@phdthesis{Biggemann2014, author = {Biggemann, Lorenz}, title = {Untersuchungen zum antikanzerogenen Potenzial von Targetstrukturen im Stoffwechsel von Tumorzellen}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-132338}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2014}, abstract = {In der Onkologie bleibt das grundlegende Ziel, neue Strukturen zu identifizieren und ihre Eignung f{\"u}r therapeutische Ans{\"a}tze zu pr{\"u}fen. Seit einigen Jahren wird der Stoffwechsel von Tumoren als zur Entwicklung neuer Therapiestrategien untersucht, nachdem dieser bereits Anfang des 20. Jahrhunderts im Fokus des wissenschaftlichen Interesses stand. So berichtete der Nobelpreistr{\"a}ger Otto Warburg bereits im Jahr 1923 {\"u}ber eine starke Bildung von Milchs{\"a}ure an Gewebeschnitten solider Tumoren in Gegenwart von Sauerstoff. F{\"u}r diese Eigenschaft von Tumoren, die bei normalen K{\"o}rperzellen nicht beobachtet wird, hat sich die Bezeichnung „Warburg-Effekt" durchgesetzt, der als Anpassung an die in soliden Tumoren vorherrschenden Sauerstoffbedingungen interpretiert wird. Der Warburg-Effekt f{\"u}hrt dazu, dass Tumorzellen einen so genannten glykolytische Stoffwechsel aufweisen, der durch einen hohen Glukoseumsatz in der Glykolyse und eine massive Bildung von Laktat charakterisiert ist. Wird die Tumorzelle daran gehindert, die f{\"u}r die Glykolyse notwendigen Reduktions{\"a}quivalente mit Hilfe der Laktatdehydrogenase zu reoxidieren, verringert sich der Umsatz von Glukose {\"u}ber die Glykolyse und die Tumorzelle ger{\"a}t in ein Energiedefizit. Wird die Tumorzelle daran gehindert, Laktat aus dem Zellinne-ren {\"u}ber die Transporter MCT1 und MCT4 nach außen zu schleusen, so kommt es zu einer intrazellul{\"a}ren {\"U}bers{\"a}uerung. Beide Strategien f{\"u}hren zum Zelltod. Als Hemmstoff f{\"u}r die Zielstruktur Laktatdehydrogenase wurde Natri-umoxamat (NaOx) und als Hemmstoff f{\"u}r die Zielstruktur MCT1 bzw. MCT4 wurde α-Cyano-4-Hydroxyzimts{\"a}ure (CHC) gew{\"a}hlt. Ihre Wirkung auf die Zellvitalit{\"a}t und den Zellstoffwechsel wurde an der Zervixkarzinomzelllinie SiHa und der kolorektalen Adenokarzinomzelllinie WiDr untersucht, die beide sowohl die Laktatdehydrogenase LDH-A als auch die Monocarboxylat-Transporter MCT1 und MCT4 exprimieren. Die Untersuchungen zum Tumorstoffwechsel wurden bei Sauerstoffkonzentrationen von 5 \% und 1 \% durchgef{\"u}hrt. Bei SiHa war die Hemmung des Laktatexports durch den MCT-Inhibitor CHC erfolgreich und bewirkte eine starke Inhibition des Zellwachstums auch in Hypoxie (1 \% Sauerstoff). Die Inkubation mit CHC f{\"u}hrte bereits nach 48 Stunden zu zelltoxischen Effekten; nach 120 Stunden lag der Anteil vitaler Zellen nur noch bei 50 \%. Die CHC-vermittelte Hemmung der MCT verringerte bei SiHa den Verbrauch an Glukose um ca. 50 \% und die Produktion von Laktat um ca. 40 \% nach 24 Stunden. Auch bei WiDr wurden durch CHC ausgel{\"o}ste zelltoxische Effekte bereits nach 24 Stunden beobachtet. Die Hemmung der Laktatdehydrogenase verminderte in beiden Tumorzelllinien eindeutig die Laktatbildung und gleichzeitig den Glukoseverbrauch um mehr als 50 \% innerhalb von 24 Stunden. Dabei nahm die Wirksamkeit der LDH-Inhibition mit abnehmender Sauerstoffkonzentration zu. W{\"a}hrend das Zellwachstum bei 5 \% Sauerstoff verz{\"o}gert war, nahm bei 1 \% Sauerstoff der Anteil vitaler Zellen um ca. 50 \% ab. Die Daten zur Kombination aus Natriumoxamat und 5-FU belegen, dass die Inhibition der Laktatdehydrogenase die Wirksamkeit von 5-FU erh{\"o}ht und dass diese Kombination nicht nur bei 21 \% Sauerstoff wirksam ist, sondern auch bei der f{\"u}r Tumoren physiologisch relevanteren Sauerstoffkonzentration von 1 \%. Die Ergebnisse der vorliegenden Arbeit best{\"a}tigen als „proof of concept", dass die Hemmung der Laktatdehydrogenase und der MCT zur Inhibition des glykolytischen Stoffwechsels von Tumorzellen f{\"u}hrt. Weitere Untersuchungen sind zweifelsohne notwendig, um die molekularen Mechanismen im Detail zu verstehen, doch scheinen beide Strategien {\"u}ber das prinzipielle Potential zur Entwicklung einer neuartigen Form der Krebstherapie zu verf{\"u}gen. Dabei wird sicherlich von Bedeutung sein, dass beide Strategien insbesondere in Hypoxie, in der die Wirksamkeit von Chemotherapeutika und Strahlentherapie begrenzt ist, ebenfalls Effekte aufweisen.}, subject = {Tumorstoffwechsel}, language = {de} } @phdthesis{Wende2014, author = {Wende, Beate}, title = {Diversity of saproxylic beetles and host tree specialisation in differently managed forests across Germany}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-107049}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2014}, abstract = {Chapter I The gradual turnover of dead organic material into mineral nutrients is a key ecological function, linking decomposition and primary production, the essential parts of the nutrient-energy cycle. However, disturbances in terms of species or resource losses might impair the equilibrium between production and decomposition. Humanity has converted large proportions of natural landscapes and intensified land-use activity for food production. Globally, only very few areas are totally unaffected by human activity today. To ensure the maintenance of