@phdthesis{Herz2021, author = {Herz, Michaela}, title = {Genome wide expression profiling of Echinococcus multilocularis}, doi = {10.25972/OPUS-20380}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-203802}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2021}, abstract = {Alveolar echinococcosis, which is caused by the metacestode stage of the small fox tapeworm Echinococcus multilocularis, is a severe zoonotic disease with limited treatment options. For a better understanding of cestode biology the genome of E. multilocularis, together with other cestode genomes, was sequenced previously. While a few studies were undertaken to explore the E. multilocularis transcriptome, a comprehensive exploration of global transcription profiles throughout life cycle stages is lacking. This work represents the so far most comprehensive analysis of the E. multilocularis transcriptome. Using RNA-Seq information from different life cycle stages and experimental conditions in three biological replicates, transcriptional differences were qualitatively and quantitatively explored. The analyzed datasets are based on samples of metacestodes cultivated under aerobic and anaerobic conditions as well as metacestodes obtained directly from infected jirds. Other samples are stem cell cultures at three different time points of development as well as non-activated and activated protoscoleces, the larval stage that can develop into adult worms. In addition, two datasets of metacestodes under experimental conditions suitable for the detection of genes that are expressed in stem cells, the so-called germinative cells, and one dataset from a siRNA experiment were analyzed. Analysis of these datasets led to expression profiles for all annotated genes, including genes that are expressed in the tegument of metacestodes and play a role in host-parasite interactions and modulation of the host's immune response. Gene expression profiles provide also further information about genes that might be responsible for the infiltrative growth of the parasite in the liver. Furthermore, germinative cell-specific genes were identified. Germinative cells are the only proliferating cells in E. multilocularis and therefore of utmost importance for the development and growth of the parasite. Using a combination of germinative cell depletion and enrichment methods, genes with specific expression in germinative cells were identified. As expected, many of these genes are involved in translation, cell cycle regulation or DNA replication and repair. Also identified were transcription factors, many of which are involved in cell fate commitment. As an example, the gene encoding the telomerase reverse transcriptase (TERT) was studied further. Expression of E. multilocularis tert in germinative cells was confirmed experimentally. Cell culture experiments indicate that TERT is required for proliferation and development of the parasite, which makes TERT a potentially interesting drug target for chemotherapy of alveolar echinococcosis. Germinative cell specific genes in E. multilocularis also include genes of densoviral origin. More than 20 individual densovirus loci with information for non-structural and structural densovirus proteins were identified in the E. multilocularis genome. Densoviral elements were also detected in many other cestode genomes. Genomic integration of these elements suggests that densovirus-based vectors might be suitable tools for genetic manipulation of tapeworms. Interestingly, only three of more than 20 densovirus loci in the E. multilocularis genome are expressed. Since the canonical piRNA pathway is lacking in cestodes, this raises the question about potential silencing mechanisms. Exploration of RNA-Seq information indicated natural antisense transcripts as a potential gene regulation mechanism in E. multilocularis. Preliminary experiments further suggest DNA-methylation, which was previously shown to occur in platyhelminthes, as an interesting avenue to explore in future. The transcriptome datasets also