A1 - Hilz, Max J. A1 - Spada, Marco A1 - Wanner, Christoph A1 - Falissard, Bruno T1 - Why systematic literature reviews in Fabry disease should include all published evidence JF - European Journal of Medical Genetics N2 - Fabry disease is an X-linked inherited, progressive disorder of lipid metabolism resulting from the deficient activity of the enzyme α-galactosidase. Enzyme replacement therapy (ERT) with recombinant agalsidase, with intravenous infusions of either agalsidase beta or agalsidase alfa, is available and clinical experience now exceeds 15 years. There are very few randomised, placebo-controlled clinical trials evaluating the outcomes of ERT. Data are often derived from observational, registry-based studies and case reports. Pooled analysis of data from different sources may be limited by the heterogeneity of the patient populations, outcomes and treatment. Therefore, comprehensive systematic literature reviews of unpooled data are needed to determine the effects of ERT on disease outcomes. A systematic literature search was conducted in the Embase and PubMed (MEDLINE) databases to retrieve original articles that evaluated outcomes of ERT in patients with Fabry disease; the outcome data were analysed unpooled. The literature analysis included the full range of published literature including observational studies and case series/case reports. Considerable heterogeneity was found among the studies, with differences in sample size, statistical methods, ERT regimens and patient demographic and clinical characteristics. We have demonstrated the value of performing an unpooled systematic literature review of all published evidence of ERT outcomes in Fabry disease, highlighting that in a rare genetic disorder like Fabry disease, which is phenotypically diverse, different patient populations can require different disease management and therapeutic goals depending on age, genotype, and disease severity/level of organ involvement. In addition, these findings are valuable to guide the design and reporting of new clinical studies. KW - Fabry disease KW - enzyme replacement therapy KW - systematic literature review Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-226654 VL - 62 ER - TY - JOUR A1 - Sondermann, Wiebke A1 - Utikal, Jochen Sven A1 - Enk, Alexander H. A1 - Schadendorf, Dirk A1 - Klode, Joachim A1 - Hauschild, Axel A1 - Weichenthal, Michael A1 - French, Lars E. A1 - Berking, Carola A1 - Schilling, Bastian A1 - Haferkamp, Sebastian A1 - Fröhling, Stefan A1 - von Kalle, Christof A1 - Brinker, Titus J. T1 - Prediction of melanoma evolution in melanocytic nevi via artificial intelligence: A call for prospective data JF - European Journal of Cancer N2 - Recent research revealed the superiority of artificial intelligence over dermatologists to diagnose melanoma from images. However, 30–50% of all melanomas and more than half of those in young patients evolve from initially benign lesions. Despite its high relevance for melanoma screening, neither clinicians nor computers are yet able to reliably predict a nevus’ oncologic transformation. The cause of this lies in the static nature of lesion presentation in the current standard of care, both for clinicians and algorithms. The status quo makes it difficult to train algorithms (and clinicians) to precisely assess the likelihood of a benign skin lesion to transform into melanoma. In addition, it inhibits the precision of current algorithms since ‘evolution’ image features may not be part of their decision. The current literature reveals certain types of melanocytic nevi (i.e. ‘spitzoid’ or ‘dysplastic’ nevi) and criteria (i.e. visible vasculature) that, in general, appear to have a higher chance to transform into melanoma. However, owing to the cumulative nature of oncogenic mutations in melanoma, a more fine-grained early morphologic footprint is likely to be detectable by an algorithm. In this perspective article, the concept of melanoma prediction is further explored by the discussion of the evolution of melanoma, the concept for training of such a nevi classifier and the implications of early melanoma prediction for clinical practice. In conclusion, the authors believe that artificial intelligence trained on prospective image data could be transformative for skin cancer diagnostics by (a) predicting melanoma before it occurs (i.e. pre-in situ) and (b) further enhancing the accuracy of current melanoma classifiers. Necessary prospective images for this research are obtained via free mole-monitoring mobile apps. KW - melanoma KW - skin cancer KW - artificial Intelligence KW - deep learning KW - prediction Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-239263 VL - 119 ER - TY - JOUR A1 - Chen, Wei-Hua A1 - Lu, Guanting A1 - Chen, Xiao A1 - Zhao, Xing-Ming A1 - Bork, Peer T1 - OGEE v2: an update of the online gene essentiality database with special focus on differentially essential genes in human cancer cell lines JF - Nucleic Acids Research N2 - OGEE is an Online GEne Essentiality database. To enhance our understanding of the essentiality of genes, in OGEE we collected experimentally tested essential and non-essential genes, as well as associated gene properties known to contribute to gene essentiality. We focus on large-scale experiments, and complement our data with text-mining results. We organized tested genes into data sets according to their sources, and tagged those with variable essentiality statuses across data sets as conditionally essential genes, intending to highlight the complex interplay between gene functions and environments/experimental perturbations. Developments since the last public release include increased number of species and gene essentiality data sets, inclusion of non-coding essential sequences and genes with intermediate essentiality statuses. In addition, we included 16 essentiality data sets from cancer cell lines, corresponding to 9 human cancers; with OGEE, users can easily explore the shared and differentially essential genes within and between cancer types. These genes, especially those derived from cell lines that are similar to tumor samples, could reveal the oncogenic drivers, paralogous gene expression pattern and chromosomal structure of the corresponding cancer types, and can be further screened to identify targets for cancer therapy and/or new drug development. OGEE is freely available at http://ogee.medgenius.info. KW - human cancer cell lines KW - gene essentiality database KW - OGEE v2 Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-181334 VL - 45 IS - D1 ER - TY - JOUR A1 - Garain, Swadhin A1 - Shoyama, Kazutaka A1 - Ginder, Lea-Marleen A1 - Sárosi, Menyhárt A1 - Würthner, Frank T1 - The delayed box: biphenyl bisimide cyclophane, a supramolecular nano-environment for the efficient generation of delayed fluorescence JF - Journal of the American Chemical Society N2 - Activating delayed fluorescence emission in a dilute solution via a non-covalent approach is a formidable challenge. In this report, we propose a strategy for efficient delayed fluorescence generation in dilute solution using a non-covalent approach via supramolecularly engineered cyclophane-based nanoenvironments that provide sufficient binding strength to π-conjugated guests and that can stabilize triplet excitons by reducing vibrational dissipation and lowering the singlet–triplet energy gap for efficient delayed fluorescence emission. Toward this goal, a novel biphenyl bisimide-derived cyclophane is introduced as an electron-deficient and efficient triplet-generating host. Upon encapsulation of various carbazole-derived guests inside the nanocavity of this cyclophane, emissive charge transfer (CT) states close to the triplet energy level of the biphenyl bisimide are generated. The experimental results of host–guest studies manifest high association constants up to 10\(^4\) M\(^{–1}\) as the prerequisite for inclusion complex formation, the generation of emissive CT states, and triplet-state stabilization in a diluted solution state. By means of different carbazole guest molecules, we could realize tunable delayed fluorescence emission in this carbazole-encapsulated biphenyl bisimide cyclophane in methylcyclohexane/carbon tetrachloride solutions with a quantum yield (QY) of up to 15.6%. Crystal structure analyses and solid-state photophysical studies validate the conclusions from our solution studies and provide insights into the delayed fluorescence emission mechanism. KW - aromatic compounds KW - complexation KW - encapsulation KW - fluorescence KW - hydrocarbons Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370385 SN - 0002-7863 VL - 146 IS - 31 ER - TY - JOUR A1 - Brinker, Titus J. A1 - Hekler, Achim A1 - Enk, Alexander H. A1 - Berking, Carola A1 - Haferkamp, Sebastian A1 - Hauschild, Axel A1 - Weichenthal, Michael A1 - Klode, Joachim A1 - Schadendorf, Dirk A1 - Holland-Letz, Tim A1 - von Kalle, Christof A1 - Fröhling, Stefan A1 - Schilling, Bastian A1 - Utikal, Jochen S. T1 - Deep neural networks are superior to dermatologists in melanoma image classification JF - European Journal of Cancer N2 - Background Melanoma is the most dangerous type of skin cancer but is curable if detected early. Recent publications demonstrated that artificial intelligence is capable in classifying images of benign nevi and melanoma with dermatologist-level precision. However, a statistically significant improvement compared with dermatologist classification has not been reported to date. Methods For this comparative study, 4204 biopsy-proven images of melanoma and nevi (1:1) were used for the training of a convolutional neural network (CNN). New techniques of deep learning were integrated. For the experiment, an additional 804 biopsy-proven dermoscopic images of melanoma and nevi (1:1) were randomly presented to dermatologists of nine German university hospitals, who evaluated the quality of each image and stated their recommended treatment (19,296 recommendations in total). Three McNemar's tests comparing the results of the CNN's test runs in terms of sensitivity, specificity and overall correctness were predefined as the main outcomes. Findings The respective sensitivity and specificity of lesion classification by the dermatologists were 67.2% (95% confidence interval [CI]: 62.6%–71.7%) and 62.2% (95% CI: 57.6%–66.9%). In comparison, the trained CNN achieved a higher sensitivity of 82.3% (95% CI: 78.3%–85.7%) and a higher specificity of 77.9% (95% CI: 73.8%–81.8%). The three McNemar's tests in 2 × 2 tables all reached a significance level of p < 0.001. This significance level was sustained for both subgroups. Interpretation For the first time, automated dermoscopic melanoma image classification was shown to be significantly superior to both junior and board-certified dermatologists (p < 0.001). KW - deep learning KW - melanoma KW - skin cancer KW - artificial intelligence Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-220539 VL - 119 ER - TY - JOUR A1 - Brinker, Titus J. A1 - Hekler, Achim A1 - Hauschild, Axel A1 - Berking, Carola A1 - Schilling, Bastian A1 - Enk, Alexander H. A1 - Haferkamp, Sebastian A1 - Karoglan, Ante A1 - von Kalle, Christof A1 - Weichenthal, Michael A1 - Sattler, Elke A1 - Schadendorf, Dirk A1 - Gaiser, Maria R. A1 - Klode, Joachim A1 - Utikal, Jochen S. T1 - Comparing artificial intelligence algorithms to 157 German dermatologists: the melanoma classification benchmark JF - European Journal of Cancer N2 - Background Several recent publications have demonstrated the use of convolutional neural networks to classify images of melanoma at par with board-certified dermatologists. However, the non-availability of a public human benchmark restricts the comparability of the performance of these algorithms and thereby the technical progress in this field. Methods An electronic questionnaire was sent to dermatologists at 12 German university hospitals. Each questionnaire comprised 100 dermoscopic and 100 clinical images (80 nevi images and 20 biopsy-verified melanoma images, each), all open-source. The questionnaire recorded factors such as the years of experience in dermatology, performed skin checks, age, sex and the rank within the university hospital or the status as resident physician. For each image, the dermatologists were asked to provide a management decision (treat/biopsy lesion or reassure the patient). Main outcome measures were sensitivity, specificity and the receiver operating characteristics (ROC). Results Total 157 dermatologists assessed all 100 dermoscopic images with an overall sensitivity of 74.1%, specificity of 60.0% and an ROC of 0.67 (range = 0.538–0.769); 145 dermatologists assessed all 100 clinical images with an overall sensitivity of 89.4%, specificity of 64.4% and an ROC of 0.769 (range = 0.613–0.9). Results between test-sets were significantly different (P < 0.05) confirming the need for a standardised benchmark. Conclusions We present the first public melanoma classification benchmark for both non-dermoscopic and dermoscopic images for comparing artificial intelligence algorithms with diagnostic performance of 145 or 157 dermatologists. Melanoma Classification Benchmark should be considered as a reference standard for white-skinned Western populations in the field of binary algorithmic melanoma classification. KW - benchmark KW - artificial intelligence KW - deep learning KW - melanoma Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-220569 VL - 111 ER - TY - JOUR A1 - Link, Jana A1 - Paouneskou, Dimitra A1 - Velkova, Maria A1 - Daryabeigi, Anahita A1 - Laos, Triin A1 - Labella, Sara A1 - Barroso, Consuelo A1 - Pacheco Piñol, Sarai A1 - Montoya, Alex A1 - Kramer, Holger A1 - Woglar, Alexander A1 - Baudrimont, Antoine A1 - Markert, Sebastian Mathias A1 - Stigloher, Christian A1 - Martinez-Perez, Enrique A1 - Dammermann, Alexander A1 - Alsheimer, Manfred A1 - Zetka, Monique A1 - Jantsch, Verena T1 - Transient and Partial Nuclear Lamina Disruption Promotes Chromosome Movement in Early Meiotic Prophase JF - Developmental Cell N2 - Meiotic chromosome movement is important for the pairwise alignment of homologous chromosomes, which is required for correct chromosome segregation. Movement is driven by cytoplasmic forces, transmitted to chromosome ends by nuclear membrane-spanning proteins. In animal cells, lamins form a prominent scaffold at the nuclear periphery, yet the role lamins play in meiotic chromosome movement is unclear. We show that chromosome movement correlates with reduced lamin association with the nuclear rim, which requires lamin phosphorylation at sites analogous to those that open lamina network crosslinks in mitosis. Failure to remodel the lamina results in delayed meiotic entry, altered chromatin organization, unpaired or interlocked chromosomes, and slowed chromosome movement. The remodeling kinases are delivered to lamins via chromosome ends coupled to the nuclear envelope, potentially enabling crosstalk between the lamina and chromosomal events. Thus, opening the lamina network plays a role in modulating contacts between chromosomes and the nuclear periphery during meiosis. KW - meiosis KW - C. elegans KW - chromosome movement KW - chromosome pairing KW - nuclear envelope KW - lamin Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-236901 VL - 45 ER - TY - JOUR A1 - Tesfamariam, Y. A1 - Jakob, T. A1 - Wöckel, A. A1 - Adams, A. A1 - Weigl, A. A1 - Monsef, I. A1 - Kuhr, K. A1 - Skoetz, N. T1 - Adjuvant bisphosphonates or RANK-ligand inhibitors for patients with breast cancer and bone metastases: A systematic review and network meta-analysis JF - Critical Reviews in Oncology / Hematology N2 - Bone-modifying agents like bisphosphonates and receptor activator of nuclear factor kappaβ ligand (RANK-L) inhibitors are used as supportive treatments in breast cancer patients with bone metastases to prevent skeletal-related events (SREs). Due to missing head-to-head comparisons, a network meta-analysis was performed to provide a hierarchy of these therapeutic options. Through a systematic literature search, 21 randomized controlled trials (RCTs) that fulfilled the inclusion criteria were identified. To prevent SREs, the ranking through P-scores showed denosumab (RR: 0.62; 95%CI: 0.50-0.76), zoledronic acid (RR: 0.72; 95%CI: 0.61-0.84) and pamidronate (RR: 0.76; 95%CI: 0.67-0.85) to be significantly superior to placebo. Due to insufficient or heterogeneous data, overall survival, quality of life, pain response and adverse events were not able to be analyzed within the network. Although data were sparse on adverse events, the risk of significant adverse events appeared low. The results of this review can therefore be used to formulate clinical studies more precisely in order to standardise and focus on patient-relevant outcomes. KW - bisphosphonates KW - RANK-L inhibitors KW - SREs KW - RCTs Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-240827 VL - 137 ER - TY - JOUR A1 - Mooij, Wolf M A1 - van Wijk, Dianneke A1 - Beusen, Arthur HW A1 - Brederveld, Robert J A1 - Chang, Manqi A1 - Cobben, Marleen MP A1 - DeAngelis, Don L A1 - Downing, Andrea S A1 - Green, Pamela A1 - Gsell, Alena S A1 - Huttunen, Inese A1 - Janse, Jan H A1 - Janssen, Annette BG A1 - Hengeveld, Geerten M A1 - Kong, Xiangzhen A1 - Kramer, Lilith A1 - Kuiper, Jan J A1 - Langan, Simon J A1 - Nolet, Bart A A1 - Nuijten, Rascha JM A1 - Strokal, Maryna A1 - Troost, Tineke A A1 - van Dam, Anne A A1 - Teurlincx, Sven T1 - Modeling water quality in the Anthropocene: directions for the next-generation aquatic ecosystem models JF - Current Opinion in Environmental Sustainability N2 - “Everything changes and nothing stands still” (Heraclitus). Here we review three major improvements to freshwater aquatic ecosystem models — and ecological models in general — as water quality scenario analysis tools towards a sustainable future. To tackle the rapid and deeply connected dynamics characteristic of the Anthropocene, we argue for the inclusion of eco-evolutionary, novel ecosystem and social-ecological dynamics. These dynamics arise from adaptive responses in organisms and ecosystems to global environmental change and act at different integration levels and different time scales. We provide reasons and means to incorporate each improvement into aquatic ecosystem models. Throughout this study we refer to Lake Victoria as a microcosm of the evolving novel social-ecological systems of the Anthropocene. The Lake Victoria case clearly shows how interlinked eco-evolutionary, novel ecosystem and social-ecological dynamics are, and demonstrates the need for transdisciplinary research approaches towards global sustainability. Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-224173 VL - 36 ER - TY - JOUR A1 - Kiefer, Markus A1 - Trumpp, Natalie M. A1 - Schaitz, Caroline A1 - Reuss, Heiko A1 - Kunde, Wilfried T1 - Attentional modulation of masked semantic priming by visible and masked task cues JF - Cognition N2 - In contrast to classical theories of cognitive control, recent evidence suggests that cognitive control and unconscious automatic processing influence each other. First, masked semantic priming, an index of unconscious automatic processing, depends on attention to semantics induced by a previously executed task. Second, cognitive control operations (e.g., implementation of task sets indicating how to process a particular stimulus) can be activated by masked task cues, presented outside awareness. In this study, we combined both lines of research. We investigated in three experiments whether induction tasks and presentation of visible or masked task cues, which signal subsequent semantic or perceptual tasks but do not require induction task execution, comparably modulate masked semantic priming. In line with previous research, priming was consistently larger following execution of a semantic rather than a perceptual induction task. However, we observed in experiment 1 (masked letter cues) a reversed priming pattern following task cues (larger priming following cues signaling perceptual tasks) compared to induction tasks. Experiment 2 (visible letter cues) and experiment 3 (visible color cues) showed that this reversed priming pattern depended only on apriori associations between task cues and task elements (task set dominance), but neither on awareness nor on the verbal or non-verbal format of the cues. These results indicate that task cues have the power to modulate subsequent masked semantic priming through attentional mechanisms. Task-set dominance conceivably affects the time course of task set activation and inhibition in response to task cues and thus the direction of their modulatory effects on priming. KW - automatic processes KW - unconscious cognition KW - attentional control KW - semantic priming KW - task cue KW - task switching Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-325751 VL - 187 ER - TY - JOUR A1 - Gerber, Bertram A1 - König, Christian A1 - Fendt, Markus A1 - Andreatta, Marta A1 - Romanos, Marcel A1 - Pauli, Paul A1 - Yarali, Ayse T1 - Timing-dependent valence reversal: a principle of reinforcement processing and its possible implications JF - Current Opinion in Behavioral Sciences N2 - Punishment feels bad, but relief upon its termination feels good. As a consequence of such timing-dependent valence reversal, memories of opposite valence can result from associating stimulus A with, for example, the occurrence of punishment (A-) versus punishment termination (-A): A- training results in aversive memory, but -A training in appetitive memory (corresponding effects exist for reward occurrence and termination). Whereas learning through the occurrence of punishment is well studied, much less is known about learning through its termination. Current research investigates how dopaminergic system function contributes to these processes in Drosophila, rats and humans. We argue that dopamine-related psychopathology may entail distortions in learning through punishment termination, and that this may contribute, for example, to non-suicidal self-injury or post-traumatic stress disorder. Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-232933 VL - 26 ER - TY - JOUR A1 - Colunga, Thomas A1 - Hayworth, Miranda A1 - Kreß, Sebastian A1 - Reynolds, David M. A1 - Chen, Luoman A1 - Nazor, Kristopher L. A1 - Baur, Johannes A1 - Singh, Amar M. A1 - Loring, Jeanne F. A1 - Metzger, Marco A1 - Dalton, Stephen T1 - Human Pluripotent Stem Cell-Derived Multipotent Vascular Progenitors of the Mesothelium Lineage Have Utility in Tissue Engineering and Repair JF - Cell Reports N2 - In this report we describe a human pluripotent stem cell-derived vascular progenitor (MesoT) cell of the mesothelium lineage. MesoT cells are multipotent and generate smooth muscle cells, endothelial cells, and pericytes and self-assemble into vessel-like networks in vitro. MesoT cells transplanted into mechanically damaged neonatal mouse heart migrate into the injured tissue and contribute to nascent coronary vessels in the repair zone. When seeded onto decellularized vascular scaffolds, MesoT cells differentiate into the major vascular lineages and self-assemble into vasculature capable of supporting peripheral blood flow following transplantation. These findings demonstrate in vivo functionality and the potential utility of MesoT cells in vascular engineering applications. KW - stem cells KW - mesothelium KW - vascular progenitor KW - tissue engineering KW - regenerative medicine Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-223217 VL - 26 ER - TY - JOUR A1 - Chhatbar, Chintan A1 - Detje, Claudia N. A1 - Grabski, Elena A1 - Borst, Katharina A1 - Spanier, Julia A1 - Ghita, Luca A1 - Elliott, David A. A1 - Jordão, Marta Joana Costa A1 - Mueller, Nora A1 - Sutton, James A1 - Prajeeth, Chittappen K. A1 - Gudi, Viktoria A1 - Klein, Michael A. A1 - Prinz, Marco A1 - Bradke, Frank A1 - Stangel, Martin A1 - Kalinke, Ulrich T1 - Type I Interferon Receptor Signaling of Neurons and Astrocytes Regulates Microglia Activation during Viral Encephalitis JF - Cell Reports N2 - In sterile neuroinflammation, a pathological role is proposed for microglia, whereas in viral encephalitis, their function is not entirely clear. Many viruses exploit the odorant system and enter the CNS via the olfactory bulb (OB). Upon intranasal vesicular stomatitis virus instillation, we show an accumulation of activated microglia and monocytes in the OB. Depletion of microglia during encephalitis results in enhanced virus spread and increased lethality. Activation, proliferation, and accumulation of microglia are regulated by type I IFN receptor signaling of neurons and astrocytes, but not of microglia. Morphological analysis of myeloid cells shows that type I IFN receptor signaling of neurons has a stronger impact on the activation of myeloid cells than of astrocytes. Thus, in the infected CNS, the cross talk among neurons, astrocytes, and microglia is critical for full microglia activation and protection from lethal encephalitis. KW - encephalitis KW - regulation of microglia activation KW - neurons KW - astrocytes KW - type I IFN receptor signaling Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-222456 VL - 25 ER - TY - JOUR A1 - Kusch, Valentin A1 - Bornschein, Grit A1 - Loreth, Desiree A1 - Bank, Julia A1 - Jordan, Johannes A1 - Baur, David A1 - Watanabe, Masahiko A1 - Kulik, Akos A1 - Heckmann, Manfred A1 - Eilers, Jens A1 - Schmidt, Hartmut T1 - Munc13-3 Is Required for the Developmental Localization of Ca2+ Channels to Active Zones and the Nanopositioning of Cav2.1 Near Release Sensors JF - Cell Reports N2 - Spatial relationships between Cav channels and release sensors at active zones (AZs) are a major determinant of synaptic fidelity. They are regulated developmentally, but the underlying molecular mechanisms are largely unclear. Here, we show that Munc13-3 regulates the density of Cav2.1 and Cav2.2 channels, alters the localization of Cav2.1, and is required for the development of tight, nanodomain coupling at parallel-fiber AZs. We combined EGTA application and Ca2+-channel pharmacology in electrophysiological and two-photon Ca2+ imaging experiments with quantitative freeze-fracture immunoelectron microscopy and mathematical modeling. We found that a normally occurring developmental shift from release being dominated by Ca2+ influx through Cav2.1 and Cav2.2 channels with domain overlap and loose coupling (microdomains) to a nanodomain Cav2.1 to sensor coupling is impaired in Munc13-3-deficient synapses. Thus, at AZs lacking Munc13-3, release remained triggered by Cav2.1 and Cav2.2 microdomains, suggesting a critical role of Munc13-3 in the formation of release sites with calcium channel nanodomains. KW - coupling KW - nanodomain KW - synapse KW - active zone KW - development KW - Ca2+ channels KW - Munc13-3 KW - cerebellar cortex KW - transmitter release Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-233468 VL - 22 ER - TY - JOUR A1 - Becher, Isabelle A1 - Andrés-Pons, Amparo A1 - Romanov, Natalie A1 - Stein, Frank A1 - Schramm, Maike A1 - Baudin, Florence A1 - Helm, Dominic A1 - Kurzawa, Nils A1 - Mateus, André A1 - Mackmull, Marie-Therese A1 - Typas, Athanasios A1 - Müller, Christoph W. A1 - Bork, Peer A1 - Beck, Martin A1 - Savitski, Mikhail M. T1 - Pervasive Protein Thermal Stability Variation during the Cell Cycle JF - Cell N2 - Quantitative mass spectrometry has established proteome-wide regulation of protein abundance and post-translational modifications in various biological processes. Here, we used quantitative mass spectrometry to systematically analyze the thermal stability and solubility of proteins on a proteome-wide scale during the eukaryotic cell cycle. We demonstrate pervasive variation of these biophysical parameters with most changes occurring in mitosis and G1. Various cellular pathways and components vary in thermal stability, such as cell-cycle factors, polymerases, and chromatin remodelers. We demonstrate that protein thermal stability serves as a proxy for enzyme activity, DNA binding, and complex formation in situ. Strikingly, a large cohort of intrinsically disordered and mitotically phosphorylated proteins is stabilized and solubilized in mitosis, suggesting a fundamental remodeling of the biophysical environment of the mitotic cell. Our data represent a rich resource for cell, structural, and systems biologists interested in proteome regulation during biological transitions. KW - thermal proteome profiling KW - cell cycle KW - proteomics Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-221565 VL - 173 ER - TY - JOUR A1 - Fazeli, Gholamreza A1 - Stetter, Maurice A1 - Lisack, Jaime N. A1 - Wehman, Ann M. T1 - C. elegans Blastomeres Clear the Corpse of the Second Polar Body by LC3-Associated Phagocytosis JF - Cell Reports N2 - To understand how undifferentiated pluripotent cells cope with cell corpses, we examined the clearance of polar bodies born during female meiosis. We found that polar bodies lose membrane integrity and expose phosphatidylserine in Caenorhabditis elegans. Polar body signaling recruits engulfment receptors to the plasma membrane of embryonic blastomeres using the PI3K VPS-34, RAB-5 GTPase and the sorting nexin SNX-6. The second polar body is then phagocytosed using receptor-mediated engulfment pathways dependent on the Rac1 ortholog CED-10 but undergoes non-apoptotic programmed cell death independent of engulfment. RAB-7 GTPase is required for lysosome recruitment to the polar body phagosome, while LC3 lipidation is required for degradation of the corpse membrane after lysosome fusion. The polar body phagolysosome vesiculates in an mTOR- and ARL-8-dependent manner, which assists its timely degradation. Thus, we established a genetic model to study clearance by LC3-associated phagocytosis and reveal insights into the mechanisms of phagosome maturation and degradation. KW - cell corpse clearance KW - phagosome maturation KW - LC3-associated phagocytosis KW - lysosomal degradation KW - phagolysosome tubulation KW - polar body KW - non-canonical autophagy KW - non-apoptotic programmed cell death Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-227651 VL - 23 ER - TY - JOUR A1 - Liese, J. G. A1 - Schoen, C. A1 - van der Linden, M. A1 - Lehmann, L. A1 - Goettler, D. A1 - Keller, S. A1 - Maier, A. A1 - Segerer, F. A1 - Rose, M. A. A1 - Streng, A. T1 - Changes in the incidence and bacterial aetiology of paediatric parapneumonic pleural effusions/empyema in Germany, 2010–2017: a nationwide surveillance study JF - Clinical Microbiology and Infection N2 - Objectives Parapneumonic pleural effusions/empyema (PPE/PE) are severe complications of community-acquired pneumonia. We investigated the bacterial aetiology and incidence of paediatric PPE/PE in Germany after the introduction of universal pneumococcal conjugate vaccine (PCV) immunization for infants. Methods Children <18 years of age hospitalized with pneumonia-associated PPE/PE necessitating pleural drainage or persisting >7 days were reported to the German Surveillance Unit for Rare Diseases in Childhood between October 2010 and June 2017. All bacteria detected in blood or pleural fluid (by culture/PCR) were included, with serotyping for Streptococcus pneumoniae. Results The median age of all 1447 PPE/PE patients was 5 years (interquartile range 3–10). In 488 of the 1447 children with PPE/PE (34%), 541 bacteria (>40 species) were detected. Aerobic gram-positive cocci accounted for 469 of 541 bacteria detected (87%); these were most frequently Streptococcus pneumoniae (41%), Streptococcus pyogenes (19%) and Staphylococcus aureus (6%). Serotype 3 accounted for 45% of 78 serotyped S. pneumoniae strains. Annual PPE/PE incidence varied between 14 (95%CI 12–16) and 18 (95%CI 16–21) PPE/PE per million children. Incidence of S. pneumoniae PPE/PE decreased from 3.5 (95%CI 2.5–4.6) per million children in 2010/11 to 1.5 (95%CI 0.9–2.4) in 2013/14 (p 0.002), followed by a re-increase to 2.2 (95%CI 1.5–3.2) by 2016/17 (p 0.205). Conclusions In the era of widespread PCV immunization, cases of paediatric PPE/PE were still caused mainly by S. pneumoniae and, increasingly, by S. pyogenes. The re-increase in the incidence of PPE/PE overall and in S. pneumoniae-associated PPE/PE indicates ongoing changes in the bacterial aetiology and requires further surveillance. KW - pleural empyema KW - pleural fluid KW - parapneumonic pleural effusion KW - Streptococcus pneumoniae KW - Streptococcus pyogenes KW - children Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-236866 VL - 25 ER - TY - JOUR A1 - Eisenhofer, Graeme A1 - Peitzsch, Mirko A1 - Kaden, Denise A1 - Langton, Katharina A1 - Mangelis, Anastasios A1 - Pamporaki, Christina A1 - Masjkur, Jimmy A1 - Geroula, Aikaterini A1 - Kurlbaum, Max A1 - Deutschbein, Timo A1 - Beuschlein, Felix A1 - Prejbisz, Aleksander A1 - Bornstein, Stefan R. A1 - Lenders, Jacques W. M. T1 - Reference intervals for LC-MS/MS measurements of plasma free, urinary free and urinary acid-hydrolyzed deconjugated normetanephrine, metanephrine and methoxytyramine JF - Clinica Chimica Acta N2 - Background Plasma or urinary metanephrines are recommended for screening of pheochromocytomas and paragangliomas (PPGLs). Measurements of urinary free rather than deconjugated metanephrines and additional measurements of methoxytyramine represent other developments. For all measurements there is need for reference intervals. Methods Plasma free, urinary free and urinary deconjugated O-methylated catecholamine metabolites were measured by LC-MS/MS in specimens from 590 hypertensives and normotensives. Reference intervals were optimized using data from 2,056 patients tested for PPGLs. Results Multivariate analyses, correcting for age and body surface area, indicated higher plasma and urinary metanephrine in males than females and sex differences in urinary normetanephrine and free methoxytyramine that largely reflected body size variation. There were positive associations of age with plasma metabolites, but negative relationships with urinary free metanephrine and methoxytyramine. Plasma and urinary normetanephrine were higher in hypertensives than normotensives, but differences were small. Optimization of reference intervals using the data from patients tested for PPGLs indicated that age was the most important consideration for plasma normetanephrine and sex most practical for urinary metabolites. Conclusion This study clarifies impacts of demographic and anthropometric variables on catecholamine metabolites, verifies use of age-specific reference intervals for plasma normetanephrine and establishes sex-specific reference intervals for urinary metabolites. KW - liquid chromatography tandem mass spectrometry (LC-MS/MS) KW - normetanephrine KW - metanephrine KW - methoxytyramine KW - reference intervals KW - age Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-226598 VL - 490 ER - TY - JOUR A1 - Casarotto, Silvia A1 - Turco, Francesco A1 - Comanducci, Angela A1 - Perretti, Alessio A1 - Marotta, Giorgio A1 - Pezzoli, Gianni A1 - Rosanova, Mario A1 - Isaias, Ioannis U. T1 - Excitability of the supplementary motor area in Parkinson's disease depends on subcortical damage JF - Brain Stimulation N2 - Background Cortical dysfunctioning significantly contributes to the pathogenesis of motor symptoms in Parkinson's disease (PD). Objective We aimed at testing whether an acute levodopa administration has measurable and specific cortical effects possibly related to striatal dopaminergic deficit. Methods In thirteen PD patients, we measured the electroencephalographic responses to transcranial magnetic stimulation (TMS/EEG) of the supplementary motor area and superior parietal lobule (n = 8) before and after an acute intake of levodopa. We also performed a single-photon emission computed tomography and [123I]N-ω-fluoropropyl-2β-carbomethoxy-3β-(4-iodophenyl)nortropane to identify the more affected and the less affected brain side in each patient, according to the dopaminergic innervation loss of the putamen. Cortical excitability changes before and after an acute intake of levodopa were computed and compared between the more and the less affected brain side at the single-patient as well as at the group level. Results We found that levodopa intake induces a significant increase (P < 0.01) of cortical excitability nearby the supplementary motor area in the more affected brain side, greater (P < 0.025) than in the less affected brain side. Notably, cortical excitability changes nearby the superior parietal lobule were not statistically significant. Conclusions These results strengthen the idea that dysfunction of specific cortico-subcortical circuits may contribute to pathophysiology of PD symptoms. Most important, they support the use of navigated TMS/EEG as a non-invasive tool to better understand the pathophysiology of PD. KW - transcranial magnetic stimulation KW - electroencephalography KW - levodopa KW - dopamine KW - putamen Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-222261 VL - 12 ER - TY - JOUR A1 - Barkhuizen, Melinda A1 - van Mechelen, Ralph A1 - Vermeer, Marijne A1 - Chedraui, Peter A1 - Paes, Dean A1 - van den Hove, Daniel L. A. A1 - Vaes, Bart A1 - Mays, Robert W. A1 - Steinbusch, Harry W. M. A1 - Robertson, Nicola J. A1 - Kramer, Boris W. A1 - Gavilanes, Antonio W. D. T1 - Systemic multipotent adult progenitor cells improve long-term neurodevelopmental outcomes after preterm hypoxic-ischemic encephalopathy JF - Behavioural Brain Research N2 - There is an urgent need for therapies that could reduce the disease burden of preterm hypoxic-ischemic encephalopathy. Here, we evaluate the long-term effects of multipotent adult progenitor cells (MAPC) on long-term behavioral outcomes in a preterm rat model of perinatal asphyxia. Rats of both sexes were treated with two doses of MAPCs within 24 h after the insult. Locomotor, cognitive and psychiatric impairments were evaluated starting at 1.5 (juvenile) and 6 months (adult). Hypoxia-ischemia affected locomotion, cognition, and anxiety in a sex-dependent