both essential ecosystem services, knowledge about the interplay of biodiversity and ecosystem functioning as well as effects of intensified management on both is crucial. The vast majority of terrestrial biomass production as well as decomposition take place in forest ecosystems. Though forestry has a long sustainable history in Europe, its intensification during the last century has caused severe impacts on forest features and, consequently, on the associated biota, especially deadwood dependent organisms. Among these, saproxylic beetles are the most diverse group in terms of species numbers and functional diversity, but also most endangered due to habitat loss. These features classify them as ideal research organisms to study effects of intensified forestry on ecosystem services. The BELONGDEAD project located in Germany aimed to investigate deadwood decay and functional consequences of diversity changes in the associated fauna on the decomposition process from the initialisation of deadwood decay to complete degradation. As part of the BeLongDead project, this dissertation focussed on saproxylic beetle species, thereby evaluating (1) regionally effects of tree species identity of fresh deadwood and (2) forest management of varying intensities on the diversity, abundance and community composition of saproxylic beetles (chapter II); (3) the specialisation degree of different trophic guilds of saproxylic beetles, and thus the stability and robustness of their interaction networks against disturbances (chapter III); (4) the impact of environmental features of local to regional spatial scales on species richness of saproxylic beetles differing in their habitat niche in terms of deadwood decay stages (chapter IV). Chapter II The vast majority of European forest ecosystems have been anthropogenically affected, leaving less than 1\% of the about 1 milliard hectare as natural forests. A long history of forestry and especially the technological progress during the last century have caused massive habitat fragmentation as well as substantial loss of essential resources in European forest ecosystems. Due to this, the substrate-dependent group of saproxylic beetles has experienced severe species losses. Thus, investigations concerning saproxylic diversity and deadwood volume were badly needed. However, the importance of different deadwood in terms of tree species identity for the colonization by saproxylic beetles under different local and regional management regimes is poorly understood. Therefore, we studied possible regional differences in colonization patterns of saproxylic beetle species in a total of 688 fresh deadwood logs of 13 tree species in 9 sites of managed conifer and beech forests, and unmanaged beech forests, respectively. We found that tree species identity was an important driver in determining saproxylic species composition and abundance within fresh deadwood. However, saproxylic species showed different colonization patterns of deadwood items of the same tree species among the study regions. Regionally consistent, conifer forests were most diverse. We attribute the latter result to the historically adaption of saproxylic beetle species to semi-open forests, which conditions are actually best reflected by conifer forests. To preserve a diverse local species pool of early successional saproxylic beetles, we suggest an equal high degree of deadwood diversity in a tree species context in due consideration of regional differences. Chapter III The extinction risk of a particular species corresponds with its species-specific requirements on resources and habitat conditions, in other words with the width of the species` ecological niche. Species with a narrow ecological niche are defined as specialists. Members of this group experience higher extinction risk by resource limitation than generalists, which are able to utilize a variety of resources. For the classification of species as specialists or generalists, thus evaluating possible extinction risks, ecologists use the concept of interaction networks. This method has often been applied for mutualistic or antagonistic plant-animal interactions, but information for networks of detritivores is scarce. Therefore, saproxylic beetle species sampled as described in chapter II were categorised according to their larval diet; additionally their interaction networks (N=108) with 13 dead host tree species were analysed. Specialisation degree was highest for wood-digesting beetles and decreased with increasing trophic level. Also the network indices evaluating robustness and generality indicated a higher susceptibility to species extinctions for xylophagous than for mycetophagous and predatory beetles. The specialisation of xylophagous species on specific tree species might be an adaption to tree species specific ingredients stored for defence against pathogens and pests. However, we conclude that the high specialisation degree of xylophages and thus their higher extinction risk by resource loss harbours certain dangers for ecosystem function and stability as species diversity is positively linked to both. Chapter IV Populations depend on individual emigration and immigration events to ensure genetic exchange. For successful