contain information about genes that are expressed in differentiated cells, for example the serotonin transporter gene that is expressed in nerve cells. Cell culture experiments indicate that serotonin and serotonin transport play an important role in E. multilocularis proliferation, development and survival. Overall, this work provides a comprehensive transcription data atlas throughout the E. multilocularis life cycle. Identification of germinative cell-specific genes and genes important for host-parasite interactions will greatly facilitate future research. A global overview of gene expression profiles will also aide in the detection of suitable drug targets and the development of new chemotherapeutics against alveolar echinococcosis.}, subject = {Fuchsbandwurm}, language = {en} } @phdthesis{Vollmuth2021, author = {Vollmuth, Nadine}, title = {Role of the proto-oncogene c-Myc in the development of Chlamydia trachomatis}, doi = {10.25972/OPUS-20365}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-203655}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2021}, abstract = {Chlamydia trachomatis, an obligate intracellular human pathogen, is the world's leading cause of infection related blindness and the most common, bacterial sexually transmitted disease. In order to establish an optimal replicative niche, the pathogen extensively interferes with the physiology of the host cell. Chlamydia switches in its complex developmental cycle between the infectious non-replicative elementary bodies (EBs) and the non-infectious replicative reticulate bodies (RBs). The transformation to RBs, shortly after entering a host cell, is a crucial process in infection to start chlamydial replication. Currently it is unknown how the transition from EBs to RBs is initiated. In this thesis, we could show that, in an axenic media approach, L glutamine uptake by the pathogen is crucial to initiate the EB to RB transition. L-glutamine is converted to amino acids which are used by the bacteria to synthesize peptidoglycan. Peptidoglycan inturn is believed to function in separating dividing Chlamydia. The glutamine metabolism is reprogrammed in infected cells in a c-Myc-dependent manner, in order to accomplish the increased requirement for L-glutamine. Upon a chlamydial infection, the proto-oncogene c-Myc gets upregulated to promote host cell glutaminolysis via glutaminase GLS1 and the L-glutamine transporter SLC1A5/ASCT2. Interference with this metabolic reprogramming leads to limited growth of C. trachomatis. Besides the active infection, Chlamydia can persist over a long period of time within the host cell whereby chronic and recurrent infections establish. C. trachomatis acquire a persistent state during an immune attack in response to elevated interferon-γ (IFN-γ) levels. It has been shown that IFN-γ activates the catabolic depletion of L-tryptophan via indoleamine 2,3-dioxygenase (IDO), resulting in the formation of non-infectious atypical chlamydial forms. In this thesis, we could show that IFN-γ depletes the key metabolic regulator c-Myc, which has been demonstrated to be a prerequisite for chlamydial development and growth, in a STAT1-dependent manner. Moreover, metabolic analyses revealed that the pathogen de routs the host cell TCA cycle to enrich pyrimidine biosynthesis. Supplementing pyrimidines or a-ketoglutarate helps the bacteria to partially overcome the persistent state. Together, the results indicate a central role of c-Myc induced host glutamine metabolism reprogramming and L-glutamine for the development of C. trachomatis, which may provide a basis for anti-infectious strategies. Furthermore, they challenge the longstanding hypothesis of L-tryptophan shortage as the sole reason for IFN-γ induced persistence and suggest a pivotal role of c-Myc in the control of the C. trachomatis dormancy.