manner, with higher vulnerability observed in males. The MAPC therapy partially attenuated deficits in object recognition memory in females of all tested ages, and in the adult males. The hypoxic insult caused delayed hyperactivity in adult males, which was corrected by MAPC therapy. These results suggest that MAPCs may have long-term benefits for neurodevelopmental outcome after preterm birth and global hypoxia-ischemia, which warrants further preclinical exploration. KW - hypoxic-ischemic encephalopathy KW - preterm brain KW - stem cell therapy KW - neurodevelopment Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-221506 VL - 362 ER - TY - JOUR A1 - Stein, Anthony S. A1 - Kantarjian, Hagop A1 - Gökbuget, Nicola A1 - Bargou, Ralf A1 - Litzow, Mark R. A1 - Rambaldi, Alessandro A1 - Ribera, Josep-Maria A1 - Zhang, Alicia A1 - Zimmerman, Zachary A1 - Zugmaier, Gerhard A1 - Topp, Max S. T1 - Blinatumomab for Acute Lymphoblastic Leukemia Relapse after Allogeneic Hematopoietic Stem Cell Transplantation JF - Biology of Blood and Marrow Transplantation N2 - Patients with relapsed/refractory (R/R) acute lymphoblastic leukemia (ALL) following allogeneic hematopoietic stem cell transplantation (alloHSCT) have a poor prognosis, and alternative therapies are needed for this patient population. Blinatumomab, a bispecific T cell engager immunotherapy, was evaluated in an open-label, single-arm, phase II study of adults with R/R Philadelphia chromosome-negative B cell precursor ALL and resulted in a rate of complete remission (CR) or CR with partial hematologic recovery of peripheral blood counts (CRh) of 43% within 2 treatment cycles. We conducted an exploratory analysis to determine the efficacy and safety of blinatumomab in 64 patients who had relapsed following alloHSCT before enrollment in the phase II study. Forty-five percent of the patients (29 of 64) achieved a CR/CRh within the first 2 cycles of treatment, 22 of whom had a minimal residual disease (MRD) response (including 19 with a complete MRD response). After 1 year and 3 years of follow-up, the median relapse-free survival was 7.4 months for patients who achieved CR/CRh in the first 2 cycles, and the median overall survival was 8.5 months; overall survival rate (Kaplan-Meier estimate) was 36% at 1 year and 18% at 3 years. Grade 3 and 4 adverse events were reported in 20 patients (31%) and 28 patients (44%), respectively, with grade 3 and 4 neurologic events in 8 and 2 patients, respectively, and grade 3 cytokine release syndrome in 2 patients. Eight patients had fatal adverse events, including 5 due to infections. Seven patients had grade ≤ 3 graft-versus-host disease during the study, none of which resulted in the discontinuation of blinatumomab or hospitalization. Our data suggest that blinatumomab is an effective salvage therapy in this patient population. KW - blinatumomab KW - Philadelphia chromosome-negative B precursor ALL KW - efficacy KW - safety KW - allogeneic hematopoietic stem cell transplantation Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-239510 VL - 25 ER - TY - JOUR A1 - Gohla, Antje T1 - Do metabolic HAD phosphatases moonlight as protein phosphatases? JF - BBA - Molecular Cell Research N2 - Mammalian haloacid dehalogenase (HAD)-type phosphatases have evolved to dephosphorylate a wide range of small metabolites, but can also target macromolecules such as serine/threonine, tyrosine-, and histidine-phosphorylated proteins. To accomplish these tasks, HAD phosphatases are equipped with cap domains that control access to the active site and provide substrate specificity determinants. A number of capped HAD phosphatases impact protein phosphorylation, although structural data are consistent with small metabolite substrates rather than protein substrates. This review discusses the structures, functions and disease implications of the three closely related, capped HAD phosphatases pyridoxal phosphatase (PDXP or chronophin), phosphoglycolate phosphatase (PGP, also termed AUM or glycerol phosphatase) and phospholysine phosphohistidine inorganic pyrophosphate phosphatase (LHPP or HDHD2B). Evidence in support of small metabolite and protein phosphatase activity is discussed in the context of the diversity of their biological functions. KW - actin cytoskeleton KW - cancer KW - haloacid dehalogenase-type phosphatase KW - major depression KW - metabolism KW - vitamin B6 Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-233168 VL - 1866 ER - TY - JOUR A1 - Jeanclos, Elisabeth A1 - Albersen, Monique A1 - Ramos, Rúben J. J. A1 - Raab, Annette A1 - Wilhelm, Christian A1 - Hommers, Leif A1 - Lesch, Klaus-Peter A1 - Verhoeven-Duif, Nanda M. A1 - Gohla, Antje T1 - Improved cognition, mild anxiety-like behavior and decreased motor performance in pyridoxal phosphatase-deficient mice JF - BBA - Molecular Basis of Disease N2 - Pyridoxal 5′-phosphate (PLP) is an essential cofactor in the catalysis of ~140 different enzymatic reactions. A pharmacological elevation of cellular PLP concentrations is of interest in neuropsychiatric diseases, but whole-body consequences of higher intracellular PLP levels are unknown. To address this question, we have generated mice allowing a conditional ablation of the PLP phosphatase PDXP. Ubiquitous PDXP deletion increased PLP levels in brain, skeletal muscle and red blood cells up to 3-fold compared to control mice, demonstrating that PDXP acts as a major regulator of cellular PLP concentrations in vivo. Neurotransmitter analysis revealed that the concentrations of dopamine, serotonin, epinephrine and glutamate were unchanged in the brains of PDXP knockout mice. However, the levels of γ-aminobutyric acid (GABA) increased by ~20%, demonstrating that elevated PLP levels can drive additional GABA production. Behavioral phenotyping of PDXP knockout mice revealed improved spatial learning and memory, and a mild anxiety-like behavior. Consistent with elevated GABA levels in the brain, PDXP loss in neural cells decreased performance in motor tests, whereas PDXP-deficiency in skeletal muscle increased grip strength. Our findings suggest that PDXP is involved in the fine-tuning of GABA biosynthesis. Pharmacological inhibition of PDXP might correct the excitatory/inhibitory imbalance in some neuropsychiatric diseases. KW - pyridoxal phosphatase KW - vitamin B6 KW - γ-Aminobutyric acid (GABA) KW - motor performance KW - neuropsychiatric diseases KW - neurotransmitter biosynthesis Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-323396 VL - 1865 ER - TY - JOUR A1 - Hochleitner, Gernot A1 - Chen, Fei A1 - Blum, Carina A1 - Dalton, Paul D. A1 - Amsden, Brian A1 - Groll, Jürgen T1 - Melt electrowriting below the critical translation speed to fabricate crimped elastomer scaffolds with non-linear extension behaviour mimicking that of ligaments and tendons JF - Acta Biomaterialia N2 - Abstract Ligaments and tendons are comprised of aligned, crimped collagen fibrils that provide tissue-specific mechanical properties with non-linear extension behaviour, exhibiting low stress at initial strain (toe region behaviour). To approximate this behaviour, we report fibrous scaffolds with sinusoidal patterns by melt electrowriting (MEW) below the critical translation speed (CTS) by exploitation of the natural flow behaviour of the polymer melt. More specifically, we synthesised photopolymerizable poly(L-lactide-co-ε-caprolactone-co-acryloyl carbonate) (p(LLA-co-ε-CL-co-AC)) and poly(ε-caprolactone-co-acryloyl carbonate) (p(ε-CL-co-AC)) by ring-opening polymerization (ROP). Single fibre (fØ = 26.8 ± 1.9 µm) tensile testing revealed a customisable toe region with Young’s Moduli ranging from E = 29 ± 17 MPa for the most crimped structures to E = 314 ± 157 MPa for straight fibres. This toe region extended to scaffolds containing multiple fibres, while the sinusoidal pattern could be influenced by printing speed. The synthesized polymers were cytocompatible and exhibited a tensile strength of σ = 26 ± 7 MPa after 104 cycles of preloading at 10% strain while retaining the distinct toe region commonly observed in native ligaments and tendon tissue. Statement of Significance Damaged tendons and ligaments are serious and frequently occurring injuries worldwide. Recent therapies, including autologous grafts, still have severe disadvantages leading to a demand for synthetic alternatives. Materials envisioned to induce tendon and ligament regeneration should be degradable, cytocompatible and mimic the ultrastructural and mechanical properties of the native tissue. Specifically, we utilised photo-cross-linkable polymers for additive manufacturing (AM) with MEW. In this way, we were able to direct-write cytocompatible fibres of a few micrometres thickness into crimp-structured elastomer scaffolds that mimic the non-linear biomechanical behaviour of tendon and ligament tissue. KW - crimp structure KW - biomimetic scaffolds KW - toe region mechanical behaviour KW - melt electrowriting (MEW) KW - photo-cross-linkable elastomer Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-320846 VL - 72 ER - TY - THES A1 - Zhu, Yan T1 - Small RNA-associated RNA-binding proteins in \(Fusobacterium\) \(nucleatum\) T1 - Kleine RNA-assoziierte RNA-bindende Proteine in \(Fusobacterium\) \(nucleatum\) N2 - Fusobacterium nucleatum is an emerging cancer-associated bacterium belonging to the Fusobacteriota phylum, which is evolutionary distant from all model bacteria. Recent analysis generated global fusobacterial RNA maps, which enabled the discovery of 24 small noncoding RNAs (sRNAs) in F. nucleatum. Notably, the σE-dependent sRNA FoxI and FoxJ act as a posttranscriptional regulator of several cell envelope proteins. The σE-dependent sRNAs in Escherichia coli and Salmonella require the RNA chaperone Hfq for their functions. Intriguingly, F. nucleatum seems to have no homologs of the three common RNA-binding proteins (RBPs) CsrA, Hfq and ProQ. However, it remains unclear if other families of RBPs act in concert with FoxI, FoxJ and other fusobacterial sRNAs. This work has successfully established a 14-mer capture tagged-sRNA affinity purification procedure initially using 6S RNA as a proof-of-concept. Applying this method to 19 different F. nucleatum sRNAs led to a comprehensive mapping of sRNA-binding proteins in this bacterium. This screen identified a total of 75 proteins significantly enriched across all sRNAs and prominent in ribosomal proteins, uncharacterized proteins and enzymes associated with metabolism. This work further focused on the homologs of two KH domain proteins KhpA and KhpB, which were recently recognized as global RBPs in various Gram-positive bacteria such as Streptococcus pneumoniae, Clostridioides difficile, and Enterococcus faecalis. Comparative analyses revealed conserved domain composition and gene synteny of KhpA and KhpB across F. nucleatum, S. pneumoniae, C. difficle and E. faecalis, indicating conserved roles of these proteins in bacteria. Further protein-protein interaction assays and global RNA targets profiling demonstrated that KhpA and KhpB form dimers and act together as broad RBPs, binding to sRNAs, mRNAs and tRNAs in F. nucleatum. Further functional characterizations unveiled that KhpA/B are required for the growth of F. nucleatum under nutrient limitation conditions and impact cell morphology. Additionally, the two RBPs also influence global gene expression in F. nucleatum affecting various bacterial physiological processes, including ethanolamine utilization. In summary, this work established a sRNA-centric approach for screening sRNA-binding proteins in F. nucleatum. Further, the assay could be applied in other non-model organisms and is feasible to screen multiple sRNA baits in parallel for sRNA-interactors. By applying this procedure to nearly all known fusobacterial sRNAs, this work generated an extensive map of sRNA-interacting proteins in F. nucleatum. Molecular and genetic studies identified that KhpA/B act as major RBPs and gene regulators in F. nucleatum, representing important first steps in elucidating key players of post-transcriptional control at the root of the bacterial phylogenetic tree. N2 - Fusobacterium nucleatum ist ein relevantes krebsassoziiertes Bakterium des Phylums Fusobacteriota, welches sich evolutionär von allen anderen Modellbakterien abgrenzt. In einer kürzlich durchgeführten Analyse wurden fusobakterielle RNAs global kartiert, was die Entdeckung von 24 kleinen nichtkodierenden RNAs (sRNAs) in F. nucleatum ermöglichte. Besonders hervorzuheben ist die σE-abhängige sRNAs FoxI und FoxJ, die als posttranskriptioneller Regulator von mehreren Proteine der Zellhülle fungiert. Die σE-abhängigen sRNAs in Escherichia coli und Salmonella benötigen das RNA-Chaperonprotein Hfq für ihre Funktionen. Interessanterweise scheint F. nucleatum aber keine Homologe der drei verbreiteten RNA-Bindeproteine (RBPs) CsrA, Hfq und ProQ zu besitzen. Es bleibt jedoch unklar, ob andere RBP-Familien mit FoxI, FoxJ und sonstigen fusobakteriellen sRNAs interagieren. Diese Arbeit hat erfolgreich ein 14-mer Capture-Markierung basierendes sRNA Affinitätsreinigungsverfahren etabliert, das zunächst unter Verwendung von 6S RNA erprobt wurde. Die Anwendung dieser Methode auf 19 verschiedene sRNAs in F. nucleatum führte zu einer umfassenden Übersicht von sRNA-bindenden Proteinen in diesem Bakterium. Unter allen sRNAs konnten mit Hilfe dieses Screenings insgesamt 75 signifikant angereicherte Proteine identifiziert werden, so vor allem ribosomale Proteine, uncharakterisierte Proteine und Metabolismus-assoziierte Enzyme. Diese Arbeit konzentrierte sich weiterführend auf die Homologe der zwei KH-Domänenproteine KhpA und KhpB, die kürzlich als globale RBPs in verschiedenen Gram-positiven Bakterien, wie Streptococcus pneumoniae, Clostridioides difficile und Enterococcus faecalis beschrieben wurden. Vergleichende Analysen bewiesen eine konservierte Domänenzusammensetzung und Gensyntenie von KhpA und KhpB in F. nucleatum, S. pneumoniae, C. difficile und E. faecalis, was wiederum auf konservierte Funktionen dieser Proteine in Bakterien hinweist. Weitere Protein-Protein-Interaktionsassays und globale Assays zur Identifizierung der Ziel-RNAs zeigten, dass KhpA und KhpB Dimere bilden und gemeinsam als umfangreiche RBPs wirken, die an sRNAs, mRNAs und tRNAs in F. nucleatum binden. Funktionelle Charakterisierungen der Proteine ergaben, dass KhpA/B für das Wachstum von F. nucleatum unter Nährstoffmangel erforderlich sind und die Zellmorphologie beeinflussen. Zusätzlich spielen die beiden RBPs auch eine Rolle in der globalen Genexpression in F. nucleatum und wirken sich auf verschiedene physiologische Prozesse aus, einschließlich der Ethanolamin-Nutzung. Zusammenfassend etablierte diese Arbeit einen sRNA-orientierten Ansatz zur Untersuchung von sRNA-Bindeproteinen in F. nucleatum. Darüber hinaus kann dieser Ansatz potenziell in anderen Nicht-Modellorganismen angewendet werden und eignet sich um mehrere sRNA-Baits parallel auf deren sRNA-Interaktionspartner zu untersuchen. Durch die Anwendung dieses Verfahrens auf nahezu allen bekannten fusobakteriellen sRNAs wurde eine umfangreiche Kartierung der sRNA-Interaktoren in F. nucleatum generiert. Die hier beschriebenen molekularen und genetischen Studien, in welchen KhpA/B als wichtige RBPs und Genregulatoren von F. nucleatum identifiziert wurden, stellen wichtige erste Schritte bei der Aufklärung der Schlüsselakteure der posttranskriptionellen Kontrolle am Ursprung des bakteriellen Stammbaums dar. KW - Fusobacterium nucleatum KW - RNA-binding proteins KW - Small non-coding RNAs KW - Proteine Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370731 ER - TY - JOUR ED - Hesselbach, Robert T1 - Interview mit Prof. Dr. Marina Ortrud Hertrampf JF - promptus - Würzburger Beiträge zur Romanistik N2 - Interview mit Prof. Dr. Marina Ortrud Hertrampf KW - Interview KW - Karriere KW - Wissenschaftlicher Nachwuchs Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370808 SN - 2510-2613 VL - 9 ER - TY - THES A1 - Drakopoulos, Antonios T1 - Opioid receptor oligomerization study through fluorescent selective ligands T1 - Untersuchung der Opioid Rezeptor Oligomerisierung mittels fluoreszierender selektiver Liganden N2 - Opioid receptors (ORs) are among the most intensively studied members of the G protein-coupled receptor (GPCR) family due to their important role in pain management and their involvement in psychological and neurological disorders. However, currently available opioid drugs exhibit both serious drawbacks, such as addiction, and life-threatening side effects, such as respiratory depression. Contrary to the classic monomeric model, indirect evidence suggests that ORs might form dimers, which could be endowed with a distinct pharmacological profile, and, thus, be exploited to develop innovative drugs. However, direct evidence for the spontaneous formation of OR dimers in living cells under physiological condition are missing. The focus of this thesis was the design, synthesis and characterization of new, highly subtype-selective OR fluorescent ligands to be used as tools for state-of-the-art microscopy methods, such as single molecule microscopy (SMM), in heterologous cells and potentially in native tissue, in order to investigate OR organization and mobility on the surface of intact, living cells, at low/physiological expression levels. The μOR is the OR subtype which plays the most critical role in pain modulation, while mediating the effects of the most powerful analgesic drugs. Also, it is the OR subtype which is mostly responsible for the major adverse effects of the currently marketed opioid drugs. We aimed to develop a new μOR-selective fluorescent ligand with a potential irreversible binding mode. Although the approach was in principle successful, i.e. the labelled cells were visible and distinguishable; this initial attempt was not suitable for SMM due to the ligands’ poor selectivity and affinity as well as due to its high background noise. A second generation of the fluorescent ligand was designed; however the synthesis and characterization are part of another doctoral thesis. Lately, δOR has received attention as a promising drug target, due to its distinct pharmacological profile which features low abuse liability and lack of physical dependence. In addition, δOR expression has been associated with cancer regulation in the periphery, thus further highlighting the interest of imaging tools for this receptor. In this thesis, the development and characterization of two new δOR-selective fluorescent probes with excellent optical properties, based on the well-studied ligand naltrindole (NTI) is presented. Their application in SMM studies is currently underway at the group of Prof. Dr. Davide Calebiro at the University of Birmingham. The κOR is a subtype which has also emerged as a drug target due to its low abuse potential. Despite a growing interest in this receptor, κOR-selective fluorescent probes have been particularly scarce in literature. Herein, the design, synthesis and