migration it is of utmost importance that spatially separated populations are obtainable by specimen. Migratory success depends on the one hand on the species dispersal abilities and on the other on the availability of suitable habitats in the surrounding landscape in which the distinct host populations exist. However, consequences of intensive forest management correspond not only to severe reduction of local deadwood amount, but, among others, also a change in tree species composition and high levels of fragmentation in the surrounding forest area. Saproxylic beetle species differ in their dispersal behaviour according to the temporal availability of their preferred habitat. Generally, early successional saproxylic beetles are able to disperse over large distances, whereas beetles inhabiting advanced decayed wood often remain close to their larval habitat. Due to this, environmental factors might affect saproxylic beetle guilds differently. We classified the saproxylic beetles sampled as described in chapter II according to their calculated habitat niche as early, intermediate or late successional saproxylic beetles. For the different guilds the effects of 14 environmental factors on different spatial scales (stand factors at 0.1 km radius, landscape composition at 2 km radius, and regionally differing abiotic factors in 400 km to 700 km distance) were investigated. Consistently for all guilds, species richness decreased with fragmentation at local and landscape scale, and increased in warmer climate. However, we found contradictory results between the guilds to some extent. We relate this to guild specific habitat requirements of the saproxylic beetles. Therefore, for the development of appropriate conservation practices guild-specific requirements saproxylic beetles have to be considered not only locally but on larger spatial scales. Chapter V In conclusion, this dissertation identified main drivers of early successional saproxylic beetle species richness on various spatial scales. Our results emphasize the importance to develop management schemes meeting species-specific and guild-specific habitat requirements of the saproxylic beetle fauna at relevant spatial and temporal scales. Therefore, short-term actions suggested for sustainable forest management should be the focus on a diverse tree species composition consisting of indigenous tree species with respect to regional differences. Moreover, senescent trees, fallen and standing deadwood should remain in the forests, and some tree individuals should be allowed to grow old. Long-term actions should involve the reduction of forest fragmentation and the connection of spatial widely separated forest fragments. Furthermore, to fully understand the effects of forest management long-term research should be conducted to compare habitat requirements of intermediate and late successional beetles with the results presented in this dissertation.}, subject = {Saproxylophage}, language = {en} } @phdthesis{Sollfrank2015, author = {Sollfrank, Teresa}, title = {Feedback efficiency and training effects during alpha band modulation over the sensorimotor cortex}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-131769}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2015}, abstract = {Neural oscillations can be measured by electroencephalography (EEG) and these oscillations can be characterized by their frequency, amplitude and phase. The mechanistic properties of neural oscillations and their synchronization are able to explain various aspects of many cognitive functions such as motor control, memory, attention, information transfer across brain regions, segmentation of the sensory input and perception (Arnal and Giraud, 2012). The alpha band frequency is the dominant oscillation in the human brain. This oscillatory activity is found in the scalp EEG at frequencies around 8-13 Hz in all healthy adults (Makeig et al., 2002) and considerable interest has been generated in exploring EEG alpha oscillations with regard to their role in cognitive (Klimesch et al., 1993; Hanselmayr et al., 2005), sensorimotor (Birbaumer, 2006; Sauseng et al., 2009) and physiological (Lehmann, 1971; Niedermeyer, 1997; Kiyatkin, 2010) aspects of human life. The ability to voluntarily regulate the alpha amplitude can be learned with neurofeedback training and offers the possibility to control a brain-computer interface (BCI), a muscle independent interaction channel. BCI research is predominantly focused on the signal processing, the classification and the algorithms necessary to translate brain signals into control commands than on the person interacting with the technical system. The end-user must be properly trained to be able to successfully use the BCI and factors such as task instructions, training, and especially feedback can therefore play an important role in learning to control a BCI (Neumann and K{\"u}bler, 2003; Pfurtscheller et al., 2006, 2007; Allison and Neuper, 2010; Friedrich et al., 2012; Kaufmann et al., 2013; Lotte et al., 2013). The main purpose of this thesis was to investigate how end-users can efficiently be trained to perform alpha band modulation recorded over their sensorimotor cortex. The herein presented work comprises three