}, language = {en} } @phdthesis{Frischholz2021, author = {Frischholz, Sebastian}, title = {Resveratrol Counteracts IL-1β-mediated Impairment of Extracellular Matrix Deposition in 3D Articular Chondrocyte Constructs}, doi = {10.25972/OPUS-23745}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-237453}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2021}, abstract = {Articular cartilage is an exceptional connective tissue which by a network of fibrillar collagen and glycosaminoglycan (GAG) molecules allows both low- friction articulation and distribution of loads to the subchondral bone (Armiento et al., 2018, Ulrich-Vinther et al., 2003). Because of its very limited ability to self-repair, chondral defects following traumatic injury increase the risk for secondary osteoarthritis (OA) (Muthuri et al., 2011). Still, current OA treatments such as common nonsteroidal anti-inflammatory drugs (NSAIDs) and joint replacement primarily address end-stage symptoms (Tonge et al., 2014). As low-grade inflammation plays a pivotal role in the pathogenesis of OA (Robinson et al., 2016), there is a strong demand for novel therapeutic concepts, such as integrating application of anti-inflammatory agents into cartilage cell- based therapies in order to effectively treat OA affected joints in early disease stages. The polyphenolic phytoalexin resveratrol (RSV), found in the skin of red grapes, berries, and peanuts, has been shown to have effective anti-inflammatory properties (Shen et al., 2012). However, its long-term effects on 3D chondrocyte constructs cultured in an inflammatory environment with regard to tissue quality have remained unexplored so far. Therefore, in this study, pellets made from expanded porcine articular chondrocytes were cultured for 14 days with either the pro-inflammatory cytokine interleukin-1β (IL-1β) (1 - 10 ng/ml) or RSV (50 μM) alone, or a co-treatment with both agents. Constructs treated with chondrocyte medium only served as control. Treatment with IL-1β at 10 ng/ml resulted in a significantly smaller pellet size and reduced DNA content. However, RSV counteracted the IL-1β-induced decrease and significantly enhanced diameter and DNA content. Also, in terms of GAG deposition, treatment with IL-1β at 10 ng/ml resulted in a tremendous depletion of absolute GAG content and GAG/DNA. Again, RSV co-treatment counteracted the inflammatory stimulus and led to a partial recovery of GAG content. Histological analysis utilizing safranin-O staining confirmed these findings. Marked expression of the cartilage-degrading enzyme matrix metalloproteinase 13 (MMP13) was detected in IL-1β-treated pellets, but none upon RSV co- treatment. Moreover, co-treatment of IL-1β-challenged constructs with RSV significantly increased absolute collagen content. However, under non- inflammatory conditions, RSV induced gene expression and protein accumulation of collagen type X, a marker for undesirable hypertrophy. Taken together, in the present thesis, RSV was demonstrated to elicit marked beneficial effects on the extracellular matrix composition of 3D cartilaginous constructs in long-term inflammatory culture in vitro, but also induced hypertrophy under non-inflammatory conditions. Based on these findings, further experiments examining multiple concentrations of RSV under various inflammatory conditions appear desirable concerning potential therapeutic applicability in OA.}, subject = {Resveratrol}, language = {en} } @phdthesis{Qureischi2021, author = {Qureischi, Musga}, title = {Selective modulation of alloreactive T cells in preclinical models of acute Graft-versus-Host Disease}, doi = {10.25972/OPUS-23603}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-236031}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2021}, abstract = {Hematopoietic cell transplantation (HCT) is a curative therapy for the treatment of malignant and non-malignant bone marrow diseases. The major complication of this treatment is a highly inflammatory reaction called Graft-versus-Host Disease (GvHD). Here, transplanted donor T cells cause massive tissue destruction and inflammation in the main target organs liver, skin and the intestine. Currently, this inflammatory reaction can be treated