characterization of the first reported set of fluorescent κOR-selective probes with antagonistic properties, based on the established ligand 5’-guanidinonaltrindole (5’-GNTI) is presented. Two of these were employed for SMM experiments to investigate κOR homodimerization, localization and trafficking. Our findings do not support homodimerization of the κOR-bound probe complexes, while showing that the majority of them follow a normal Brownian diffusion on the cell surface. N2 - Opioid-Rezeptoren (OR) gehören aufgrund ihrer wesentlichen Rolle bei der Schmerztherapie und ihrer Beteiligung an physiologischen und neurologischen Störungen zu den am intensivsten untersuchten Mitgliedern der G-Protein-gekoppelten Rezeptor (GPCR) Familie. Jedoch haben aktuell erhältliche Opioid-Arzneimittel schwerwiegende Nachteile, wie Abhängigkeit, und lebensbedrohliche Nebenwirkungen, wie Atemdepression. Im Gegensatz zu dem klassischen Monomer-Modell legen indirekte Hinweise nahe, dass ORs Dimere formen können, welche mit einem spezifischen pharmakologischen Profil ausgestattet sein könnten und daher für die Entwicklung innovativer Arzneimittel verwendet werden könnten. Jedoch gibt es keinen direkten Beweis für die spontane Bildung von OR-Dimeren in lebenden Zellen unter physiologischen Bedingungen. Der Fokus dieser Doktorarbeit war daher das Design, die Synthese und Charakterisierung von neuen hoch subtyp-selektiven fluoreszierenden OR Liganden, welche als Hilfsmittel für hochmoderne Mikroskopie-Anwendungen Anwendung finden sollen, wie Einzelmolekül-Mikroskopie (EMM) in heterologen Zellen und potentiell in nativem Gewebe, um OR-Organisierung und Mobilität auf der Oberfläche von intakten lebenden Zellen bei niedrigen/physiologischen Expressions-Spiegeln zu untersuchen. Der μOR ist der OR Subtyp, der die entscheidenste Rolle bei der Schmerzmodulierung spielt, indem er die Wirkung der stärksten analgetischen Arzneien vermittelt. Des Weiteren ist dieser OR-Subtyp der Subtyp, der größtenteils für die wesentlichen unerwünschten Nebenwirkungen der aktuell vermarkteten Opioid-Arzneimittel verantwortlich ist. Das Ziel dieser Arbeit war daher, einen neuen μOR-selektiven fluoreszierenden Liganden mit einem potentiell irreversiblen Bindungsmodus zu entwickeln. Obwohl dieser Ansatz prinzipiell erfolgreich war, das heißt die markierten Zellen waren sicht- und unterscheidbar, war dieser erste Ansatz aufgrund der geringen Selektivität und Affinität des Liganden und aufgrund seines hohen Hintergrundrauschens nicht für EMM geeignet. Daher wurde eine zweite Generation fluoreszierender Liganden entworfen. Deren Synthese und Charakterisierung ist jedoch Teil einer anderen Doktorarbeit. Kürzlich erhielt der δOR aufgrund seines spezifischen pharmakologischen Profils, welches ein geringes Missbrauchsrisiko und das Fehlen körperlicher Abhängigkeit beinhaltet, vielseitige Beachtung als ein vielversprechendes Arznei-Target. Des Weiteren wurde δOR-Expression mit Krebsregulation in der Peripherie assoziiert, was das Interesse an einem bildgebenden Werkzeug für diesen Rezeptor zusätzlich unterstreicht. In dieser Doktorarbeit wird die Entwicklung und Charakterisierung von zwei neuen, auf dem gut untersuchten Liganden Naltrindol (NTI) basierenden, δOR-selektiven fluoreszierenden Sonden mit sehr guten optischen Eigenschaften gezeigt. Ihre Anwendung in EMM Untersuchungen läuft derzeit bei Kooperationspartnern im Arbeitskreis von Professor Davide Calebiro an der Universität Birmingham an. Der κOR ist der Subtyp, der auch als Arznei-Target aufgrund seines geringen Missbrauchspotentials in Erscheinung getreten ist. Obwohl steigendes Interesse an diesem Rezeptor besteht, sind κOR-selektive fluoreszierende Sonden in der Literatur bisher kaum beschrieben. In dieser Arbeit wird das Design, die Synthese und Charakterisierung des ersten beschriebenen Sets von fluoreszierenden κOR-selektiven Sonden mit antagonistischen Eigenschaften, basierend auf dem Liganden 5’-Guanidinonaltrindol (5’-GNTI) gezeigt. Zwei dieser Liganden wurden für EMM Experimente verwendet, um die κOR Homodimerisierung, Lokalisation und Transportwege zu untersuchen. Unsere Ergebnisse zeigen keine Homodimerisierung des κOR-gebundenen Sondenkomplexes und außerdem, dass die Mehrheit der Rezeptoren einer normalen Brown’schen Diffusion auf der Zelloberfläche folgt. KW - Opioidrezeptor KW - fluorescent ligands KW - opioid receptors KW - TIRF microscopy KW - GPCR oligomerization KW - Oligomerisation KW - Ligand KW - Fluoreszierende Liganden KW - GPCR Oligomerisierung Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-207179 ER - TY - THES A1 - Döhler, Ida T1 - Reduktion von Blutungskomplikationen bei Patientinnen und Patienten mit oraler Antikoagulation in der elektiven Allgemein- und Viszeralchirurgie durch individuelles Risiko-adjustiertes Bridging T1 - Reduction of bleeding complications in patients on oral anticoagulation in elective general and visceral surgery by individual risk-adjusted bridging N2 - Zahlreiche Studien zeigten, dass perioperatives Bridging der oralen Antikoagulation zu einem erhöhten Blutungsrisiko führt. Ursache hierfür könnte eine zu aggressive Herangehensweise bezüglich der Dosierung des Bridgings sein. Daher war das Ziel dieser Arbeit herauszufinden, ob ein Risiko-adjustiertes Bridging-Schema in der elektiven Allgemein- und Viszeralchirurgie zu einem geringeren Auftreten von postoperativen Blutungsereignissen führt und ob trotzdem ein adäquater Schutz vor thromboembolischen Ereignissen gegeben ist. Hierfür wurde retrospektiv und monozentrisch das Auftreten der genannten postoperativen Ereignisse in zwei Zeiträumen untersucht. Das erste Studienintervall erstreckte sich von Januar 2011 bis Dezember 2014 und spiegelt die Ereignisraten vor der internen Leitlinienänderung wider. Es wurden 263 Personen eingeschlossen. Das zweite Intervall begann im Januar 2017 und endete im Dezember 2019, in diesem wurden 271 Personen untersucht. Zwischen diesen beiden Zeiträumen wurde eine überarbeitete klinikinterne Bridging-Leitlinie etabliert, welche an das individuelle thromboembolische Risiko, Alter, Gewicht und die Nierenfunktion der Patientinnen und Patienten angepasst war. Postoperative Major- (8.4% vs. 4.1%, p=0.039) und Minor-Blutungen (13.7% vs. 6.3%, p=0.004) nahmen im zweiten Intervall signifikant ab, während das thromboembolische Risiko weiterhin niedrig blieb (0.8% vs. 1.1%, p=1). Außerdem zeigte sich, dass es zu keiner signifikanten Zunahme der Mortalität, der Reoperationen, der Länge des postoperativen stationären Aufenthalts oder der Erythrozytenkonzentrat-Transfusionen kam. Die Ergebnisse dieser Arbeit zeigen, dass die differenzierte Bridging-Leitlinie für die Allgemein- und Viszeralchirurgie mit einer signifikant erniedrigten Blutungsrate assoziiert ist und eine Anpassung des Bridgings an die patientenspezifischen Risikofaktoren wichtig ist. N2 - Multiple studies have shown that perioperative bridging of oral anticoagulation leads to an increased risk of bleeding. This could be due to an overly aggressive approach to bridging dosing. Therefore, the aim of this study was to find out whether a risk-adjusted bridging regimen in elective general and visceral surgery leads to a lower incidence of postoperative bleeding events and whether adequate protection against thromboembolic events is still provided. For this purpose, the occurrence of the aforementioned postoperative events was examined retrospectively and monocentrically in two time periods. The first study interval extended from January 2011 to December 2014 and reflects the event rates before the internal guideline change. 263 people were included. The second interval began in January 2017 and ended in December 2019, in which 271 people were examined. Between these two periods, a revised internal clinical bridging guideline was established, which was adapted to the individual thromboembolic risk, age, weight and renal function of the patients. Postoperative major (8.4% vs. 4.1%, p=0.039) and minor bleeding complications (13.7% vs. 6.3%, p=0.004) decreased significantly in the second interval, while the thromboembolic risk remained low (0.8% vs. 1.1%, p=1). In addition, there was no significant increase in mortality, reoperations, length of postoperative hospital stay or red blood cell transfusions. The results of this study show that the differentiated bridging guideline for general and visceral surgery is associated with a significantly lower bleeding rate and that it is important to adapt bridging to patient-specific risk factors. KW - Heparin KW - Blutung KW - Chirurgie KW - Perioperatives Bridging KW - Risikoadjustiertes Bridging KW - Blutungskomplikationen KW - Allgemein-/Viszeralchirurgie Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370639 ER - TY - THES A1 - Polzin, Charlotte T1 - Entwicklung eines Screeningverfahrens für Linezolid-resistente Enterokokken und Aufnahme der Prävalenz T1 - Development of a screening method for linezolid-resistant enterococci and determination of prevalence N2 - Enterokokken gehören zu den bedeutendsten nosokomialen Keimen. Die Verbreitung von Multiresistenzen bei diesen Keimen stellt das deutsche Gesundheitssystem aufgrund von wenigen verbleibenden Therapieoptionen von Infektionen vor große Probleme. Die KRINKO des Robert-Koch-Instituts empfiehlt als mögliche Präventionsmaßnahme ein regelmäßiges Screening auf Enterokokken mit Vancomycin- bzw. Linezolid-Resistenzen. Ziel dieser Arbeit war es, ein kulturelles Screeningverfahren für Linezolid-resistente Enterokokken (LRE) zu entwickeln und dieses anschließend im Routinescreening des Universitätsklinikums Würzburg zu etablieren. Es wurde ein Verfahren entwickelt, welches sich aus einem Anreicherungsschritt mit 3 mg/l Linezolid versetzter selektiver Enterococcosel-Bouillon und einer anschließenden Subkultivierung auf Linezolid-Enterococcosel-Agar mit 4 mg/l Linezolid zusammensetzt. In einer Simulation von klinischen Bedingungen zeigte sich eine gute Sensitivität und Spezifität. Das entwickelte Screeningverfahren wurde mit einem geringen Sensitivitätsverlust und ohne zusätzliche Belastung für die Patienten in das bestehende Routinescreening für Vancomycin-resistente Enterokokken des Universitätsklinikums Würzburg eingegliedert. Die nachgewiesen LRE zeigten unterschiedliche Resistenzmechanismen, wobei bei dem Großteil der Isolate Resistenzgene nachgewiesen werden konnten. Des Weiteren zeigte sich ein breit gestreuter genetischer Hintergrund. Viele der Isolate gehörten genetischen Gruppen an, welche bisher kaum in hospitalisierten Patienten nachgewiesen wurden. Durch die labortechnische Weiterentwicklung von Screeningverfahren für LRE können diese möglicherweise bald routinemäßig in vielen Kliniken etabliert werden. N2 - Enterococci are one of the most important nosocomial pathogens. The spread of multiresistance in these pathogens poses a major problem for the German healthcare system due to the few remaining treatment options for infections. The Robert Koch Institute's KRINKO recommends regular screening for enterococci with vancomycin or linezolid resistance as a possible preventive measure. The aim of this work was to develop a cultural screening method for linezolid-resistant enterococci (LRE) and to establish it in routine screening at the University Hospital of Würzburg. A procedure was developed consisting of an enrichment step with 3 mg/l linezolid-added selective enterococcosel broth and a subsequent subcultivation on linezolid-enterococcosel agar with 4 mg/l linezolid. A simulation of clinical conditions showed good sensitivity and specificity. The developed screening method was integrated into the existing routine screening for vancomycin-resistant enterococci at the University Hospital of Würzburg with little loss of sensitivity and no additional burden for patients. The detected LRE showed different resistance mechanisms, with resistance genes being detected in the majority of isolates. In addition, a broad genetic background was found. Many of the isolates belonged to genetic groups that have rarely been detected in hospitalized patients. With further development of laboratory screening methods for LRE, it may soon be possible to establish them routinely in many hospitals. KW - Enterococcus KW - Linezolid KW - Multidrug-Resistenz KW - Linezolid-resistente Enterokokken KW - linezolid-resistant enterococci KW - Screeningverfahren KW - screening method KW - Screening Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370665 ER - TY - THES A1 - Engelbrecht, Elisabeth T1 - Retrospektive Auswertung des Therapieerfolges einer PTCD-Anlage bei Insuffizienz der Pankreatojejunostomie nach Pankreaskopfresektionen T1 - Retrospective evaluation of effective treatment of biliopancreatic fistulas due to leakage of the pancreatojejunostomy after pancreatic head resection by transhepatic biliary drainage N2 - Trotz stetiger Weiterentwicklung und Verbesserungen in chirurgischen Anastomosetechniken treten postoperative Pankreasfisteln (POPF) in 20 - 25 % der Patienten und Patientinnen als Komplikation nach partieller Pankreatikoduodenektomie (PPD) auf. Kommt es zu einer kombinierten Leckage aus Gallen- und Pankreassekret, wurde in dieser Arbeit die Definition einer komplizierten POPF (CPPF) eingeführt, welche eine seltene, aber schwerwiegende und gefährliche postoperative Komplikation darstellt. Neben einer Relaparotomie kann eine Restpankreatektomie als ultima ratio zur Beherrschung dieser schweren Komplikation notwendig werden, welche mit einer Mortalität von 50 % verbunden ist. Die Internationale Studiengruppe der Pankreaschirurgie (ISGPS) entwickelte ein Klassifikationssystem für POPF, welches auf Abweichungen der üblichen postoperativen Behandlungsstrategie beruht. Jedoch wurden keine spezifischen Behandlungsalgorithmen bzw. Therapiekonzepte, insbesondere im Falle einer CPPF, vorgeschlagen. In dieser Arbeit soll die therapeutische Effektivität einer perkutanen transhepatischen Cholangiodrainage (PTCD) bei Patienten und Patientinnen mit einer CPPF evaluiert werden. Dazu wurde eine retrospektive Analyse an Patienten und Patientinnen durchgeführt, welche eine CPPF nach PPD entwickelten. Die Patienten und Patientinnen wurden hinsichtlich der gewählten Behandlungsstrategie, des Outcomes, postoperativer Komplikationen nach Clavien-Dindo-Klassifikation, des CCI (Comprehensive Complication Index), der 30- und 90-Tage-Mortalität sowie Restpankreatektomie, postoperativer Arrosionsblutungen und der Hospitalisierungsdauer nach Behandlung einer CPPF analysiert. Zwischen 2007 und 2018 entwickelten 56 (19,1 %) von insgesamt 293 Patienten und Patientinnen eine relevante POPF (ISGPS Grad B/C) nach einer Pankreaskopfresektion. Darunter wurden 17 Patienten und Patientinnen mit einer komplizierten POPF (CPPF) identifiziert. 11 Patienten und Patientinnen erhielten als Behandlung eine PTCD und sechs Patienten und Patientinnen erhielten eine chirurgisch eingebrachte transhepatische Cholangiodrainage (CTCD) im Rahmen eines Revisionseingriffes. Es wurde keine Restpankreatektomie oder Reoperation nach einer initialen PTCD Therapie notwendig. In 4 von 17 Fällen kam es zu postoperativen Blutungen nach Einbringen einer transhepatischen Cholangiodrainage, der mediane CCI lag bei 44 ± 17,3, die mediane Hospitalisierungsdauer betrug 36 ± 19,2 Tage, die 30-Tage-Mortalität war 0 % und die 90-Tage-Mortalität 17,7 %. Es wurde kein Sterbefall in Verbindung mit einer PTCD beobachtet. Mit Hilfe dieser Studie kann gezeigt werden, dass eine PTCD eine praktikable, sichere und effektive Behandlungsoption für Patienten und Patientinnen mit einer CPPF bietet. Die Separierung von Galle und Pankreassaft stellt eine neuartige Behandlungsoption in ausgewählten Patienten und Patientinnen mit ausreichend drainierter CPPF nach PPD dar. N2 - Despite continuous advancements and improvements in surgical anastomosis techniques, postoperative pancreatic fistulas (POPF) occur as complications in 20-25 % of patients after partial pancreaticoduodenectomy (PPD). In cases of combined leakage of bile and pancreatic secretions, this work introduces the definition of a complicated POPF (CPPF), which is a rare but severe and dangerous postoperative complication. Besides a relaparotomy, a remaining pancreatectomy may be necessary as a last resort to control this severe complication, which is associated with a mortality rate of 50 %. The International Study Group of Pancreatic Surgery (ISGPS) developed a classification system for POPF based on deviations from the usual postoperative treatment strategy. However, no specific treatment algorithms or therapeutic concepts, especially in the case of a CPPF, have been proposed. This study aims to evaluate the therapeutic effectiveness of percutaneous transhepatic biliary drainage (PTCD) in patients with a CPPF. For this purpose, a retrospective analysis was conducted on patients who developed a CPPF after PPD. The patients were analyzed regarding the chosen treatment strategy, outcome, postoperative complications according to the Clavien-Dindo classification, the Comprehensive Complication Index (CCI), the 30- and 90-day mortality rates, as well as remaining pancreatectomy, postoperative erosive bleeding and hospitalization duration after treatment of a CPPF. Between 2007 and 2018, 56 (19.1%) out of a total of 293 patients developed a relevant POPF (ISGPS Grade B/C) after pancreatic head resection. Among them, 17 patients with a complicated POPF (CPPF) were identified. Eleven patients received PTCD as treatment, and six patients received surgically placed transhepatic biliary drainage (CTCD) as part of a revision procedure. No remaining pancreatectomy or reoperation was necessary after initial PTCD therapy. In 4 out of 17 cases, postoperative bleeding occurred after the introduction of a transhepatic biliary drainage; the median CCI was 44 ± 17.3, the median hospitalization duration was 36 ± 19.2 days, the 30-day mortality was 0%, and the 90-day mortality was 17.7%. No deaths associated with PTCD were observed. This study demonstrates that PTCD offers a feasible, safe and effective treatment option for patients with a CPPF. The separation of bile and pancreatic juice presents an innovative treatment option in selected patients with adequately drained CPPF after PPD. KW - Bauchspeicheldrüsenkrebs KW - Postoperative Komplikation KW - Pankreasfistel KW - PTCD KW - postoperative Pankreasfistel KW - Anastomoseninsuffizienz Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370395 ER - TY - THES A1 - Korte, Pamela T1 - Die funktionelle Bedeutung des Lipidstoffwechsels für die Stomataöffnung bei Hitzestress in \(Arabidopsis\) \(thaliana\) T1 - The functional significance of lipid metabolism for stomatal opening during heat stress in \(Arabidopsis\) \(thaliana\) N2 - Pflanzen sind verschiedenen Umweltbedingungen ausgesetzt, die zu suboptimalen Wachstumsbedingungen führen können. Dies gilt für eine Vielzahl von biotischen und abiotischen Faktoren. In der hier vorgelegten Arbeit wird der Effekt von erhöhten Temperaturen und Hitze genauer