studies with healthy participants and participants with schizophrenia focusing on the effects of feedback and training time on cortical activation patterns and performance. In the first study, the application of a realistic visual feedback to support end-users in developing a concrete feeling of kinesthetic motor imagery was tested in 2D and 3D visualization modality during a single training session. Participants were able to elicit the typical event-related desynchronisation responses over sensorimotor cortex in both conditions but the most significant decrease in the alpha band power was obtained following the three-dimensional realistic visualization. The second study strengthen the hypothesis that an enriched visual feedback with information about the quality of the input signal supports an easier approach for motor imagery based BCI control and can help to enhance performance. Significantly better performance levels were measurable during five online training sessions in the groups with enriched feedback as compared to a conventional simple visual feedback group, without significant differences in performance between the unimodal (visual) and multimodal (auditory-visual) feedback modality. Furthermore, the last study, in which people with schizophrenia participated in multiple sessions with simple feedback, demonstrated that these patients can learn to voluntarily regulate their alpha band. Compared to the healthy group they required longer training times and could not achieve performance levels as high as the control group. Nonetheless, alpha neurofeedback training lead to a constant increase of the alpha resting power across all 20 training session. To date only little is known about the effects of feedback and training time on BCI performance and cortical activation patterns. The presented work contributes to the evidence that healthy individuals can benefit from enriched feedback: A realistic presentation can support participants in getting a concrete feeling of motor imagery and enriched feedback, which instructs participants about the quality of their input signal can give support while learning to control the BCI. This thesis demonstrates that people with schizophrenia can learn to gain control of their alpha oscillations recorded over the sensorimotor cortex when participating in sufficient training sessions. In conclusion, this thesis improved current motor imagery BCI feedback protocols and enhanced our understanding of the interplay between feedback and BCI performance.}, subject = {Neurofeedback}, language = {en} } @phdthesis{Pusch2015, author = {Pusch, Tobias}, title = {The transcription factor NFATc1 mediates cytotoxic T cell function in vitro and in vivo}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-123690}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2015}, abstract = {While numerous experiments on NFAT were already performed with CD4+ T cells showing defective cytokine release and a reduced T helper cell development, no detailed studies existed for CD8+ T cells. From this point, we wanted to examine the impact of NFATc1 and c2 on the physiological functions of CD8+ T cells in vitro and in vivo. Therefore, we used a murine infection model with the bacteria Listeria monocytogenes and mice in which NFATc1 was specifically depleted in the T cell compartment. Our first in vitro studies showed a typical NFATc1 and c2 nuclear translocation and changes on mRNA levels upon T cell activation similarly in CD4+ as well as in CD8+ T cells extracted from wild type mice. NFAT nuclear translocation is important for target gene activation and generation of effector functions. Stimulated T cell populations lacking NFATc1 and/or NFATc2 showed a markedly decreased expression of Th1/Tc1 cytokines, as e.g. IL 2 and IFNγ being important for the clearance of intracellular pathogens. From our in vitro model for the generation of allogenically reactive cytotoxic CD8+ T cells, we revealed a decreased killing and lytic granule-release capacity in Nfatc1 inactivated CD8+ T cells whereas NFATc2-/- cytotoxic T cells did not show an altered cytotoxic response compared to wild type cells. Interestingly, we found lytic granules accumulated and mitochondria not getting translocated to the immunological synapse upon re-stimulation in NFATc1-deficient CD8+ T cells. Together with results showing the CsA insensitivity of the CTL killing/degranulation capacities, we assume that some major cellular processes are affected by NFATc1 which are not directly linked to the TCR-induced signal transduction cascade. We also showed the importance of NFATc1 in T cells during intracellular infections with the bacteria Listeria monocytogenes in an in vivo mouse model. After five days, only few bacteria were detected in wt mice whereas high amounts of Listeria particles were extracted from livers of Nfatc1fl/fl x Cd4 cre mice. Although the reactivity towards the pathogen was similar in both groups, a decreased cytokine expression in NFATc1-/- CD8+ T cells was observed together with an altered memory cell generation. Our results show the importance of NFATc1 in CD8+ T cells and give some clue for a possible connection to other basal cellular functions, as e.g. the formation of an immunological synapse.