successfully using strong immunosuppressive agents. One efficient group of immunosuppressants are calcineurin inhibitors such as Cyclosporin A (CsA) and Tacrolimus (FK506). These treatment strategies target all T lymphocytes subsets equally and do not separate GvH from the desirable Graft-versus-Leukemia (GvL) effect. Therefore, we aimed to find immunological targets on alloreactive T cells in order to develop novel treatment strategies, which selectively modulates alloreactive T cells without impairing the GvL effect or hematopoietic immune reconstitution. The aim of this thesis was to develop a predictive marker panel to track alloreactive T cells in the peripheral blood (PB) of murine allo-HCT recipients. In clinically relevant model of aGvHD we demonstrated that alloreactive T cells have a distinct surface marker expression profile and can be detected in the PB before aGvHD manifestation. Based on our data, we propose a combinatory panel consisting of 4 surface markers (a4b7 integrin, CD162E, CD162P und CD62L) on circulating CD8+ T cells to identify the risk of aGvHD after allo-HCT. Since tumor necrosis factor receptor superfamily (TNFR SF) members are involved in several immunological processes, we did extensive surface marker expression analysis of several TNFR superfamily members and other immunomodulatory molecules on conventional and regulatory T cells (Tcons vs. Tregs) on different time points during aGvHD progression. The aim of this study was to find subset-specific immunomodulatory molecules on recently activated Tcons and Tregs. We found that GITR, 4-1BB and CD27 were highly expressed on alloreactive and na{\"i}ve Tregs. In contrast, PD1 expression was highly upregulated on recently activated alloreactive Tcons. The data of this study serves as basis for future approaches, which aim to develop T cell subset specific therapeutic antibody fusion proteins. a4b7 integrin and CD162P (P-Selectin ligand) are highly upregulated on alloreactive T cells and mediate the infiltration of these cells into GvHD target organs. We developed recombinant (antibody) fusion proteins to target these two homing molecules and could show that antibody-based fusion proteins are superior to ligand-based fusion proteins regarding production efficiency and binding affinity. Therefore, we propose for future studies to focus on the described antibody-based fusion proteins for the selective targeting of T cells. Since the widely used calcineurin inhibitors are impairing the desirable GvL effect, we investigated if selective NFATc1 inhibition might be a novel strategy to prevent or reduce alloreactivity, while hopefully maintaining the GvL effect. In particular, we addressed the role of the isoform NFATc1 and inhibited its posttranslational modification by SUMO (Small Ubiquitin-related Modifier). Indeed, inhibition of NFATc1 SUMOylation resulted in reduced inflammation and increased Treg frequencies in a murine MHC major mismatch aGvHD model. Conclusively, we showed that alloreactive T cells can be identified by their surface profile in the PB of allo-HCT recipients before aGvHD symptoms appeared. Furthermore, we introduced a approach to selectively target alloreactive T cells by antibody fusion proteins, which might serve as a novel strategy to separate GvH from GvL. Additionally, we demonstrated that averted posttranslational modification of NFATc1 by SUMOylation serves as potential target to reduce alloreactivity of T cells.