analysiert. Hitze ist einer der wichtigsten abiotischen Stressfaktoren, der das Pflanzenwachstum und die Reproduktion beeinflusst. Viele wichtige Kulturpflanzen zeigen immense Ertragseinbußen, die durch Hitze hervorgerufen werden. Durch den fortschreitenden Klimawandel werden jedoch Hitzeperioden immer häufiger und somit die Folgen für die Nahrungsproduktion immer gravierender. Zur Züchtung von Pflanzen die hitzetolerant sind und weniger hohe Ertragseinbußen unter diesem Stress aufweisen, ist es essenziell die grundlegenden molekularen Mechanismen der Hitzetoleranz zu verstehen. Es müssen die verschiedenen physiologischen und biochemischen Prozesse identifiziert werden, die es Pflanzen ermöglichen, sich anzupassen. Es ist bekannt, dass die Anpassungsmechanismen von Pflanzen komplex sind und sowohl Veränderungen auf zellulärer wie auch auf organismischer Ebene beinhalten. Ziel dieser Arbeit war es, weitere Erkenntnisse zu gewinnen, wie diese Anpassung vonstattengeht und welche molekularen Prozesse an ihr beteiligt sind. Ein Hauptaugenmerk lag dabei auf dem Einfluss des Lipidmetabolismus und den daran beteiligten Enzymen. Es konnte bereits gezeigt werden, dass die Akkumulation von Triacylglycerolen bei hohen Temperaturen die basale Thermotoleranz bei Arabidopsis thaliana erhöht. Wie jedoch der genaue Mechanismus dieser durch Triacylglycerole vermittelten Thermotoleranz funktioniert, war bis dato nicht bekannt. Ich konnte zeigen, dass die angesammelten Triacylglycerole genutzt werden können, um die Stomata während des Hitzestress zu öffnen. Dies führt zu einer erhöhten Transpiration und somit einer Kühlung der Blätter. Der Abbau von Triacylglycerolen und Stärke am Morgen ist notwendig, um die Stomata zu öffnen. Zusätzlich dient der Abbau der Aufrechterhaltung des Citratzyklus und somit der Energieversorgung. In weiteren Experimenten konnte ich durch Fütterung mit stabil markierter Laurinsäure zeigen, dass die Triacylglycerole auch dem Aufbau neuer Aminosäuren unter Stressbedingungen dienen. Die hier vorgestellten Arbeiten bieten die Grundlage, um den Mechanismus der Thermotoleranz besser zu verstehen. Das Verständnis der in dieser Arbeit beschriebenen molekularen Signalwege und Enzyme kann langfristig dazu beitragen hitzeresistentere Nutzpflanzen zu züchten. N2 - Plants are exposed to various environmental conditions that can lead to suboptimal growth conditions. This applies to a variety of biotic and abiotic factors. In the work presented here, the effect of elevated temperatures and heat is analyzed in more detail. Heat is one of the most important abiotic stress factors affecting plant growth and reproduction. Many important crops show immense yield losses caused by heat. However, as climate change progresses, periods of heat are becoming more frequent and the consequences for food production are becoming increasingly serious. Understanding the basic molecular mechanisms of heat tolerance is essential to breed plants that are heat tolerant and show less yield loss under this stress. The various physiological and biochemical processes that enable plants to adapt need to be identified. It is known that the adaptation mechanisms of plants are complex and involve changes at both the cellular and organismal level. The aim of this work was to gain further insights into how this adaptation takes place and which molecular processes are involved. The main focus was on the influence of lipid metabolism and the enzymes involved. It has already been shown that the accumulation of triacylglycerols at high temperatures increases basal thermotolerance in Arabidopsis thaliana. However, the exact mechanism of this triacylglycerol mediated thermotolerance was not known until now. I was able to show that the accumulated triacylglycerols can be used to open the stomata during heat stress. This leads to increased transpiration and thus cooling of the leaves. The degradation of triacylglycerols and starch in the morning is necessary to open the stomata. In addition, the degradation serves to maintain the citrate cycle and thus the energy supply. In further experiments, I was able to show by feeding stably labeled lauric acid that the triacylglycerols also serve to build up new amino acids under stress conditions. The work presented here provides the basis for a better understanding of the mechanism of thermotolerance. Understanding the molecular signaling pathways and enzymes described in this work could - in the long term - contribute to breeding of more heat-resistant crops. KW - Hitzestress KW - Ackerschmalwand KW - Arabidopsis thaliana KW - Triacylglycerol Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370461 ER - TY - THES A1 - Danner, Elisabeth T1 - Systolische Ejektionszeit - Referenzwerte und Einfluss kardiovaskulärer Risikofaktoren in einer populationsbasierten Kohortenstudie T1 - Systolic ejection time - Reference values and impact of cardiovascular risk factors in a population-based cohort study N2 - Die systolische Ejektionszeit (SET) und die prä-Ejektionszeit (pET) sind Zeitintervalle, die sich zuverlässig mittels transthorakaler Echokardiographie erheben lassen und wichtige Aspekte in der kardialen Leistungsdiagnostik abbilden. Gleichwohl gibt es bislang für diese systolischen Zeitintervalle keine Normwerte. Die vorliegende Arbeit analysierte echokardiographische Daten von 4965 ProbandInnen der STAAB-Studie, einer umfänglich phänotypisierten populationsbasierten Kohortenstudie mit dem Ziel der Erstellung von Normwerten für die systolischen Zeitintervalle sowie der Identifizierung und Quantifizierung ihrer Determinanten mittels multivariable Regressionsanalysen. Aufgrund der starken Abhängigkeit der SET von der Herzfrequenz wurde die herzfrequenzkorrigierte SETc eingeführt, die in Anlehnung an die QTc-Zeit nach Fridericia berechnet wurde ("SET" /∛("RR-Intervall" )). Die Normwerte wurden anhand der gesunden Untergruppe (definiert durch Abwesenheit von kardiovaskulären Risikofaktoren oder Erkrankungen; N=966) aus STAAB generiert. Dem starken Einfluss von Geschlecht und Alter wurde dabei Rechnung getragen, indem für SET, SETc und pET alters- und geschlechtsspezifische Referenzwerte berechnet wurden. SETc war stark korreliert mit linksventrikulärer Ejektionsfraktion sowie enddiastolischem Volumen und Schlagvolumen. Zudem zeigte sich ein deutlicher Zusammenhang von SETc mit spezifischen Markern der Nachlast (Ea und Ees). Aus der großen Liste der klinischen Marker, die in STAAB erhoben wurden, ergab sich eine größere Anzahl von Einflussfaktoren. Bedeutsame Determinanten der systolischen Zeitintervalle waren insbesondere das metabolische Syndrom (sowie dessen Komponenten), das Rauchverhalten und die Einnahme von β Blockern. Die Ergebnisse zeigen, dass die systolischen Zeitintervalle, insbesondere SETc, reliable Informationen über das kardiale Kontraktionsverhalten liefern können. Derzeit werden neue Substanzklassen untersucht, die unter anderem über die Modifizierung von SET wirken sollen. Hier zu nennen sind insbesondere Myosin-Aktivatoren bei Herzinsuffizienz mit reduzierter Pumpfunktion wie zum Beispiel Omecamtiv Mecarbil oder Myosin-Inhibitoren bei Hypertropher Obstruktiver Kardiomyopathie. Die hierzu laufenden Studien betrachten auch die Effekte dieser Medikamente auf die systolischen Zeitintervalle als bedeutsame Surrogate der klinischen Effekte und letztlich der Prognose. Die nun vorliegenden Normwerte dieser Zeitintervalle erlauben es, die pathologisch veränderten Werte bei diesen spezifischen Krankheitsbildern und klinischen Studien besser einzuordnen und zu verstehen. N2 - The systolic ejection time (SET) and the pre-ejection time (pET) are time intervals that can be reliably recorded using transthoracic echocardiography and represent important aspects in cardiac performance diagnostics. However, there are currently no standard values for these systolic time intervals. The present research paper analyzed echocardiographic data from 4965 subjects from the STAAB study, a comprehensively characterized population-based cohort study with the aim of establishing standard values for the systolic time intervals and identifying and quantifying their determinants using multivariable regression analyses. Due to the strong dependency of SET on heart rate, the heart rate-corrected SETc was introduced which was calculated based on the QTc-time according to Fridericia ("SET" /∛("RR-Intervall" )). The standard values were generated from the STAAB study based on the healthy subgroup (defined by the absence of cardiovascular risk factors or diseases; N=966). Regarding the strong influence of gender and age, specific reference values for SET, SETc and pET implying gender and age affection were calculated. SETc was strongly correlated with left ventricular ejection fraction as well as end-diastolic volume and stroke volume. In addition, there was a notable correlation between SETc and specific markers of afterload (Ea and Ees). The large list of clinical markers collected in STAAB resulted in a number of affecting factors. Significant determinants of the systolic time intervals were in particular the metabolic syndrome (and its components), smoking behavior and the use of β-blockers. The results show that the systolic time intervals, especially SETc, can provide reliable information about cardiac contraction. New classes of substances are currently being investigated, which are supposed to work, among other things, by modifying SET. In particular, myosin activators in heart failure with reduced ejection fraction such as Omecamtiv Mecarbil or myosin inhibitors in hypertrophic obstructive cardiomyopathy should be mentioned here. The current studies also consider the effects of these drugs on the systolic time intervals as important surrogates of the clinical effects and the prognosis. The standard values for these time intervals enable better classifiying and unterstanding pathologically changed values in these specific disease pattern and clinical studies. KW - Referenzwert KW - Herzinsuffizienz KW - Risikofaktor KW - Systolische Ejektionszeit KW - kardiovaskuläre Risikofaktoren Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370480 ER - TY - THES A1 - Dusel, Marco T1 - Exziton-Polariton-Kondensation in organischen Halbleiter-Mikrokavitäten mit hemisphärischen Potentiallandschaften T1 - Exciton-polariton condensation in organic semiconductor microcavities with hemispherical potential landscapes N2 - Exziton-Polaritonen sind hybride Quasiteilchen, die entstehen durch die starke Kopplung zwischen Halbleiter-Exzitonen und Mikrokavitätsphotonen in einem optischen Resonator. Aufgrund ihres bosonischen Charakters können die Polaritonen Kondensate ausbilden. In dieser Arbeit ist der emittierende organische Halbleiter das fluoreszierende Protein mCherry. Um einen räumlichen Einschluss zu generieren wurden hemisphärische Potentiale genutzt. Durch die Variation der Potentiallandschaft (Linse, Molekül, Kette, Su-Schrieffer-Heeger-Kette und Honigwaben-Gitter) konnten Eigenschaften wie beispielsweise topologisch nicht-triviale Defekte experimentell bei Umgebungstemperatur demonstriert werden. Zusammengefasst beschäftigt sich diese Arbeit mit der Exziton-Polartion Kondensation in unterschiedlichen Potentiallandschaften mit dem organischen Halbleiter mCherry. N2 - Exciton polaritons are hybrid quasiparticles that are created by the strong coupling between semiconductor excitons and microcavity photons in an optical cavity. Due to their bosonic character, the polaritons can form condensates. In this work, the emitting organic semiconductor is the fluorescent protein mCherry. Hemispherical potentials were used to create a spatial confinement. By varying the potential landscape (lens, molecule, chain, Su-Schrieffer-Heeger chain and honeycomb lattice), properties such as topological non-trivial defects were experimentally demonstrated at ambient temperature. In conclusion, this work deals with exciton-polarisation condensation in different potential landscapes with the organic semiconductor mCherry. KW - Exziton-Polariton KW - Kondensation KW - Organischer Halbleiter KW - Optischer Resonator KW - mCherry Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370554 ER - TY - JOUR T1 - Measurement of prompt photon production in √ s(NN) = 8.16 TeV \(p\) Pb collisions with ATLAS JF - Physics letters B N2 - The inclusive production rates of isolated, prompt photons in p Pb collisions at root s(NN) = 8.16 TeV are studied with the ATLAS detector at the Large Hadron Collider using a dataset with an integrated luminosity of 165 nb(-1) recorded in 2016. The cross-section and nuclear modification factor R-p pb are measured as a function of photon transverse energy from 20 GeV to 550 GeV and in three nucleon-nucleon centre-of-mass pseudorapidity regions, (-2.83, -2.02), (-1.84, 0.91), and (1.09, 1.90). The cross-section and R-p pb values are compared with the results of a next-to-leading-order perturbative QCD calculation, with and without nuclear parton distribution function modifications, and with expectations based on a model of the energy loss of partons prior to the hard scattering. The data disfavour a large amount of energy loss and provide new constraints on the parton densities in nuclei. (C) 2019 The Author. Published by Elsevier B.V. KW - Boson Production KW - PPB Collisions Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-312697 VL - 796 ER - TY - GEN A1 - Aichele, Thorsten A1 - Heurich, Tina A1 - Müller, Noemi A1 - Odenbreit, Carina A1 - Radičević, Jana A1 - Raith, Sarah A1 - Röseler, Christoph A1 - Zaus, Petra T1 - 7 + 4. SEED – Scenarios for the Use of ePortfolios in Digital Learning N2 - The SEED project is developing ePortfolios for teaching at the Julius-Maximilians-Universität Würzburg. ePortfolios make it possible to further develop teaching and learning in a competence-oriented manner and to strengthen the individual reflection aspect of academic studies to support training professional skills. A total of seven use cases were developed. They provide examples of how ePortfolios can be used in university teaching. Four exam variants help to illustrate both subject-specific and reflective components when examining using ePortfolios. KW - ePortfolio KW - action orientation KW - theory-praxis-transfer KW - reflective practice KW - peer-feedback KW - collaborative work KW - Handlungsorientierung Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370091 N1 - Deutsche Ausgabe unter https://doi.org/10.25972/OPUS-37007 ER - TY - GEN A1 - Aichele, Thorsten A1 - Heurich, Tina A1 - Müller, Noemi A1 - Odenbreit, Carina A1 - Radičević, Jana A1 - Raith, Sarah A1 - Röseler, Christoph A1 - Zaus, Petra T1 - 7 + 4. SEED – Szenarien für den Einsatz von E-Portfolios N2 - Mit dem Projekt SEED werden E-Portfolios für die Lehre an der Julius-Maximilians-Universität Würzburg erschlossen. E-Portfolios ermöglichen es, Lehren und Lernen kompetenzorientiert weiterzuentwickeln und den individuellen Reflexionsanteil eines wissenschaftlichen Studiums im Sinne der Ausbildung professioneller Handlungsfähigkeit zu stärken. Insgesamt wurden sieben Nutzungsszenarien herausgearbeitet. Sie zeigen exemplarisch, auf welche Weise E-Portfolios in der Hochschullehre eingesetzt werden können. Vier Prüfungsvarianten helfen, beim Prüfen mittels E-Portfolios sowohl fachliche als auch reflexive Anteile abzubilden. KW - E-Portfolio KW - Theorie-Praxis-Transfer KW - reflexive Praxis KW - Peer-Feedback KW - kollaboratives Arbeiten KW - Handlungsorientierung Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370078 N1 - Englische Ausgabe unter https://doi.org/10.25972/OPUS-37009 ER - TY - THES A1 - Wagner, Alena T1 - Herstellung und Qualitätskontrolle einer vaskularisierten Trägerstruktur zur Blasenrekonstruktion T1 - Production and quality control of a vascularized structure for bladder reconstruction N2 - Die regenerative Medizin gewinnt heutzutage immer mehr an Bedeutung. Der klinische Ersatz der Harnblase nach Tumoren oder bei Fehlbildungen stellt bis heute einen komplexen Eingriff mit zahlreichen Langzeitkomplikationen dar. Trotz etlicher Behandlungsmöglichkeiten können die aktuellen therapeutischen Maßnahmen nicht als langfristige Heilung angesehen werden. Meine Arbeit ist Teil einer präklinischen Großtierstudie zur Entwicklung eines neuartigen Blasenersatzes auf der Basis eines vaskularisierten Tissue-Engineering-Konstruktes. Mit der Herstellung eines vaskularisierten Augmentats (UroVaSc) wird ein Arzneimittel für neuartige Therapien (ATMP) für die Anwendung am Menschen entwickelt. Unter Zuhilfenahme fortschrittlicher Verfahren aus dem Bereich des Tissue Engineerings wird ein Gewebe hergestellt, welches im Empfänger die beiden kritischen Punkte der Vernarbung und insbesondere bei jungen Empfängern die Problematik eines nicht mitwachsenden Gewebes reduzieren oder verhindern soll. Als Ausgangsmaterialien dienen ein Abschnitt porcinen Jejunums und eine porcine Hautbiopsie. In der klinischen Anwendung wird die Hautbiopsie dem Empfänger des Augmentats entnommen. Aus den beiden Ausgangsmaterialien werden als Zwischenprodukte dezellularisiertes Jejunum (BioVaSc) und aus der Hautbiopsie eine primäre, mikrovaskuläre Endothelzellkultur (mvEC) hergestellt. Die mvEC besiedeln die Gefäße der Trägerstruktur BioVaSc in einem Bioreaktorsystem und führen zum vaskularisierten Endprodukt, der UroVaSc. Ziel der vorliegenden Arbeit war die Entwicklung eines dreidimensionalen, vaskularisierten Blasenaugmentats. Im Verlauf dieser Arbeit waren die Methoden der Isolation und Kultivierung der Zellen, die Rebesiedlung und Kultur des autologen Augmentats, als auch die Qualitätskontrolle unter den Richtlinien der Guten Herstellungspraxis zu etablieren. Für die Isolierung der mvEC wurde ein Protokoll erarbeitet, mit dem sich die Zellen, trotz intraindividueller Unterschiede der Spendertiere, in ausreichender Zellzahl und Reinheit darstellen ließen. Des Weiteren wurde die endotheliale Rebesiedlung der Trägerstruktur erfolgreich durchgeführt und dies mit Hilfe zellbiologischer und immunhistologischer Methoden belegt. In der Risikobeurteilung des Herstellungsprozesses wurde die Überwachung des Inkubators als wichtigen Schritt zur Erhöhung der Produktqualität identifiziert, der in weiterführenden Arbeiten adressiert werden sollte. Auf Grundlage meiner Forschungsergebnisse und weiterer Forschungsarbeiten erfolgt derzeit die funktionale Testung des Endproduktes im Großtierversuch. Mit der erfolgreichen Herstellung eines vaskularisierten Blasenaugmentats wird betroffenen Patienten eine neuartige Therapieoption eröffnet, welche die Aussicht auf eine Heilung schwerer Erkrankungen an der Blase ermöglicht. N2 - Regenerative medicine is becoming increasingly important nowadays. The clinical replacement of the urinary bladder after tumors or in cases of malformations has so far been a serious procedure with many long-term problems. Although there are diverse treatment options, the current therapeutic measures cannot be considered a permanent cure. My work is part of a preclinical animal study