}, subject = {Transkriptionsfaktor}, language = {en} } @phdthesis{Praetorius2015, author = {Praetorius, Christian Michael}, title = {Ce M4,5 XAS and XMCD as Local Probes for Kondo and Heavy Fermion Materials - A Study of CePt5/Pt(111) Surface Intermetallics -}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-132504}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2015}, abstract = {The aim of the present thesis is to explore the potential of X-ray magnetic circular dichroism(XMCD) experiments on gaining new insights into Kondo and heavy fermion materials. XMCD, which is derived from X-ray absorption spectroscopy (XAS), allows probing magnetic polarization specific to the different elements in a material and to their atomic orbitals. In particular, at the Ce M4,5 edges the method is sensitive to the localized 4f level, which provides the magnetic impurity moment responsible for Kondo physics in Ce compounds. Hence, Ce M4,5 XMCD is ideally suited to investigate local magnetism in the presence of interaction of impurity and conduction electrons in such materials. As a model material, CePt5/Pt(111) surface intermetallics were chosen for the present study. This thin-film material can be prepared by well-defined procedures involving molecular beam epitaxy. Crystalline Ordered samples are obtained by exploiting the single-crystallinity of the Pt(111) substrate. The surface character of thin films ideally matches the probing depth of soft X-ray spectroscopy in the total electron yield mode. The XMCD and XAS experiments, taking into account dependence on temperature, angle of incidence, sample thickness and external magnetic field, revealed the presence of four relevant energy scales that influence the magnetic response: 1. The 4f level in CePt5/Pt(111) is subject to significant crystal field (CF) splitting, which leads to reorganization of the six j = 5/2 sublevels. The hexagonal symmetry of the crystal structure conserves mj as a good quantum number. The proposed CF scheme, which is derived from measurements of the paramagnetic susceptibility by XMCD as well as linear dichroism in XAS, consists of nearly degenerate |1/2> and |3/2> doublets with the |5/2> doublet excited by E5/2 = 15 ... 25 meV. 2. Single impurity Kondo interaction significantly couples the magnetic moments of the impurity and conduction electrons. A signature thereof is the f0 -> f1 contribution to Ce M4,5 XAS, the strength of which can be tuned by control of the sample thickness. This finding is in line with the observation of reduced effective 4f moments as detected by XMCD. 3. Ruderman-Kittel-Kasuya-Yosida (RKKY) interaction induces ferromagnetic correlations on the impurity lattice, which induces a positive Curie-Weiss temperature in the temperature-dependent inverse susceptibility. 4. Indications for the transition to a coherent heavy fermion state are found in the inverse susceptibility at T ~ 20 K; the ferromagnetic ground state is not observed. The fielddependence of the magnetic moment in the coherent state can be interpreted in terms of a metamagnetic transition. This allows studying basic characteristics of the renormalized band structure of a heavy fermion system by XMCD. The disentanglement of these different contributions to the 4f magnetism not only required extensive Ce M4,5 XAS and XMCD data, but also a thorough structural characterization of the material, a fundamental study of the Ce M4,5 line shape in relation to the degree of 4f hybridization and the development of a model for the paramagnetic susceptibility. The unit cell dimensions and sample morphology of CePt5/Pt(111) intermetallics were studied by low-energy electron diffraction (LEED) and scanning transmission electron microscopy (STEM). These experiments showed that well-defined intermetallic films form on top of the substrate. This lead to introduction of the film thickness t, measured in unit cells (u.c.), as a key feature to characterize the samples. Systematic LEED measurements in the thickness range t ~ 1 ... 15 u.c. allowed identification of six different phases, which could be interpreted as resulting from the same crystal structure with different rotational alignments and lattice constants. An accurate determination of the surface lattice constant at t ~ 3 u.c. could be achieved by interpretation of additional superstructure spots as arising from a well-defined combination of substrate and film lattices. The thicknessdependence of the lateral lattice constant could be explained in terms of lattice relaxation. Confirmation of the CePt5 stoichiometry and structure was performed by use of thicknessdependent XAS and a representative LEED-IV study. The results of this study indicate that the intermetallic films exhibit hexagonal CaCu5 structure over the entire range of thicknesses that were studied. The terminating layer consists purely of Pt with one additional Pt atom per unit cell compared to the bulk structure. The line shape of Ce M4,5 spectra was analyzed with the help of full multiplet calculations. Experimentally, characteristic variations of the line shape were observed with increasing f0 -> f1 contribution. The calculations show that these variations are not due to an admixture of j = 7/2 character to the ground state, as often stated in the literature. As alternatives, this observation can be explained by either considering an additional contribution to the spectrum or by assumption of an asymmetric lifetime profile. The model that was developed for the inverse paramagnetic susceptibility contains the hexagonal crystal field, magnetic coupling of the impurity moments in a mean field scheme and Kondo screening. The latter is included phenomenologically by screening factors for the effective moment. Assumption of doublet-specific screening factors, which means that the degree of Kondo interaction depends on the mj character of the 4f sublevels, allows satisfactory reproduction of the experimental data.