}, language = {en} } @phdthesis{Kuhn2021, author = {Kuhn, Johannes Helmut Max}, title = {IP\(_3\)-vermittelte Aktivierung des mitochondrialen Metabolismus}, doi = {10.25972/OPUS-23625}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-236259}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2021}, abstract = {Mit jedem Herzschlag werden enorme Mengen an Kalzium (Ca2+) in der Herzmuskelzelle freigesetzt. Dies geschieht vornehmlich {\"u}ber Ryanodinrezeptororen (RyR) und dient der Induktion der Muskelkontraktion. Daneben vermittelt aber auch der Inositoltrisphosphat (IP3)-Rezeptor, nach Aktivierung durch den Botenstoff IP3, unabh{\"a}ngig von der Elektromechanischen Kopplung eine Ca2+-Freisetzung aus dem sarkoplasmatischen Retikulum (SR). Die hier vorliegende Arbeit hatte das Ziel an isolierten Herzmuskelzellen die Interaktion von SR und Mitochondrien zu untersuchen, unter besonderer Ber{\"u}cksichtigung einer IP3-vermittelten Aktivierung des mitochondrialen Metabolismus. Wir verglichen den Effekt einer IP3- bzw. RyR-vermittelten zytosolischen Ca2+-Erh{\"o}hung auf die mitochondriale Ca2+-Aufnahme und Adenosintriphosphat (ATP)-Produktion. Sowohl unter den IP3-Rezeptor-Agonisten Endothelin-1 (ET-1) bzw. Angiotensin II (Ang II), als auch unter Verwendung des ß-Rezeptor-Agonisten Isoprenalin war eine mitochondriale Ca2+-Aufnahme nachweisbar, allerdings kam es nur IP3-abh{\"a}ngig zu einer ATP-Produktion. Unter Zugabe des IP3-Rezeptor-Blockers 2-Aminoethoxydiphenylborat (2-APB) konnte die zuvor nachgewiesene mitochondriale Ca2+-Aufnahme deutlich reduziert werden, gleiches zeigte sich bei Zellen isoliert aus transgenen IP3-sponge-M{\"a}usen, entsprechend einem funktionellen IP3-Knockout. Hinsichtlich des Mechanismus der mitochondrialen Ca2+-Aufnahme kamen prinzipell zwei Strukturen in Frage: der mitochondriale Ryanodinrezeptor (mRyR1) und der mitochondriale Ca2+-Kanal (MCU). Wir unternahmen in der Folge weitere Versuche mit den anerkannten Rezeptorblockern Ru360 bzw. Dantrolen, um wechselseitig den MCU oder den mRyR1 zu blockieren. Das Ergebnis dieser Versuchsreihe legt den Schluss nahe, dass die Ca2+-Aufnahme in die Mitochondrien nach betaadrenerger Stimulation mit Isoprenalin prim{\"a}r {\"u}ber den MCU vermittelt wird, demgegen{\"u}ber erfolgt die IP3-vermittelte Ca2+-Aufnahme {\"u}ber den mRyR1. Unter Verwendung von immunhistochemischer F{\"a}rbungen identifizierten wir den IP3-Rezeptor vom Typ III, der ein {\"u}berwiegend mitochondriales Verteilungsmuster aufzeigte. Wir schließen daraus, dass die von uns beobachteten Effekte der mitochondrialen Ca2+-Aufnahme und ATP-Produktion IP3-abh{\"a}ngig induziert werden bzw. zu einem Großteil auf eine Aktivit{\"a}t des IP3-Rezeptors, vermutlich der Unterform vom Typ III, zur{\"u}ckzuf{\"u}hren sind. Zusammenfassend konnte in der hier vorgelegten Arbeit gezeigt werden, dass die Aktivit{\"a}t des IP3-Rezeptors wesentlich am zellul{\"a}ren Energiehaushalt der Kardiomyozyten beteiligt ist. Der IP3-Signalweg vermittelt die Ca2+-Aufnahme in die Mitochondrien und f{\"u}hrt so zu einer Energiebereitstellung in Form von ATP.}, subject = {Inositoltrisphosphat}, language = {de} } @phdthesis{Balles2021, author = {Balles, Andreas}, title = {In-line phase contrast and grating interferometry at a liquid-metal-jet source with micrometer resolution}, doi = {10.25972/OPUS-23591}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-235917}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2021}, abstract = {As a non-destructive testing method, X-ray imaging has proved to be suitable for the examination of a variety of objects. The measurement principle is based on the attenuation of X-rays caused by these objects. This attenuation can be recorded as shades of intensity using X-ray detectors and thus contains information about the inner structure of the investigated object. Since X-rays are electromagnetic waves, they also experience a change of phase in addition to their attenuation while penetrating an object. In general, imaging methods based on this effect are referred to as phase contrast imaging techniques. In the laboratory, the two mainly used methods are the propagation based phase contrast or in-line phase contrast and the grating interferometry. While in-line phase contrast - under certain conditions - shows edge enhancement at interfaces due to interference, phase contrast in the grating interferometry is only indirectly measurable by the use of several gratings. In addition to phase contrast, grating interferometry provides access to the so-called dark-field imaging contrast, which measures the scattering of