to develop a novel bladder replacement based on a vascularized tissue-engineered construct. The manufacturing of a vascularized bladder replacement (UroVaSc) will develop a advanced therapy medical product (ATMP) for human use. Using innovative tissue engineering techniques, a tissue is produced that is intended to reduce or prevent the two critical points of scarring in the recipient and, especially in young recipients, the problem of tissue that does not grow with the recipient. The raw material is a section of porcine jejunum and a porcine skin biopsy. In clinical use, the skin biopsy is taken from the recipient. Out of the two starting materials, the intermediates vascularized porcine jejunum (BioVaSc) and a primary, microvascular endothelial cell culture (mvEC) isolated from the porcine skin biopsy are prepared. The mvEC colonize the vessels of the BioVaSc in a bioreactor system, leading to the final product, UroVaSc. The aim of the study was to create a three-dimensional vascularized bladder augmentation. In the course of this work, the methods of isolation and cultivation of the cells, the re-colonization and culture of the autologous augmentation product, as well as the quality control under the guidelines of Good Manufacturing Practice had to be established. For the isolation of the mvEC, a protocol was developed that, despite intra-individual differences of the donor animals, allows the reproduction of cells in sufficient cell count and purity. Furthermore, the endothelial recolonization of the carrier structure was successfully executed and this was proven with the help of cell biological and immunohistological methods. In the area of quality control, the monitoring of the incubator was identified as an important step to increase product quality, which should be addressed in further work. Based on my research results and further research work, the functional testing of the final product in animal experiments is currently being performed. The successfully produced vascularized bladder replacement introduces a novel therapeutic option for affected patients, offering the prospect of a cure for severe diseases of the bladder. KW - Augmentation KW - Endothelzelle KW - Harnblasenkrankheit KW - Tissue Engineering KW - Blasenerkrankung Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370280 ER - TY - THES A1 - Steinmüller, Sophie Anna Maria T1 - Benzimidazole-Based Photoswitches and Photoswitchable Cannabinoid 2 Receptor Ligands T1 - Benzimidazol-Basierte Photoschalter und Photoschaltbare Liganden für den Cannabinoid 2 Rezeptor N2 - The field of photopharmacology has attracted considerable attention due to applying the spatial and temporal precision of light to pharmacological systems. Photoswitchable biologically active compounds have proven useful in the field of G protein-coupled receptors (GPCRs), which are of tremendous therapeutic relevance. Generally, the pharmacology of GPCRs is complex, perhaps even more complex than originally thought. Suitable tools are required to dissect the different signalling pathways and mechanisms and to unravel how they are connected in a holistic image. This is reflected in the enormous scientific interest in CB2R, as the neuroprotective and immunomodulatory effects attributed to CB2R agonists have not yet translated into effective therapeutics. This work focused on the development of a novel photoswitchable scaffold based on the privileged structure of benzimidazole and its application in photoswitchable CB2R ligands as photopharmacological tools for studying the CB2R. The visible-light photoswitchable ligand 10d enables the investigation of CB2R activation with regard to βarr2 bias, exhibiting a unique pharmacological profile as a “cis-on” affinity switch at receptor level and as a “trans-on” efficacy-switch in βarr2-mediated receptor internalization. The novel photoswitchable scaffold developed in this work further serves as a guide for the development of novel photoswitchable GPCR ligands based on the privileged structure of benzimidazole. To obtain a different tool compound for studying CB2R activation and signalling mechanisms, a previously reported putatively dualsteric CB2R ligand was rendered photoswitchable, by linking the orthosteric agonist to a CB2R-selective PAM via photoswitchable azobenzene. Compound 27-para exhibits a desirable “cis-on” behaviour across all investigated assays with >10-fold higher potency compared to its trans-isomer and can be used as an efficacy-switch employing specific concentrations. N2 - Das Forschungsfeld der Photopharmakologie hat stark an Beachtung gewonnen, da es die Anwendung der räumlichen und zeitlichen Präzision von Licht auf pharmakologische Systeme ermöglicht. Photoschaltbare biologisch aktive Verbindungen haben sich besonders für die Erforschung von G-Protein-gekoppelten Rezeptoren (GPCRs) als nützlich erwiesen, welche sich durch ihr enormes therapeutisches Potenzial auszeichnen. Die Pharmakologie der GPCRs ist komplex, vielleicht sogar komplexer als ursprünglich angenommen. Um die verschiedenen Signalwege und Mechanismen zu verstehen und zu entschlüsseln, wie sie in einem ganzheitlichen Bild zusammenhängen, werden geeignete Instrumente benötigt. Dies zeigt sich auch in dem enormen wissenschaftlichen Interesse am CB2R, da die den CB2R-Agonisten zugeschriebenen neuroprotektiven und immunmodulatorischen Effekte noch nicht in wirksame Therapeutika umgesetzt werden konnten. Die vorliegende Arbeit konzentrierte sich auf die Entwicklung eines neuartigen photoschaltbaren Gerüsts, das auf der privilegierten Struktur von Benzimidazol basiert, und dessen Anwendung in photoschaltbaren CB2R-Liganden als photopharmakologische Werkzeuge zur Untersuchung des CB2R. Der mit sichtbarem Licht schaltbare Ligand 10d ermöglicht die Untersuchung der CB2R-Aktivierung in Hinblick auf bevorzugte βarr2-Rekrutierung gegenüber G-Proteinen, mit einem einzigartigen pharmakologischen Profil als „cis-on"-Affinitätsschalter auf Rezeptorebene und als „trans-on"-Wirksamkeitsschalter bei der βarr2-vermittelten Rezeptorinternalisierung. Das in dieser Arbeit entwickelte neuartige photoschaltbare Gerüst dient als Leitfaden für die Entwicklung neuartiger photoschaltbarer GPCR-Liganden basierend auf der privilegierten Struktur von Benzimidazol. Um ein anderes Werkzeug für die Untersuchung der CB2R-vermittelten Signalmechanismen zu erhalten, wurde ein zuvor beschriebener, vermeintlich dualsterischer CB2R-Ligand photoschaltbar gemacht. Hierfür wurde ein orthosterischer Agonist mit einem CB2R-selektiven PAM über ein photoschaltbares Azobenzol verknüpft. Die Verbindung 27-para zeigt in allen untersuchten Assays das bevorzugte „cis on"-Verhalten mit einer >10-fach höheren Potenz im Vergleich zu ihrem trans-Isomer. KW - Cannabinoide KW - Photoswitchable KW - Cannabinoids Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-348943 ER - TY - THES A1 - Hadi, Naji Said Aboud T1 - In vitro Studies on the Genotoxicity of Selected Pyrrolizidine Alkaloids T1 - In-vitro-Studien zur Genotoxizität ausgewählter Pyrrolizidinalkaloide N2 - Cancer is one of the leading causes of death worldwide. Toxic contaminants in human food or medicinal products, such as substances like pyrrolizidine alkaloids (PAs), have been thought to contribute to cancer incidence. PAs are found in many plant species as secondary metabolites, and they may affect humans through contaminated food sources, herbal medicines, and dietary supplements. Hundreds of compounds belonging to PAs have been identified, differing in their chemical structures, either in their necine base moiety or esterification at their necic acid moiety. PAs undergo hepatic metabolism, and after this process, they can induce hepatotoxicity, genotoxicity, and carcinogenicity. However, the mechanism of inducing genotoxicity and carcinogenicity is still unclear and warrants further investigation. Therefore, the present study aims to investigate the mechanism of genotoxicity induced by selected PAs with different chemical structures in in vitro systems. Primarily, human hepatoma HepG2 cells were utilized, and in co-culture, metabolically active HepG2 cells were combined with non-metabolically active human cervical HeLa H2B-GFP cells. First, the genotoxicity of the PAs europine, lycopsamine, retrorsine, riddelliine, seneciphylline, echimidine, and lasiocarpine was investigated in the cytokinesis-block micronucleus (CBMN) assay. All seven selected PAs caused the formation of micronuclei in a dose-dependent manner, with the maximal increase of micronucleus formation ranging from 1.64 to 2.0 fold. The lowest concentrations at which significant induction of micronuclei was found were 3.2 µM for lasiocarpine and riddelliine, 32 µM for retrorsine and echimidine, and 100 µM for seneciphylline, europine, and lycopsamine. These results confirmed previously published potency rankings in the micronucleus assay. The same PAs, with the exception of seneciphylline, were also investigated in a crosslink-modified comet assay, and reduced tail formation after hydrogen peroxide treatment was found in all diester-type PAs. Meanwhile, an equimolar concentration of the monoesters europine and lycopsamine did not significantly reduce DNA migration. Thus, the crosslinking activity was related to the ester type. Next, the role of metabolic enzymes and membrane transporters in PA-induced genotoxicity was assessed. Ketoconazole (CYP 450-3A4 inhibitor) prevented lasiocarpine-induced micronucleus formation completely, while furafylline (CYP 450-1A2 inhibitor) reduced lasiocarpine-induced micronucleus formation, but did not abolish it completely. This implies that the CYP 450 enzymes play an important role in PA-induced genotoxicity. Carboxylesterase 2 enzyme (CES 2) is commonly known to be involved in the detoxification of xenobiotics. Loperamide (CES 2 inhibitor) yielded an increased formation of lasiocarpine-induced micronuclei, revealing a possible role of CES-mediated detoxification in the genotoxicity of lasiocarpine. Also, intracellular glutathione (GSH) plays an important role in the detoxification of xenobiotics or toxins in the cells. Cells which had been pretreated with L-buthionine sulfoximine (BSO) to reduce GSH content were significantly more sensitive for the induction of micronucleus formation by lasiocarpine revealing the importance of GSH in PA-induced genotoxicity. Quinidine (Q) and nelfinavir (NFR) are OCT1 and OATP1B1 influx transporter inhibitors, respectively, which reduced micronucleus induction by lasiocarpine (only quinidine significantly), but not completely, pointing to a relevance of OCT1 for PA uptake in HepG2 cells. Verapamil (V) and benzbromarone (Bz) are MDR1 and MRP2 efflux transporter inhibitors, respectively, and they caused a slightly increased micronucleus induction by lasiocarpine (significant only for benzbromarone) thus, revealing the role of efflux transporters in PA-induced genotoxicity. The mechanistic approach to PA-induced genotoxicity was further studied based on oxidative stress via the formation of reactive oxygen species (ROS) in HepG2 cells. Overproduction of ROS can cross-link cellular macromolecules such as DNA, leading to genomic damage. An equimolar concentration of 10 µM of lasiocarpine (open-diester PA), riddelliine (cyclic-diester PA), and europine (monoester) significantly induced ROS production, with the highest ROS generation observed after lasiocarpine treatment, followed by riddelliine and then europine. No significant increase in ROS production was found with lycopsamine (10 µM; monoester PA), even at a higher concentration (320 µM). The generation of ROS by these PAs was further analyzed for confirmation by using 5 mM of the thiol radical scavenger antioxidant N-acetyl cysteine (NAC) combined with lasiocarpine, riddelliine, or europine. This analysis yielded a significant decrease in ROS after combining NAC with lasiocarpine, riddelliine, and europine. In addition, lasiocarpine, riddelliine, and europine induced a loss of mitochondrial membrane potential, pointing to mitochondria as the source of ROS generation. In vivo, hepatic sinusoidal epithelial cells (HSECs) are known to be damaged first by PAs after hepatic metabolization, but HSECs themselves do not express the required metabolic enzymes for activation of PAs. To mimic this situation, HepG2 cells were used to metabolically activate PA in a co-culture with HeLa H2B-GFP cells as non-metabolically active neighbours. Due to the green fluorescent GFP label the HeLa cells could be identified easily based in the co-culture. The PAs europine, riddelliine and lasiocarpine induced micronucleus formation in HepG2 cells, and in HeLa H2B-GFP cells co-cultured with HepG2 cells, but not in HeLa H2B-GFP cells cultured alone. Metabolic inhibition of CYP 450 enzymes with ketoconazole abrogated micronucleus formation induced by the same PAs tested in the co-culture. The efflux transporter inhibitors verapamil and benzbromarone reduced the micronucleus formation in the co-culture. Furthermore, mitotic disturbances as an additional genotoxic mechanism of action were observed in HepG2 cells and in HeLa H2B-GFP cells co-cultured with HepG2 cells, but not in HeLa H2B-GFP cells cultured alone. Overall, we were able to show that PAs were activated by HepG2 cells and the metabolites induced genomic damage in co-cultured non-metabolically active green HeLa cells. Finally, in HepG2 cells as well as the co-culture, combinations of PAs lasiocarpine and riddelliine favoured an additive effect rather than synergism. Thus, this study therefore provides support that the assumption of dose-addition can be applied in the characterization of the genotoxicity risk of PAs present in a mixture. N2 - Krebs ist eine der häufigsten Todesursachen weltweit. Toxische Verunreinigungen in Lebensmitteln oder pflanzlichen Arzneimitteln, wie Pyrrolizidinalkaloide (PAs), können zur Krebsinzidenz beitragen. PAs kommen in vielen Pflanzenarten als Sekundärmetabolite vor. Menschen können diese über kontaminierte Nahrungsquellen, pflanzliche Arzneimittel und Nahrungsergänzungsmittel aufnehmen. Eine Vielzahl von Verbindungen, die zu pyrrolizidinalkaloidhaltigen Substanzen (PAs) gehören, wurden identifiziert. Diese unterscheiden sich in ihrer chemischen Struktur entweder durch ihre Necinbaseneinheit oder ihre Veresterung an der Necicsäureeinheit. Nach metabolischer Aktivierung in der Leber können PAs Hepatotoxizität, Genotoxizität und Karzinogenität induzieren. Jedoch ist der Genotoxizitätsmechanismus nicht vollständig aufgeklärt und erfordert weitere Untersuchungen. Das Ziel dieser Studie liegt in der Untersuchung des Mechanismus der Genotoxizität, die in vitro durch bestimmte PAs mit unterschiedlicher chemischer Struktur induziert wird. Hierbei wurden primär humane Hepatom-HepG2-Zellen verwendet sowie in Co-Kultur metabolisch aktive HepG2-Zellen und nicht-metabolisch aktive humane zervikale HeLa H2B-GFP-Zellen. Zunächst wurde die Genotoxizität der PAs Europin, Lycopsamin, Retrorsin, Riddelliin, Seneciphyllin, Echimidin und Lasiocarpin im Zytokinese-Block-Mikronukleus-Assay (CBMN) untersucht. Die sieben (7) ausgewählten PAs führten dosisabhängig zur Bildung von Mikrokernen. Der maximale Anstieg der Mikronukleusbildung lag für alle PAs im Bereich des 1,64- bis 2,0-fachen des Ausgangswertes. Die niedrigsten Konzentrationen, bei denen eine signifikante Induktion von Mikrokernen gefunden wurde, waren 3,2 μM für Lasiocarpin und Riddelliin, 32 μM für Retrorsin und Echimidin sowie 100 μM für Seneciphyllin, Europin und Lycopsamin. Diese Ergebnisse bestätigen zuvor veröffentlichte Potenz-Rankings im Mikronukleus-Assay. Die Genotoxizität der gleichen PAs, mit Ausnahme von Seneciphyllin, wurde zusätzlich mittels eines Crosslink-modifizierten Comet-Assay untersucht. Es wurde eine reduzierte Schweifbildung nach der Behandlung mit Wasserstoffperoxid in allen PAs des Diestertyps gefunden, während eine äquimolare Konzentration der Monoester Europin und Lycopsamin die DNA-Migration nicht signifikant reduzierte. Dies deutet darauf hin, dass die Vernetzungsaktivität von PAs auf der Ester-Einheit beruht. Als nächstes wurde die Rolle von Stoffwechselenzymen und Membrantransportern in der PA-induzierten Genotoxizität untersucht. Ketoconazol (CYP 450-3A4-Inhibitor) verhinderte die Lasiocarpin-induzierte Mikronukleusbildung vollständig, während Furafyllin (CYP 450-1A2-Inhibitor) die Lasiocarpin-induzierte Mikronukleusbildung reduzierte, aber nicht vollständig beseitigte. Dies deutet darauf hin, dass CYP 450-Enzyme eine wichtige Rolle bei der PA-induzierten Genotoxizität spielen. Es ist allgemein bekannt, dass das Enzym Carboxylesterase 2 (CES-2) an der Entgiftung von Xenobiotika beteiligt ist. Loperamid (CES-2-Inhibitor) führte zu einer erhöhten Bildung von Lasiocarpin-induzierten Mikrokernen, was auf eine mögliche Rolle der CES-vermittelten Entgiftung bei der Genotoxizität von Lasiocarpin hindeutet. Auch intrazelluläres Glutathion (GSH) spielt eine wichtige Rolle bei der Entgiftung von Xenobiotika oder Toxinen. Zellen, die mit L-Buthioninsulfoximin (BSO) vorbehandelt worden waren, um den GSH-Gehalt zu reduzieren, waren signifikant empfindlicher für die Induktion der Mikronukleusbildung durch Lasiocarpin, was die Bedeutung von GSH für die PA-induzierte Genotoxizität zeigt. Chinidin (Q) und Nelfinavir (NFR) sind OCT1- bzw. OATP1B1-Influx-Transporter-Inhibitoren, die die Mikronukleus-Induktion durch Lasiocarpin reduzierten (nur Chinidin signifikant), aber nicht vollständig, was auf eine Relevanz von OCT1 für die PA-Aufnahme in HepG2-Zellen hindeutet.Verapamil (V) und Benzbromaron (Bz) sind MDR1- bzw. MRP2-Efflux-Transporter-Inhibitoren und verursachten eine leicht erhöhte Mikronukleus-Induktion durch Lasiocarpin (signifikant nur für Benzbromaron), was die Rolle von Efflux-Transportern bei der PA-induzierten Genotoxizität aufzeigt. Der Mechanismus der PA-induzierten Genotoxizität wurde auf der Grundlage von oxidativem Stress durch die Bildung von reaktiven Sauerstoffspezies (ROS) in HepG2-Zellen weiter untersucht. Eine Überproduktion von ROS kann zelluläre Makromoleküle wie DNA vernetzen, was zu genomischen Schäden führt. Eine äquimolare Konzentration von 10 μM von Lasiocarpin (Open-Diester PA), Riddelliin (Cyclic-Diester PA) und Europin (Monoester) induzierte signifikant die ROS-Produktion, wobei die höchste ROS-Erzeugung nach Lasiocarpin-Behandlung beobachtet wurde, gefolgt von Riddelliin und Europin. Mit Lycopsamin (10 μM; Monoester PA) wurde auch bei höherer Konzentration (320 μM) keine signifikante Steigerung der ROS-Produktion gefunden. Um die Beteiligung von ROS am Mechanismus der Genotoxizität einzelner PAs genauer zu betrachten und die bisherigen Ergebnisse zu bestätigen, wurden weitere Untersuchungen in Anwesenheit des Sauerstoffradikalfängers N-Acetylcysteine (NAC) in Kombination mit Lasiocarpin, Riddelliin oder Europin durchgeführt. Diese Analyse ergab eine signifikante Abnahme der ROS-Produktion nach der Kombination von NAC mit Lasiocarpin, Riddelliin und Europin. Darüber hinaus induzierten