}, subject = {Magnetischer R{\"o}ntgenzirkulardichroismus}, language = {en} } @phdthesis{Junker2015, author = {Junker, Markus}, title = {Development and characterization of monoclonal antibodies to GDF-15 for potential use in cancer therapy}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-132424}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2015}, abstract = {Background GDF-15 is a divergent member of the TGF-superfamily, which was first described as macrophage inhibitory cytokine-1 (MIC-1), revealing an immune modulatory function. GDF-15 is a soluble protein which is, under physiological conditions, highly expressed in the placenta and found in elevated levels in blood sera of pregnant women. Apart from the placenta, GDF-15 is expressed in healthy tissue, albeit to a lower extent and overexpressed in many solid tumors. A variety of different functions are attributed to GDF-15 in healthy as well as diseased humans. On the one hand, GDF-15 is required for successful pregnancy and low GDF-15 serum levels during pregnancy correlate with fetal abortion. On the other hand, overexpression of GDF-15, which can be observed in several malignancies is correlated with a poor prognosis. Furthermore, tumor derived GDF-15 leads to cancer associated anorexia-cachexia syndrome in mice. The aim of my PhD thesis was to further investigate the role of GDF-15 as an immune modulatory factor in cancer, in particular, by inhibiting the target molecule in vitro and in vivo. Therefore, the main focus was placed on the generation and characterization of monoclonal GDF-15 specific blocking antibodies, which were tested in vitro and in vivo, which represents a substantial part of my work. Results Here, GDF-15 was shown to be highly expressed in human gynecological cancer and brain tumors. We could then demonstrate that GDF-15 modulates effector immune cells in vitro. GDF-15 mediated a slight downregulation of the activating NKG2D receptor on NK and CD8+ T cells, which is crucial for proper anti-tumoral immune responses. Furthermore, we could demonstrate that GDF-15 reduces the adhesion of CD4+ and CD8+ T cells on endothelial cells in vitro. A negatively affected trans-endothelial migration of leukocytes into inflamed tissue could explain the low T cell infiltration in GDF-15 expressing tumors, which were observed in vivo, where mice bearing (shRNA mediated) GDF-15 deficient glioma cells revealed enhanced immune cell infiltrates in the tumor microenvironment, compared with the GDF-15 expressing control group. Those animals further exhibited a decreased tumor growth and prolonged survival. GDF-15 is a soluble protein, secreted by more than 50 \% of solid tumors and associated with grade of malignancy. Therefore a neutralizing monoclonal antibody to GDF-15 was assumed to be an auspicious therapeutically anti-cancer tool. Such an antibody was thus generated in GDF-15 knock out mice against human GFD-15. Amongst many clones, the GDF-15 antibody clone B1-23 was found to be applicable in Western Blot as well as in ELISA techniques, detecting a three-dimensional epitope of the mature GDF-15 dimer with high affinity and specificity. To enable the humanization for a later administration in humans, the variable regions of antibody B1-23 were identified by a special PCR method using degenerate primers and cloned into a sequencing vector. The sequence obtained thereby enabled the generation of chimeric and humanized B1-23 variants. After further comprehensive characterization, the original mouse antibody B1-23 as well as the chimeric antibody (ChimB1-23) and the humanized B1-23 antibody (H1L5) were applied in a melanoma xenograft study in vivo. None of the antibodies could significantly inhibit tumor growth. .However of utmost importance, body weight loss mediated by tumor derived GDF-15 could be significantly prevented upon administration of all three GDF-15 specific antibodies, which confirmed the antagonizing functionality of the immunoglobulin. Conclusion GDF-15 is a promising cancer target, involved in tumor progression and cancer related cachexia. A monoclonal GDF-15 antibody was generated, which served on one hand as a tool for molecular biological applications (Western Blot, ELISA, etc.) and on the other hand was applied as an antagonizing antibody in vitro and in vivo. Even though tumor growth inhibition by GDF-15 depletion in T cell deficient athymic mice failed using B1-23, the same antibody and derivates thereof (chimeric and humanized) impressively prevented tumor associated cachexia in