X-rays caused by an object. These two imaging techniques, together with a novel concept of laboratory X-ray sources, the liquid-metal-jet, form the main part of this work. Compared to conventional X-ray sources, the liquid-metal-jet source offers higher brightness. The term brightness is defined by the number of X-ray photons per second, emitting area (area of the X-ray spot) and solid angle at which they are emitted. On the basis of this source, a high resolution in-line phase contrast setup was partially developed in the scope of this work. Several computed tomographies show the feasibility of in-line phase contrast and the improvement of image quality by applying phase retrieval algorithms. Moreover, the determination of optimized sample positions for in-line phase contrast imaging is treated at which the edge enhancement is maximized. Based on primitive fiber objects, this optimization has proven to be a good approximation. With its high brightness in combination with a high spatial coherence, the liquid-metal-jet source is also interesting for grating interferometry. The development of such a setup is also part of this work. The overall concept and the characterization of the setup is presented as well as the applicability and its limits for the investigation of various objects. Due to the very unique concept of this grating interferometer it was possible to realize a modified interferometer system by using a single grating only. Its concept and results are also presented in this work. Furthermore, a grating interferometer based on a microfocus X-ray tube was tested regarding its performance. Thereby, parameters like the anode material, acquisition geometry and gratings were altered in order to find the advantages and disadvantages of each configuration.}, subject = {Phasenkontrastverfahren}, language = {en} } @phdthesis{Kraemer2021, author = {Kr{\"a}mer, Kristin}, title = {Organisationskultur und Gesundheit im Hochschulkontext}, doi = {10.25972/OPUS-23456}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-234562}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2021}, abstract = {Einleitung: Die gesamtgesellschaftlichen Ver{\"a}nderungen und der Wandel der Arbeit halten auch in den Hochschulen Einzug und stellen diese vor große Herausforderungen. Weitreichende und anhaltende Reformen sowie Ver{\"a}nderungsprozesse bed{\"u}rfen in den einzelnen Hochschulen Maßnahmen, um die Leistungsbereitschaft und die psychische Gesundheit der Besch{\"a}ftigten zu erhalten und zu f{\"o}rdern. Organisationskultur stellt einen wichtigen zu ber{\"u}cksichtigenden Faktor innerhalb diesen Wandels dar und ist in der Literatur ein oft benutztes Konzept zur Vorhersage der Leistungsf{\"a}higkeit in Wirtschafts-, aber auch Nonprofit - Organisationen. Bedeutsame Zusammenh{\"a}nge zwischen Organisationskultur und Gesundheit zeigen sich insbesondere in den ver- schiedenen Studien zum Bielefelder Sozialkapitalansatz. Im Hochschulkontext findet das Konzept Organisationskultur jedoch kaum Ber{\"u}cksichtigung. Um die Gestaltungsm{\"o}glichkeiten zu einer gesundheitsf{\"o}rderlichen und motivieren den Organisation aufzeigen zu k{\"o}nnen, war es das Ziel der vorliegenden Arbeit her- auszustellen, dass Hochschulen individuelle Organisationskulturen innehaben und Or- ganisationskultur auch im Hochschulkontext ein wichtiger Einflussfaktor f{\"u}r die Vorher- sage der psychischen Gesundheit und der Leistungsbereitschaft ist. Die Dissertation richtete sich an zwei Forschungsfragen aus: 1.Weisen Hochschulen spezifische Organisationskulturen auf? 2.Welche kulturellen Aspekte beeinflussen die psychische Gesundheit, sowie die motivationalen Aspekte von Hochschulmitarbeiter*innen? Methodik: Nach der theoretischen Einf{\"u}hrung in die Besonderheiten der Organisation Hochschule und der Darstellung des Bielefelder Sozialkapitalkonzepts mit Schwerpunkt auf der Organisationskultur wird auf Grundlage einer Fragebogenerhebung untersucht, ob sich die Hochschulen in ihren Auspr{\"a}gungen der Organisationskultur