Lasiocarpin, Riddelliin und Europin Veränderungen im mitochondrialen Membranpotenzial. Dies deutet darauf hin, dass ROS vermehrt in den Mitochondrien der Zellen gebildet werden. Aus in vivo Daten ist bekannt, dass hepatische sinusoidale Epithelzellen (HSECs) die Zelltypen innerhalb der Leber sind, die nach der metabolischen Aktivierung von PAs zuerst geschädigt werden. Jedoch exprimieren HSECs nicht die erforderlichen Stoffwechselenzyme für die Aktivierung von PAs. Um diese Situation nachzuahmen, wurden HepG2-Zellen verwendet, um PAs in einer Kokultur mit HeLa H2B-GFP-Zellen als nicht-metabolisch aktive Nachbarn metabolisch zu aktivieren. Durch die grün fluoreszierende GFP-Markierung konnten die HeLa-Zellen in der Co-Kultur leicht identifiziert werden. Die PAs Europine, Riddelliin und Lasiocarpin induzierten die Bildung von Mikrokernen in HepG2-Zellen und in HeLa H2B-GFP-Zellen, die mit HepG2-Zellen kokultiviert wurden, jedoch nicht in HeLa H2B-GFP-Zellen, die allein kultiviert wurden. Die metabolische Hemmung von CYP 450-Enzymen mit Ketoconazol hob die Mikronukleusbildung, welche durch die zuvor getesteten PAs induziert wurde, auf. Die Efflux-Transporter-Inhibitoren Verapamil und Benzbromaron reduzierten die Mikronukleusbildung in der Kokultur. Darüber hinaus wurden mitotische Störungen als zusätzlicher genotoxischer Wirkmechanismus in der Co-Kultur aus HepG2-Zellen und in HeLa H2B-GFP-Zellen beobachtet, jedoch nicht in HeLa H2B-GFP-Zellen, die allein kultiviert wurden. Zusammengefasst deuten diese Ergebnisse darauf hin, dass PAs durch HepG2-Zellen bioaktiviert werden können und aus PAs gebildete Metabolite genomische Schäden in kokultivierten, nicht-metabolisch aktiven HeLa-Zellen induzierten. Abschließend zeigen Kombinationen der PAs Lasiocarpin und Riddelliin sowohl in HepG2-Zellen als auch in der Co-Kultur eher einen additiven Effekt als einen Synergismus. Diese Studie liefert daher Unterstützung für die Annahme, dass die Dosisaddition zur Charakterisierung des genotoxischen Risikos von in einem Gemisch vorhandenen PAs angewendet werden kann. KW - Pyrrolizidine alkaloids KW - HeLa H2B-GFP-Zellen KW - Pyrrolizidinalkaloide KW - Kleinkern KW - Mutagenität KW - Genotoxizität KW - DNA-Vernetzung KW - mitotische Störung KW - Co-culture KW - metabolische Aktivierung KW - Membrantransporter KW - metabolische Enzyme KW - HepG2-Zellen KW - Genotoxicity KW - Micronuclei KW - DNA crosslink KW - Mitotic disturbance KW - Metabolic activation KW - Membrane transporters KW - Metabolic enzymes KW - HepG2 cells KW - HeLa H2B-GFP cells KW - micronucleus Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370376 ER - TY - THES A1 - Koch, Hanna Ulrike T1 - Funktionelle Untersuchung von IGF1R Mutationen im Multiplen Myelom T1 - Functional Investigation of IGF1R Mutations in Multiple Myeloma N2 - Das Mutationsspektrum einzelner Gene beziehungsweise zusammengefasster Gengruppen innerhalb von Signalwegen bei Patienten mit Multiplem Myelom wurde in den letzten Jahren eingehend untersucht und charakterisiert. Die Herausforderung besteht nun in der Interpretation der erhobenen Daten, insbesondere der Bewertung einzelner durch Sequenzierung identifizierter Biomarker bezüglich deren prognostischer Aussagekraft und konkreter therapeutischer Relevanz. Als übergeordnetes Ziel gilt die Ableitung von klinischen (Therapie-) Ansätzen. Auf dem Weg zu einem individualisierten Therapieansatz ist entscheidend, dass wir unser Wissen über die funktionelle Relevanz einzelner Mutationen wie hier im IGF1R im Hinblick auf deren Einbettung in Signalnetzwerke und auf das Proliferationsverhalten der MM Zellen erweitern. Konkret wurde im Rahmen der vorliegende Doktorarbeit der Einfluss von zwei IGF1R Punktmutationen, nämlich D1146N (Punktmutation des IGF1R der HMCL L-363) und N1129S (Punktmutation des IGF1R eines Patienten der DSMM XI Kohorte) auf die Proliferation und das nachgeschaltete Signalling in IGF1R-Überexpressionsmodellen der MM Zelllinien AMO-1 und U-266 untersucht. Zur stabilen Transfektion der HMCLs mit IGF1RWT und den zwei IGF1R Mutanten wurde ein Protokoll auf Grundlage des Sleeping Beauty (SB) Transposase Systems genutzt. In dieser und anderen assoziierten Arbeit konnte unter zu Hilfenahme von insgesamt vier verschiedenen gentechnisch veränderter HMCLs gezeigt werden, dass funktionelle Mutationen im IGF1R Effekte auf das Downstream Signalling zum Beispiel die Aktivierung von AKT und ERK, jedoch nicht auf die Zellproliferation haben. Im Vergleich der untersuchten HMCLs konnten jedoch keine verallgemeinerbaren Schlüsse gezogen werden, was die Heterogenität der Erkrankung und die Wichtigkeit der Einzelfallbetrachtung unterstreicht. N2 - Multiple myeloma (MM) is a malignant disease of the plasma cell and represents around 15% of all hematological neoplasms. There is a marked heterogeneity in terms of the severity of the disease, the progression and prognosis of the patients. This is also reflected in the underlying genetic heterogeneity. Genetic screenings at diagnosis and during the course of the disease are therefore essential. However, a better understanding of the pathogenesis of MM and the influence of individual genetic aberrations is essential to achieve improvements in personalized, targeted and, above all, risk-adapted therapy. The dysregulation of Receptor Tyrosine Kinases (RTKs), which significantly influences growth and progression, plays a decisive role in many types of cancer. Hence, RTKs also represent interesting target structures for cancer therapy. Specific RTK inhibitors have been a fixed element of oncological therapy in guidelines for many years with good therapeutic results, e. g. for breast, colon, or lung cancer. RTK signal transduction also plays an important role in MM. In a next generation sequencing study on a MM cohort, tumor-associated mutations were detected in RTK genes, which were associated with a significantly poorer prognosis. IGF1R was among the most frequently mutated RTKs in this. It has a decisive influence on e. g. cell proliferation of MM cells and therefore plays an important role in the pathogenesis of MM. Studies also suggest a connection between IGF1R overexpression and disease progression. IGF1R inhibitors were tested in clinical phase 1 studies as a monotherapy without significantly improved clinical response. However, in combination schemes with dexamethasone and bortezomib in patients with relapsed or refractory disease better results have been achieved. They cause manageable side effects and are promising concerning the length and depth of remission, especially in proteasome inhibitor refractory patients. Based on this information a project of the AG Leich aimed to study the influence of IGF1R and specifically IGF1R mutations in different HMCLs by means of functional analysis to identify patient cohorts, who might benefit from a therapy with IGF1R inhibitors. More specifically, the influence of two IGF1R mutations, namely D1146N (point mutation of IGF1R in the HMCL L-363) and N1129S (point mutation of IGF1R in a patient of the DSMM XI cohort), on proliferation and downstream signaling was to be investigated in IGF1R-overexpression models of the HMCLs AMO-1 and U-266 in this doctoral thesis. A protocol based on the Sleeping Beauty (SB) Transposase System was used for stable transfection of the HCMLs with IGF1RWT and the two IGF1R mutants. An increased expression or activation of downstream effectors could be detected in AMO-1. For example, the degree of phosphorylation of MEK and ERK in all three AMO-1 IGF1R overexpression cell lines (WT and two IGF1R mutant cell lines) under normal cell culture conditions seemed to be elevated in comparison to the empty vector control. However, no mutant specific differences could be detected even after stimulation with IGF1. Regarding IGF1R overexpression cell lines that were derived from U-266, expression and activation of IGF1R was especially pronounced for the IGF1R mutant IGF1RN1129S. In contrast, expression and activation of AKT, MEK and ERK in this IGF1R mutant overexpression cell line compared to the WT overexpression cell line, were not distinctively higher. Thus, it seems as if the role of IGF1R in different HMCLs varies, which could be also shown in other MM in vitro studies. The proliferation rate of the individual cell lines was not measured higher due to the overexpression of IGF1R, although important kinases such as AKT, MEK and ERK with their great importance concerning survival, growth and proliferation had been induced. Examinations with the IGF1R inhibitor Linsitinib on different HMCLs in subsequent studies of the AG Leich showed a reduction in metabolism in six out of seven cell lines, whereby the response was highly variable across cell lines and was independent of the IGF1R expression level or the IGF1R mutational status. Clear signs of apoptosis could be only detected in the HMCL MM1.S. An additive effect when combining Linsitinib with the proteasome inhibitor Carfilzomib, mostly used for therapy of refractory MM, was only detected in the IGF1R mutated HMCL L-363. Therefore, this combination might be a promising approach for patients with refractory MM, especially for patients with a IGF1R mutation. However, those compiled preliminary findings should be examined more closely in further in vitro and in vivo studies to determine the therapeutic potential of IGF1R inhibitors applied solely or in combination schemes with other specific inhibitors (e. g. iAKT or iMEK) or licensed standard drugs for patients with IGF1R mutations. KW - Plasmozytom KW - IGF1R Mutationen KW - Multiples Myelom KW - Funktionelle Untersuchung KW - Insulin-like Growth Factor I KW - IGF1 Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370406 ER - TY - THES A1 - Woidich, Robert T1 - Einfluss von IL-17 auf die Stabilität und Funktion von regulatorischen T-Zellen T1 - Influence of IL-17 on the stability and function of regulatory T cells N2 - In der Pathogenese der Psoriasis spielen IL 17 und die Plastizität von Tregs zu Th17 Zellen mit Produktion proinflammatorischer Zytokine sowie die möglicherweise reduzierte suppressive Funktion von Tregs eine entscheidende Rolle. Wir versuchten daher in unserer Arbeit einen Überblick über die T Zellverteilung im peripherem Blut bei PSO und HC zu erhalten und die Reaktion der Zellen auf IL 17, anti IL 17 und Secukinumab sowie ein Th 17 induzierendes Milieu im Vergleich von PSO und HC zu evaluieren. In der Analyse der PBMCs von PSO und HC konnten bei PSO tendenziell weniger inflammatorische Marker, wahrscheinlich aufgrund der niedrigen Krankheitsaktivität und der bereits eingeleiteten medikamentösen Therapie festgestellt werden. Nach Isolierung der Tregs und Kultivierung konnten bei PSO im Vergleich zu HC erhöhte inflammatorische Marker nachgewiesen werden. Dies kann an der höheren Plastizität von Tregs bei PSO ex vivo ohne den Einfluss einer medikamentösen Therapie hin zu inflammatorischen Zellen. In den Suppressionsversuchen zeigte sich sowohl bei PSO als auch bei HC unter Th17 Milieu eine verminderte Inhibition der PBMCs durch die autologen Tregs. Ursächlich hierfür könnte eine Dysregulation der Tregs durch das Th17 Milieu oder eine Auswirkung des Th17-induzierenden Cocktails auf die PBMCs im Sinne einer Effektorresistenz gegenüber den Tregs sein. Eine Veränderung der Suppression ergab sich für IL 17 oder anti IL 17 nicht. Unter der gleichzeitigen Kultivierung mit Secukinumab und einem Th17 induzierendem Cocktail konnte keine verbesserte Inhibition festgestellt werden. Insgesamt bestätigt die Arbeit eine Instabilität der Tregs bei PSO mit der Möglichkeit der Plastizität zu Th17 Zellen unter proinflammatorischem Milieu, sowie einen Verlust der Suppressionsfähigkeit durch eine Treg Dysfunktion oder eine erhöhte Effektorresistenz. Für IL 17 oder die Blockade von IL 17 durch monoklonale Antikörper konnte in unserer Studie kein Einfluss festgestellt werden. N2 - In the pathogenesis of psoriasis IL 17 and the plasticity of Tregs to Th17 cells with the production of pro-inflammatory cytokines, as well as the possibly reduced suppressive function of Tregs, play a crucial role. Therefore we aimed to obtain an overview of the T cell distribution in peripheral blood in PSO and HC and to evaluate the response of the cells to IL 17, anti-IL 17, and Secukinumab, as well as a Th17-inducing milieu in comparison between PSO and HC. In the analysis of PBMCs from PSO and HC, fewer inflammatory markers were found in PSO, probably due to the low disease activity and the already initiated medical therapy. After isolating and culturing the Tregs, increased inflammatory markers were detected in PSO compared to HC. This may be due to the higher plasticity of Tregs in PSO ex vivo towards inflammatory cells without the influence of medical therapy. In the suppression assays, both PSO and HC showed reduced inhibition of PBMCs by autologous Tregs under Th17 milieu. This could be caused by a dysregulation of Tregs due to the Th17 milieu or an effect of the Th17-inducing cocktail on PBMCs in terms of effector resistance to Tregs. No change in suppression was observed for IL 17 or anti-IL 17. Co-cultivation with Secukinumab and a Th17-inducing cocktail did not show improved inhibition. Overall, the study confirms the instability of Tregs in PSO with the potential for plasticity to Th17 cells under pro-inflammatory milieu, as well as a loss of suppressive ability due to Treg dysfunction or increased effector resistance. No influence was observed for IL 17 or the blockade of IL 17 by monoclonal antibodies in our study. KW - Regulatorischer T-Lymphozyt KW - Schuppenflechte KW - Interleukin 17 KW - Treg-Plastizität Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370199 ER - TY - THES A1 - Hofmann, Kristina Simone T1 - Untersuchung von mechanischen Eigenschaften, Bruchfestigkeit und Haftfestigkeit von Multilayer Zirkoniumdioxidkeramik zu dualhärtenden Befestigungskompositen T1 - Investigation of mechanical properties, fracture strength and shear bond strength of multilayer zirconia ceramics to dual-curing luting composites N2 - Ziel der Arbeit war es, den Einfluss der Platzierung der Restauration im Rohling auf die mechanischen Eigenschaften und die Scherfestigkeit zu dualhärtenden Befestigungskompositen zu untersuchen sowie Unterschiede in der Bruchfestigkeit zwischen zwei Multilayerkeramiken zu ermitteln. Material und Methodik: Es wurden 160 zylindrische Prüfkörper aus der Multilayerkeramik Katana Zirconia ML hergestellt, um mechanische Eigenschaften wie Dichte, Biegefestigkeit und Härte zu bestimmen. Eine Gruppe wurde künstlich gealtert. Die Bruchfestigkeit von 32 Kronen (Katana Zirconia ML, Ceramill Zolid FX Multilayer) wurde vor und nach thermischer sowie mechanischer Belastung untersucht. Zur Bestimmung der Scherfestigkeit wurden 512 quadratische Prüfkörper hergestellt, die verschiedenen thermischen Belastungen ausgesetzt wurden. Die Scherfestigkeit wurde mit einer Universalprüfmaschine bestimmt und die Brucharten (adhäsiv, kohäsiv, gemischt) wurden analysiert. Ergebnisse: Es gab keinen signifikanten Unterschied zwischen den Schichten oder der Alterung bei Dichte, Biegefestigkeit und Härte. Katana Zirconia ML zeigte höhere Bruchfestigkeit als Ceramill Zolid FX Multilayer. Die Scherfestigkeit von Panavia V5 zu Katana Zirconia ML war nicht durch thermische Belastung beeinflusst, jedoch bei Ceramill Zolid FX Multilayer. Der Haftverbund von Visalys CemCore war durch thermische Belastung beeinflusst, während Panavia V5 zu beiden Keramiken höhere Werte aufwies. Katana Zirconia ML hatte höhere Scherfestigkeitswerte als Ceramill Zolid FX Multilayer. Schlussfolgerung: Multilayerkeramik stellt eine arbeitsverringernde Alternative für den Seitenzahnbereich dar, ohne mechanische und ästhetische Einbußen. Die Platzierung im Rohling hat keinen Einfluss auf die Eigenschaften, jedoch ist der Haftverbund vom Befestigungskomposit abhängig. N2 - The aim of the work was to investigate the influence of the placement of the restoration in the blank on the mechanical properties and the shear bond strength of dual-curing luting composites and to determine differences in the fracture strength between two multilayer ceramics. Material and method: 160 cylindrical test specimens were made from the multilayer ceramic Katana Zirconia ML to determine mechanical properties such as density, flexural strength and hardness. One group was artificially aged. The breaking strength of 32 crowns (Katana Zirconia ML, Ceramill Zolid FX Multilayer) was examined before and after thermal and mechanical loading. To determine the shear bond strength, 512 square test specimens were produced and subjected to various thermal loads. The shear bond strength was determined using a universal testing machine and the fracture types (adhesive, cohesive, mixed) were analyzed. Results: There was no significant difference between layers or aging in density, flexural strength and hardness. Katana Zirconia ML showed higher breaking strength than Ceramill Zolid FX Multilayer. The shear bond strength of Panavia V5 to Katana Zirconia ML was not affected by thermal loading, but was affected in combination with Ceramill Zolid FX Multilayer. The adhesive bond of Visalys CemCore was influenced by thermal stress, while Panavia V5 had higher shear bond strength to both ceramics. Katana Zirconia ML had higher shear bond strength than Ceramill Zolid FX Multilayer. Conclusion: Multilayer ceramics represent a labor-reducing alternative for the posterior region, without mechanical and aesthetic losses. The placement in the blank has no influence on the properties, but the adhesive bond depends on the fixing composite. KW - Zirkoniumoxidkeramik KW - Multilayer-Zirkoniumdioxidkeramiken KW - Biaxiale Biegefestigkeit KW - Vickers-Härte KW - CAD/CAM restoration material KW - adhesive luting agent KW - shear bond strength KW - Biegefestigkeit KW - Härte KW - Mechanische Eigenschaft KW - Restaurative Zahnmedizin KW - Scherfestigkeit KW - Befestigungszement Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370308 ER - TY - THES A1 - Schrauth, Monika Maria T1 - Therapeutisches Drug Monitoring (TDM) von Kindern und Jugendlichen unter Pharmakotherapie mit Escitalopram und Mirtazapin T1 - Therapeutic Drug Monitoring (TDM) of Children and Adolescents Treated with Escitalopram and Mirtazapine N2 - Diese retrospektive, naturalistische Studie beschäftigte sich mit dem Therapeutischen Drug Monitoring von Kindern und Jugendlichen unter Psychopharmakotherapie mit Escitalopram und Mirtazapin. Die Datenauswertung erfolgte anhand von klinischen Routinedaten aus dem TDM-Service des Speziallabors für TDM des Zentrums für psychische Gesundheit des Universitätsklinikums Würzburg. In der Studie wurden die Zusammenhänge zwischen Dosis, Serumkonzentration und positiver bzw. negativer klinischer Effekte, auch im Hinblick auf mögliche Einflussfaktoren wie Geschlecht, Alter, BMI-Status, Komedikation und Raucherstatus, untersucht. Ein weiteres Ziel der Arbeit war, Hinweise für die Definition eines altersspezifischen therapeutischen Referenzbereiches (Diagnoseübergreifend und Depressions-spezifisch) für Kinder und Jugendliche beider Medikamente zu gewinnen. Hierfür wurden für Escitalopram 41 Patienten im Alter zwischen elf und 18 Jahren und für Mirtazapin 23 Patienten im Alter von sechs bis 18 Jahren eingeschlossen und Daten zur Demographie, Serumkonzentrationsbestimmungen im Steady State, Schwere der Erkrankung (CGI-S), Therapieeffektivität (CGI-I) und Nebenwirkungen (UKU-Skala) ausgewertet. Escitalopram: Die mittlere Tagesdosis betrug 14,8 mg, wobei die Serumkonzentrationen mit einer mittleren Konzentration von 32,2 ng/ml (SD= 26,6 ng/ml) zwischen sechs und 109 ng/ml schwankten. Bei 63,4 % der Patienten lag die ermittelte Serumkonzentration in dem für Erwachsene definierten therapeutischen Referenzbereich (15-80 ng/ml). Zwischen der Tagesdosis und der Serumkonzentration ergab sich eine auf dem 1 %-Niveau signifikante positive lineare Beziehung (rs= 0,46; p= 0,003). 