UACC-257 melanoma bearing nude mice. The missing anti-tumor effect in our own melanoma model in nude mice can only partially be explained by the missing secondary immunity, in particular cytotoxic T cells, in the athymic animals, since in a similar melanoma model, performed by an external company, a tumor reduction in immunocompromised animals was observed, when B1-23 was administered. These findings support the idea that T cells are substantial for an effective tumor immunity and are in line with the results of the syngeneic, T cell comprising, mouse glioma model, where silencing of tumor expressed GDF-15 led to an enhanced intratumoral T cell infiltration and a prolonged survival. Taken together our data allow for the conclusion that tumor associated cachexia can be combatted with the GDF-15 antibody B1-23. Further, B1-23 might elicit direct anti-tumor effects in immune competent models, which contain T cells, rather than in an athymic, T cell deficient nude mouse model.}, subject = {Growth-differentiation Factor 15}, language = {en} } @phdthesis{Topczak2015, author = {Topczak, Anna Katharina}, title = {Mechanismen des exzitonischen Transports und deren Dynamik in molekularen D{\"u}nnschichten f{\"u}r die organische Photovoltaik}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-132280}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2015}, abstract = {Der Fokus dieser Arbeit liegt in der Untersuchung des exzitonischen Transports, sowie der Dynamik exzitonischer Zust{\"a}nde in organischen Halbleitern. Als fundamentale Fragestellung werden die inh{\"a}renten, materialspezifischen Parameter untersucht, welche Einfluss auf die Exzitonen-Diffusionsl{\"a}nge besitzen. Sowohl der Einfluss der strukturellen Ordnung als auch die fundamentalen exzitonischen Transporteigenschaften in molekularen Schichten werden anhand der archetypischen, morphologisch unterschiedlichen organischen Halbleiter Diindenoperylen (DIP), sowie dessen Derivaten, α-6T und C60 studiert. Die resultierende Filmbeschaffenheit wird mittels R{\"o}ntgendiffraktometrie (XRD) und Rasterkraftmikroskopie (AFM) analysiert, welche Informationen {\"u}ber die Morphologie, die strukturelle Ordnung und die Mikrostruktur der jeweiligen molekularen Schichten auf verschiedenen L{\"a}ngenskalen liefern. Um Informationen {\"u}ber die Exzitonen-Diffusion und die damit einhergehende Exzitonen- Diffusionsl{\"a}nge LD zu erhalten, wurde die Methode des Photolumineszenz (PL)-Quenchings gew{\"a}hlt. Um umfassende Informationen zur Exzitonen-Bewegung in molekularen D{\"u}nnschichten zu erhalten, wurde mit Hilfe der Femtosekunden-Transienten-Absorptionsspektroskopie (TAS) und der zeitkorrelierten Einzelphotonenz{\"a}hlung (TCSPC) die Dynamik angeregter Energiezust{\"a}nde und deren jeweiliger Lebensdauer untersucht. Beide Messverfahren gew{\"a}hren Einblicke in den zeitabh{\"a}ngigen Exzitonen-Transport und erm{\"o}glichen eine Bestimmung des Ursprungs m{\"o}glicher Zerfallskan{\"a}le. Die zentralen Ergebnisse dieser Arbeit zeigen zum einen eine Korrelation zwischen LD und der strukturellen Ordnung der Schichtmorphologie, zum anderen weist die temperaturunabh{\"a}ngige Exzitonen-Bewegung in hochgeordneten polykristallinen DIP-Filmen auf die M{\"o}glichkeit der Existenz eines koh{\"a}renten Exzitonen-Transports bei tiefen Temperaturen unterhalb von 80 K hin. Zeitaufgel{\"o}ste spektroskopische Untersuchungen lassen zudem auf ein breites Absorptionsband h{\"o}herer angeregter Zust{\"a}nde schließen und weisen eine h{\"o}here Exzitonen- Zustandsdichte in polykristallinen DIP-Schichten im Vergleich zu ungeordneten Filmen auf.}, subject = {Organische Solarzelle}, language = {de} } @phdthesis{Gnamlin2015, author = {Gnamlin, Prisca}, title = {Use of Tumor Vasculature for Successful Treatment of Carcinomas by Oncolytic Vaccinia Virus}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-119019}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2015}, abstract = {Tumor-induced angiogenesis is of major interest for oncology research. Vascular endothelial growth factor (VEGF) is the most potent angiogenic factor characterized so far. VEGF blockade was shown to be sufficient for angiogenesis inhibition and subsequent tumor regression in several preclinical tumor models. Bevacizumab was the first treatment targeting specifically tumor-induced angiogenesis through VEGF blockade to be approved by the Food and Drugs Administration (FDA) for cancer treatment. However, after very promising results in preclinical evaluations, VEGF blockade did not show the expected success in patients. Some tumors became resistant to VEGF blockade. Several factors have been accounted responsible, the over-expression of other angiogenic factors, the noxious influence of VEFG blockade on normal tissues, the selection of hypoxia resistant neoplastic cells, the recruitment of hematopoietic progenitor cells and finally the transient nature of angiogenesis inhibition by VEGF blockade. The development of blocking agents against other angiogenic factors like placental growth factor (PlGF) and Angiopoietin-2 (Ang-2) allows the development of an anti-angiogenesis strategy adapted to the profile of the tumor. Oncolytic virotherapy uses the natural propensity of viruses