unterscheiden und ob diese eine Ressource f{\"u}r die psychische Gesundheit und einen Garanten f{\"u}r Leistungsbereitschaft darstellt. Der Einfluss der einzelnen Dimensionen von Organisationskultur wurde detailliert untersucht, um ein differenziertes Bild {\"u}ber die Wirkmechanismen zu erhalten und Handlungsempfehlungen ableiten zu k{\"o}nnen. Zus{\"a}tzlich wurde gepr{\"u}ft, ob der Zugang zur Ressource Organisationskultur von soziodemografischen Daten abh{\"a}ngig ist. Die Querschnittsanalyse basierte auf schriftlichen Befragungen an insgesamt 10 Hochschulen in Deutschland. In die Analyse wurden die Daten von 5453 Befragten eingeschlossen. Diese wurden mittels einer multiplen Imputation bearbeitet, um trotz fehlender Werte die inferenzstatistischen Verfahren umsetzen zu k{\"o}nnen. Die Datenanalyse erfolgte anhand uni-, bi- und schließlich multivariater Verfahren. Ergebnisse: Die Varianzaufkl{\"a}rung durch die Hochschulen in Bezug auf die Organisationskultur mittels Random-Intercept-Only-Modellen ergab f{\"u}r 2 von 3 Dimensionen signifikante Effekte (p < 0,05) mit einem ICC von 0,047 f{\"u}r die Ebene Dezernat / Fakult{\"a}t und einem ICC von 0,074 f{\"u}r die Ebene Hochschule. Die zentralen Ergebnisse der Zusammenhangsanalysen mittels multipler linearer Regressionen zeigen, dass Organisationskultur unter Adjustierung soziodemografischer Daten einen Einfluss auf die Aspekte der psychischen Gesundheit und der motivationalen Aspekte hat. Der Anteil aufgekl{\"a}rter Varianz f{\"u}r die Modelle bel{\"a}uft sich f{\"u}r die Vorhersagen zwischen R²kor = .092 f{\"u}r das Merkmal kognitiven Stresssymptome und R²kor = .361 f{\"u}r das Merkmal Arbeitszufriedenheit. Mittels einfacher linearer Regressionen konnte aufgezeigt wer- den, dass sowohl das Commitment als auch die Arbeitszufriedenheit Einfluss auf das Wohlbefinden, die depressive Verstimmung und die Ersch{\"o}pfungszust{\"a}nde haben. Die Haupteinflussfaktoren der Organisationskultur sind auf die Dimensionen Arbeitsbereich und Hochschule zur{\"u}ckzuf{\"u}hren. Hierzu z{\"a}hlen im Arbeitsbereich die Partizipation, das Vorhandensein gemeinsamer Ziele und Werte und der Umgang mit Problemen, f{\"u}r die Dimension Hochschule die gelebte Kultur und die Verl{\"a}sslichkeit der Hochschulleitung. Diskussion: Aufgrund der Ergebnisse kann angenommen werden, dass Hochschulen individuelle Organisationskulturen innehaben. Dies bietet den Entscheidungstr{\"a}gern der einzelnen Hochschulen individuelle Ansatzpunkte zur Gestaltung einer gesund- heitsf{\"o}rderlichen und motivierenden Organisationskultur. Es zeigt sich außerdem, dass die Organisationskultur auch im Hochschulkontext einen wichtigen Einflussfaktor f{\"u}r die psychische Gesundheit und die Leistungsbereitschaft der Mitarbeiter*innen darstellt. Insbesondere im Arbeitsbereich und auf Ebene der Hochschulleitung bestehen Ansatz- punkte, um eine an Mitarbeiter*innen orientierte, gesundheitsf{\"o}rderliche und motivierende Arbeitsumgebung f{\"u}r die Mitarbeiter*innen zu gestalten und zu f{\"o}rdern.}, subject = {Gesundheit}, language = {de} } @article{OberdorfHanftRamleretal.2021, author = {Oberdorf, Kai and Hanft, Anna and Ramler, Jacqueline and Krummenacher, Ivo and Bickelhaupt, Matthias and Poater, Jordi and Lichtenberg, Crispin}, title = {Bismuth Amides Mediate Facile and Highly Selective Pn-Pn Radical-Coupling Reactions (Pn=N, P, As)}, series = {Angewandte Chemie, International Edition}, volume = {60}, journal = {Angewandte Chemie, International Edition}, number = {12}, doi = {10.1002/anie.202015514}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-236582}, pages = {6441-6445}, year = {2021}, abstract = {The controlled release of well-defined radical species under mild conditions for subsequent use in selective reactions is an important and challenging task in synthetic chemistry. We show here that simple bismuth amide species [Bi(NAr\(_2\))\(_3\)] readily release aminyl radicals [NAr\(_2\)]. at ambient temperature in solution. These reactions yield the corresponding