65,9 % der Patienten respondierten seit Behandlungsbeginn. Zwischen der Serumkonzentration und dem therapeutischen Effekt (rs= 0,193; p= 0,282) und zwischen der Serumkonzentration und den Nebenwirkungen (r= 0,127; p= 0,467) konnte jeweils kein signifikanter Zusammenhang gefunden werden. Die Nebenwirkungsrate lag bei 25,7 %, wobei am häufigsten Spannung und innere Unruhe dokumentiert wurde. Mit der Idee, die Definition für den vorläufigen therapeutischen Referenzbereich sowohl der Konsensus-Leitlinie der AGNP (Hiemke et al., 2018) als auch von Hiemke (2019) zu berücksichtigen, wird als vorläufiger therapeutischer Referenzbereich für Escitalopram für Kinder und Jugendliche mit Depression eine untere Grenze zwischen 10 ng/ml bis 15 ng/ml und eine obere Grenze von 50 ng/ml vorgeschlagen. Dieser Bereich liegt niedriger als der für erwachsene Patienten definierte Bereich für Escitalopram von 15 bis 80 ng/ml. Mirtazapin: Die mittlere Tagesdosis betrug 28,6 mg, wobei die Serumkonzentrationen mit einer mittleren Konzentration von 40,8 ng/ml (SD= 28,1 ng/ml) zwischen 13 und 130 ng/ml schwankten. Für 52,2 % der Patienten lag die Serumkonzentration in dem für Erwachsene definierten therapeutischen Referenzbereich (30-80 ng/ml). Zwischen der Tagesdosis und der Serumkonzentration ergab sich eine auf dem 1 %-Niveau signifikante positive Korrelation (rs= 0,655; p= 0,001). Hinsichtlich des Therapieeffektes respondierten 52,2 % der Patienten seit Behandlungsbeginn. Zwischen der Serumkonzentration und dem therapeutischen Effekt ergab sich ein auf dem 5 %-Niveau signifikanter positiver Zusammenhang (rs= 0,534; p= 0,015). Zwischen der Serumkonzentration und den Nebenwirkungen konnte kein signifikanter Zusammenhang gefunden werden (r= 0,240; p= 0,282). Die Nebenwirkungsrate lag bei 30,4 %, wobei Schläfrigkeit und Sedierung am häufigsten berichtet wurden. Als vorläufiger therapeutischer Referenzbereich für Mirtazapin für Kinder und Jugendliche mit Depression wird eine untere Grenze zwischen 15 ng/ml bis 20 ng/ml und eine obere Grenze von 50 ng/ml vorgeschlagen. Dieser Bereich liegt niedriger als der für erwachsene Patienten definierte Bereich für Mirtazapin von 30 bis 80 ng/ml. Die Limitationen der vorliegenden naturalistischen Studie beachtend, sollten die Ergebnisse mit Vorsicht interpretiert und anhand einer größeren Stichprobe unter kontrollierteren Bedingungen überprüft werden. N2 - This retrospective, naturalistic study focussed on the therapeutic drug monitoring of children and adolescents treated with escitalopram and mirtazapine. The data analysis was based on routine clinical data from the TDM service of the special laboratory for TDM at the Centre for Mental Health at the University Hospital of Würzburg. The study analysed the correlations between dose, serum concentration and positive or negative clinical effects, also with regard to possible influencing factors such as gender, age, BMI status, comedication and smoking status. A further aim of the study was to obtain indications for the definition of an age-specific therapeutic reference range (cross-diagnostic and depression-specific) for children and adolescents of both drugs. For this purpose, 41 patients aged between eleven and 18 years were included for escitalopram and 23 patients aged between six and 18 years for mirtazapine, and data on demographics, serum concentration determinations in steady state, severity of illness (CGI-S), treatment efficacy (CGI-I) and side effects (UKU scale) were analysed. Escitalopram: The mean daily dose was 14.8 mg, with serum concentrations varying between six and 109 ng/ml with a mean concentration of 32.2 ng/ml (SD= 26.6 ng/ml). In 63.4 % of patients, the serum concentration determined was within the therapeutic reference range defined for adults (15-80 ng/ml). There was a significant positive linear relationship between the daily dose and the serum concentration (rs= 0.46; p= 0.003). 65.9 % of patients responded since the start of treatment. No significant correlation was found between the serum concentration and the therapeutic effect (rs= 0.193; p= 0.282) and between the serum concentration and the side effects (r= 0.127; p= 0.467). The side effect rate was 25.7 %, with tension and restlessness being the most frequently documented. With the idea of taking into account the definition for the preliminary therapeutic reference range of both the AGNP consensus guideline (Hiemke et al., 2018) and Hiemke (2019), a lower limit of between 10 ng/ml and 15 ng/ml and an upper limit of 50 ng/ml is proposed as the preliminary therapeutic reference range for escitalopram for children and adolescents with depression. This range is lower than the range for escitalopram defined for adult patients of 15 to 80 ng/ml. Mirtazapine: The mean daily dose was 28.6 mg, with serum concentrations varying between 13 and 130 ng/ml with a mean concentration of 40.8 ng/ml (SD= 28.1 ng/ml). For 52.2 % of patients, the serum concentration was within the therapeutic reference range defined for adults (30-80 ng/ml). There was a significant positive correlation between the daily dose and the serum concentration (rs= 0.655; p= 0.001). With regard to the treatment effect, 52.2 % of patients responded since the start of treatment. There was a significant positive correlation between the serum concentration and the therapeutic effect (rs= 0.534; p= 0.015). No significant correlation was found between the serum concentration and the side effects (r= 0.240; p= 0.282). The adverse event rate was 30.4%, with drowsiness and sedation being the most frequently reported. A lower limit of 15 ng/ml to 20 ng/ml and an upper limit of 50 ng/ml is proposed as a preliminary therapeutic reference range for mirtazapine for children and adolescents with depression. This range is lower than the range for mirtazapine defined for adult patients of 30 to 80 ng/ml. Bearing in mind the limitations of the present naturalistic study, the results should be interpreted with caution and verified using a larger sample size under more controlled conditions. KW - Arzneimittelüberwachung KW - Therapeutisches Drug Monitoring KW - Kinder und Jugendliche KW - Therapeutic Drug Monitoring KW - Children and Adolescents KW - Escitalopram and Mirtazapine KW - Kind KW - Jugend KW - Escitalopram KW - Mirtazapin Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-370222 ER - TY - THES A1 - Kawan, Mona T1 - The membrane trafficking protein myoferlin is a novel interactor of p97 T1 - Das Membrantransportprotein Myoferlin ist ein neuer Interaktor von p97 N2 - p97 uses the energy of ATP hydrolysis to unfold and thereby segregate proteins. It is involved in various cellular processes such as proteasomal degradation, DNA damage repair, autophagy, and endo-lysosomal trafficking. The specificity for these processes is controlled by more than 30 regulatory cofactors. Interactions of p97 with cofactors and target proteins are known to be highly dynamic and transient. To identify new interaction partners and to uncover novel cellular functions of p97, the interactome of endogenous p97 was determined by using in cellulo crosslinking followed by immunoprecipitation and mass spectrometry. Myoferlin (MYOF) was identified as a novel interactor of p97 and the interaction was validated in reciprocal immunoprecipitation experiments for different cell lines. The ferlin family member MYOF is a tail-anchored membrane protein containing multiple C2 domains. MYOF is involved in various membrane repair and trafficking processes such as the endocytic recycling of cell surface receptors. The MYOF interactome was determined by mass spectrometry. Among others, the p97 cofactor PLAA, CD71 and Rab14 were identified as common interactors of p97 and MYOF. Immunoprecipitation experiments with PLAA KO cells revealed that the interaction between MYOF and p97 depends on PLAA. Immunofluorescence microscopy showed a co-localization of MYOF with Rab14 and Rab11, which are both involved in endocytic recycling pathways. Furthermore, immunofluoroscence experiments revealed that MYOF and the p97 cofactor PLAA are localized to Rab14- and Rab5-positive endosomal compartments. Using p97 inhibitors and p97 trapping mutants, the presence of p97 at MYOF-positive and Rab14-positive structures could be demonstrated. Consistent with this finding, the endocytic recycling of transferrin was delayed upon inhibition of p97. Taken together, this work identified MYOF as a novel interactor of p97 and suggests a role for p97 in the recycling of endocytic cargo. N2 - p97 nutzt die aus der ATP-Hydrolyse gewonnene Energie, um Proteine zu entfalten und dadurch zu trennen. Es ist an verschiedenen zellulären Prozessen wie dem proteasomalen Abbau, der Reparatur von DNA-Schäden, der Autophagie und dem endo-lysosomalen Transport beteiligt. Die Spezifität für diese Prozesse wird durch mehr als 30 regulatorische Cofaktoren gesteuert. Wechselwirkungen von p97 mit Cofaktoren und Zielproteinen sind bekanntermaßen hochdynamisch und treten oft nur vorübergehend auf. Um neue Interaktionspartner zu identifizieren und neue zelluläre Funktionen von p97 aufzudecken, wurde das Interaktom von endogenem p97 unter Verwendung von in cellulo crosslinking, gefolgt von IP und Massenspektrometrie bestimmt. Dabei wurde MYOF als neuartiger Interaktor von p97 entdeckt und diese Interaktion wurde in reziproken IP-Experimenten und für verschiedene Zelllinien bestätigt. MYOF gehört der Ferlin Familie an und besitzt mehrere C2-Domänen sowie eine Trans-membrandomäne. MYOF ist bekanntermaßen an verschiedenen Membranreparatur- und Transportvorgängen wie beispielsweise dem endozytischen Recycling von Zelloberflächenrezeptoren beteiligt. Das Interaktom von MYOF wurde durch Massenspektrometrie bestimmt. Dabei wurden unter anderem der p97 Cofaktor PLAA, CD71 und Rab14 als gemeinsame Interaktoren von p97 und MYOF identifiziert. Durch IP-Experimente mit PLAA KO Zellen wurde eine Abhängigkeit der Interaktion zwischen MYOF und p97 von PLAA nachgewiesen. Mit IF-Mikroskopie konnte eine Kolokalisation von MYOF mit Rab14 und Rab11, die beide an endosomalen Recycling-Wegen beteiligt sind, beobachtet werden. Des Weiteren zeigten IF-Experimente, dass MYOF und der p97-Cofaktor PLAA an Rab14- und Rab5-positiven endosomalen Kompartimenten lokalisiert sind. Durch die Verwendung von p97-Inhibitoren oder p97 Mutanten, die ATP nicht hydrolysieren können und so verstärkt Substrate anreichern, konnte gezeigt werden, dass p97 an MYOF-positiven und Rab14-positiven Strukturen nachgewiesen werden kann. In Übereinstimmung mit diesem Befund wurde das endozytische Recycling von Transferrin durch die Inhibierung von p97 verzögert. Zusammengefasst zeigt diese Arbeit, dass MYOF ein neuer Interaktor von p97 ist, und deutet auf eine Rolle von p97 beim Recycling von endozytischer Fracht hin. KW - Endosom KW - p97 KW - Myoferlin Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-281218 ER - TY - THES A1 - Völter, Maximilian Friedrich T1 - In vitro-Analyse der Auswirkungen einer Methioninrestriktion auf die Proliferation von Myelomzellen des murinen Modellsystems MPC11 und der humanen Zelllinien L363 und KMS12-BM T1 - In vitro analysis of the effects of methionine restriction on the proliferation of myeloma cells of the murine model system MPC11 and the human cell lines L363 and KMS12-BM N2 - Trotz zahlreicher medizinischer Fortschritte sind Krebserkrankungen weiterhin eine der häufigsten Todesursachen weltweit (Bhupender S. Chhikara und Keykavous Parang 2023). Dabei ist das Multiple Myelom (MM) die zweithäufigste Krebserkrankung des blutbildenden Systems und für ca. 20% aller Todesfälle durch hämatologische Erkrankungen verantwortlich (Derlin und Bannas 2014). Die Krankheit gilt als schwer heilbar, die Patienten leiden unter schwerwiegenden Symptomen und die aktuelle Standardtherapie mittels hochdosierter Chemotherapeutika geht mit starken Nebenwirkungen einher (Cowan et al. 2022). Insofern besteht ein großes Interesse daran, neue und ergänzende Behandlungsmethoden zu finden. In der Forschung etablierte und bereits mit vielversprechenden Ergebnissen an Menschen mit anderen Krebserkrankungen getestete Verfahren sind die Methionin- (MetR) (Kaiser 2020) bzw. Cysteinrestriktion (CysR) (Garcia-Bermudez et al. 2020). Deshalb wurde in der vorliegenden Arbeit in vitro überprüft, ob diese Methoden grundsätzlich einen möglichen Ansatz für die Therapie des MM darstellen. Untersucht wurden die murine MPC11- sowie die humanen L363- und KMS12-BM-Zelllinien des MM. Dabei konnte die antiproliferative Wirkung der Restriktionen bestätigt werden. Darüber hinaus wurde nachgewiesen, dass der Mangel der Aminosäuren nicht über endogene Stoffwechselwege kompensiert werden kann, die Zellen also von der exogenen Zufuhr abhängig sind. Des Weiteren wurde das Metabolom der MPC11-Zellen unter MetR massenspektrometrisch analysiert und ein charakteristischer „metaboler Fingerabdruck“ erstellt. Die Proliferationshemmung ohne Rückgang der Zellzahlen unter den Anfangswert zusammen mit den die gesunde Morphologie der Zellen dokumentierenden EVOS Bildern belegt das Vorliegen eines Low-Energy-Metabolismus (LEM) ohne Absterben der Zellen (Schmitz et al. 2021a). Als geeignete Marker (charakteristischer „metabolen Fingerabdruck“) für einen MetR induzierten LEM eignen sich das bereits in L929-Zellen herauskristallisierte Absinken des Kreatins, der Aminosäuren und Purine bzw. Pyrimidine sowie der Anstieg des Acetoacetats. In den MPC11-Zellen kommen zusätzlich eine Zunahme der Folsäure und eine Abnahme des SAM, SAH und MTA aus dem Methionin- bzw. MTA-Zyklus, des Pentose-5-Phosphats aus dem Pentose-Phosphat-Weg und des Hexose- und Glyceralphosphats sowie des Pyruvats und des Laktats aus der Glykolyse hinzu. Kein klassischer Marker für einen LEM, aber aufgrund des signifikanten Anstiegs dennoch als auffällige Abweichung unter MetR zusätzlich erwähnenswert, ist der deutliche Anstieg des Cystins. N2 - Despite numerous medical advances, cancer remains one of the most common causes of death worldwide (Bhupender S. Chhikara and Keykavous Parang 2023). Multiple myeloma (MM) is the second most common cancer of the haematopoietic system and is responsible for around 20% of all deaths from haematological diseases (Derlin and Bannas 2014). The disease is considered difficult to cure, patients suffer from severe symptoms and the current standard therapy using high-dose chemotherapeutic agents is associated with severe side effects (Cowan et al. 2022). There is therefore great interest in finding new and complementary treatment methods. Methionine restriction (MetR) (Kaiser 2020) and cysteine restriction (CysR) (Garcia-Bermudez et al. 2020) are established research methods that have already been tested with promising results in humans with other cancer entities. This study therefore examined in vitro whether these methods also represent a possible approach for the treatment of MM. The murine MPC11 and the human L363 and KMS12 BM cell lines of MM were investigated. The antiproliferative effect of the restrictions was confirmed. In addition, it was demonstrated that the deficiency of amino acids cannot be compensated via endogenous metabolic pathways, i.e. the cells are dependent on exogenous supply. Furthermore, the metabolome of the MPC11 cells was analysed by mass spectrometry under MetR and a characteristic "metabolic fingerprint" was defined. The inhibition of proliferation without a decrease in cell numbers below the initial value together with the EVOS images documenting the healthy morphology of the cells confirms the presence of low-energy metabolism (LEM) without cell death (Schmitz et al. 2021a). Suitable markers (characteristic "metabolic fingerprint") for a MetR-induced LEM are the decrease in creatine, amino acids and purines or pyrimidines already shown in L929 cells and the increase in acetoacetate. In the MPC11 cells, there is also an increase in folic acid and a decrease in SAM, SAH and MTA from the methionine and MTA cycle, pentose-5-phosphate from the pentose-phosphate pathway and hexose and glyceral phosphate as well as pyruvate and lactate from glycolysis. The marked increase in cystine is not a classic marker for an LEM, but due to the significant increase it is nevertheless worth mentioning as a conspicuous deviation under MetR. KW - Methioninbedarf KW - Multiples Myelom KW - Methioninrestriktion KW - Cysteinrestriktion KW - Plasmozytom Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-369832 ER - TY - JOUR T1 - Search for new phenomena in events with same-charge leptons and b-jets in pp collisions at √\(s\) = 13 TeV with the ATLAS detector JF - Journal of High Energy Physics N2 - A search for new phenomena in events with two same- charge leptons or three leptons and jets identi fi ed as originating from b - quarks in a data sample of 36.1 fb of pp collisions at ps = 13TeV recorded by the ATLAS detector at the Large Hadron Collider is reported. No signi fi cant excess is found and limits are set on vector- like quark, fourtop- quark, and same- sign top- quark pair production. The observed ( expected) 95% CL mass limits for a vector- like T - and B - quark singlet are mT > 0 : 98 ( 0 : 99) TeV and mB > 1 : 00 ( 1 : 01) TeV respectively. Limits on the production of the vector- like T5=3 - quark are also derived considering both pair and single production; in the former case the lower limit on the mass of the T5=3 - quark is ( expected to be) 1.19 ( 1.21) TeV. The Standard Model fourtop- quark production cross- section upper limit is ( expected to be) 69 ( 29) fb. Constraints are also set on exotic four- top- quark production models. Finally, limits are set on samesign top- quark pair production. The upper limit on uu ! tt production is ( expected to be) 89 ( 59) fb for a mediator mass of 1TeV, and a dark- matter interpretation is also derived, excluding a mediator of 3TeV with a dark- sector coupling of 1.0 and a coupling to ordinary matter above 0.31. KW - Hadron-Hadron scattering (experiments) KW - SUSHI Y1 - 2018 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-312681 VL - 12 IS - 39 ER -