hydrazines, Ar\(_2\)N-NAr\(_2\), as a result of highly selective N-N coupling. The exploitation of facile homolytic Bi-Pn bond cleavage for Pn-Pn bond formation was extended to higher homologues of the pnictogens (Pn=N-As): homoleptic bismuth amides mediate the highly selective dehydrocoupling of HPnR\(_2\) to give R\(_2\)Pn-PnR\(_2\). Analyses by NMR and EPR spectroscopy, single-crystal X-ray diffraction, and DFT calculations reveal low Bi-N homolytic bond-dissociation energies, suggest radical coupling in the coordination sphere of bismuth, and reveal electronic and steric parameters as effective tools to control these reactions.}, language = {en} } @phdthesis{Traxler2021, author = {Traxler, Claudia}, title = {Untersuchung serumpiegelabh{\"a}ngiger unerw{\"u}nschter Arzneimittelwirkungen von selektiven Serotonin-R{\"u}ckaufnahme-Inhibitoren sowie Serotonin-Noradrenalin-R{\"u}ckaufnahme-Inhibitoren}, doi = {10.25972/OPUS-23594}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-235946}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2021}, abstract = {Hyponatri{\"a}mie, definiert als Serum-Natrium < 135 mmol/l, ist ein potentiell lebensbedrohender Zustand und wird h{\"a}ufig bei {\"a}lteren und psychiatrischen Patienten beobachtet. In den letzten Jahren wurden viele Case reports {\"u}ber SSRI- und SNRI- induzierte Hyponatri{\"a}mien publiziert. Kardiale Ver{\"a}nderungen, insbesondere eine verl{\"a}ngerte QT-Zeit oder erh{\"o}hte Herzfrequenz, werden auch als h{\"a}ufig beobachtete Nebenwirkungen unter Therapie mit Antidepressiva beschrieben. Dies konnte bislang insbesondere w{\"a}hrend der Einnahme von trizyklischen Antidepressiva beobachtet werden. Oft kann der beobachtete Effekt in Zusammenhang mit der verabreichten Dosis gebracht werden. Bei der SSRI- bzw. SNRI-induzierten Hyponatri{\"a}mie konnte dies bislang nicht gezeigt werden. In der Literatur lassen sich im Allgemeinen kaum Studien finden, die einen Zusammenhang der Serumkonzentration von SSRI und SNRI auf potentiell auftretende Nebenwirkungen untersucht haben. Ziel der vorliegenden Studie war zu zeigen, ob h{\"o}here Serumkonzentrationen von Citalopram, Escitalopram, Sertralin, Venlafaxin oder Duloxetin h{\"a}ufiger zu Hyponatri{\"a}mien bzw. Verl{\"a}ngerungen der QT-Zeit f{\"u}hren.}, subject = {Sertralin}, language = {de} } @phdthesis{Pilgram2021, author = {Pilgram, Sabine Christine}, title = {Komorbidit{\"a}ten bei Patienten mit PAH und CTEPH: Einfluss auf die Belastungsf{\"a}higkeit, auf klinische und h{\"a}modynamische Parameter sowie auf die Mortalit{\"a}t}, doi = {10.25972/OPUS-23585}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-235859}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2021}, abstract = {Die PAH sowie die CTEPH stellen schwerwiegende Erkrankungen des pulmonalen Gef{\"a}ßsystems dar. Der moderne PAH-Patienten des 21. Jahrhunderts wird zunehmend {\"a}lter. Der H{\"a}ufigkeitsgipfel der CTEPH-Erkrankung liegt zwischen dem 60. und 70. Lebensjahr. Aufgrund des fortgeschrittenen Alters leiden viele der Betroffenen an weiteren Komorbidit{\"a}ten, weshalb eine genauere Betrachtung der Auswirkungen auf Belastbarkeit, verschiedene klinische und h{\"a}modynamische Parameter sowie auf die Mortalit{\"a}t sinnvoll erscheint. Die vorliegende Arbeit basiert auf einer monozentrischen, retrospektiven Datenanalyse eines fortlaufenden Patientenkollektivs, bestehend aus 114 PAH-Patienten, 42 CTEPH-Patienten und einer Kontrollgruppe mit 99 Patienten ohne pulmonale Hypertonie. Zudem wurden PAH- und CTEPH-Patienten als gepooltes Kollektiv betrachtet und analysiert. Die Daten zeigen, dass verschiedene wichtige Parameter, wie die 6-Minuten-Gehstrecke, die Fl{\"a}che des linken und rechten Atriums, der NT-proBNP-Wert aber auch die TAPSE oder der mPAP durch Vorliegen h{\"a}ufiger Komorbidit{\"a}ten beeinflusst werden k{\"o}nnten. Auch Auswirkungen der Begleiterkrankungen auf die Mortalit{\"a}t der Betroffenen sind mit Verweis auf vorliegende Daten wahrscheinlich.}, subject = {Pulmonale Hypertonie}, language = {de} }