to colonize tumors to treat cancer. The recombinant vaccinia virus GLV-1h68 was shown to infect, colonize and lyse several tumor types. Its descendant GLV-1h108, expressing an anti-VEGF antibody, was proved in previous studies to inhibit efficiently tumor induced angiogenesis. Additional VACVs expressing single chain antibodies (scAb) antibodies against PlGF and Ang-2 alone or in combination with anti VEGF scAb were designed. In this study, VACV-mediated anti-angiogenesis treatments have been evaluated in several preclinical tumor models. The efficiency of PlGF blockade, alone or in combination with VEGF, mediated by VACV has been established and confirmed. PlGF inhibition alone or with VEGF reduced tumor burden 5- and 2-folds more efficiently than the control virus, respectively. Ang-2 blockade efficiency for cancer treatment gave controversial results when tested in different laboratories. Here we demonstrated that unlike VEGF, the success of Ang-2 blockade is not only correlated to the strength of the blockade. A particular balance between Ang-2, VEGF and Ang-1 needs to be induced by the treatment to see a regression of the tumor and an improved survival. We saw that Ang-2 inhibition delayed tumor growth up to 3-folds compared to the control virus. These same viruses induced statistically significant tumor growth delays. This study unveiled the need to establish an angiogenic profile of the tumor to be treated as well as the necessity to better understand the synergic effects of VEGF and Ang-2. In addition angiogenesis inhibition by VACV-mediated PlGF and Ang-2 blockade was able to reduce the number of metastases and migrating tumor cells (even more efficiently than VEGF blockade). VACV colonization of tumor cells, in vitro, was limited by VEGF, when the use of the anti-VEGF VACV GLV-1h108 drastically improved the colonization efficiency up to 2-fold, 72 hours post-infection. These in vitro data were confirmed by in vivo analysis of tumors. Fourteen days post-treatment, the anti-VEGF virus GLV-1h108 was colonizing 78.8\% of the tumors when GLV-1h68 colonization rate was 49.6\%. These data confirmed the synergistic effect of VEGF blockade and VACV replication for tumor regression. Three of the tumor cell lines used to assess VACV-mediated angiogenesis inhibition were found, in certain conditions, to mimic either endothelial cell or pericyte functions, and participate directly to the vascular structure. The expression by these tumor cells of e-selectin, p-selectin, ICAM-1 and VCAM-1, normally expressed on activated endothelial cells, corroborates our findings. These proteins play an important role in immune cell recruitment, and there amount vary in presence of VEGF, PlGF and Ang-2, confirming the involvement of angiogenic factors in the immuno-modulatory abilities of tumors. In this study VACV-mediated angiogenesis blockade proved its potential as a therapeutic agent able to treat different tumor types and prevent resistance observed during bevacizumab treatment by acting on different factors. First, the expression of several antibodies by VACV would prevent another angiogenic factor to take over VEGF and stimulate angiogenesis. Then, the ability of VACV to infect tumor cells would prevent them to form blood vessel-like structures to sustain tumor growth, and the localized delivery of the antibody would decrease the risk of adverse effects. Next, the blockade of angiogenic factors would improve VACV replication and decrease the immune-modulatory effect of tumors. Finally the fact that angiogenesis blockade lasts until total regression of the tumor would prevent the recovery of the tumor-associated vasculature and the relapse of patients.}, subject = {Vaccinia-Virus}, language = {en} } @phdthesis{Kirscher2014, author = {Kirscher, Lorenz}, title = {Melanogene rekombinante Vaccinia-Viren als diagnostisches und therapeutisches Agenz zur Tumorbehandlung}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-112074}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2014}, abstract = {Die g{\"a}ngigen therapeutischen Behandlungsmethoden f{\"u}r die verschiedensten Krebserkrankungen zeigen nach wie vor M{\"a}ngel bez{\"u}glich der Effizienz sowie zahlreiche Nebenwirkungen w{\"a}hrend und nach der Behandlung. Maßgeblich f{\"u}r diese Defizite ist die teilweise geringe Sensitivit{\"a}t der meisten konventionellen diagnostischen Systeme und damit einhergehend die oftmals zu sp{\"a}te Identifikation entarteter Gewebsbereiche. Zur L{\"o}sung dieser Problematik bieten onkolytische Vaccinia-Viren einen Ansatz, sowohl die Effizienz der Therapie wie auch die Diagnostik zu verbessern. In beiden F{\"a}llen sind die Tumorzell-spezifische Vermehrung der Viren und die M{\"o}glichkeit entscheidend, die Viren als Vektorsystem zur Expression therapeutischer oder diagnostischer Fremdgenkassetten zu nutzen. Um ein auf Vaccinia-Virus-basierendes Reportersystem zum diagnostischen Nachweis von Krebszellen mittels Tiefengewebs-Tomographie bereit zu stellen, wurden die f{\"u}r die murine Tyrosinase (mTyr) und das Tyrosinase-Helferprotein 1 (Tyrp1) kodierenden Gene in das Genom eines onkolytischen Vaccinia-Virus inseriert. Die Tyrosinase ist das Schl{\"u}sselenzym der Melaninsynthese. Bereits die solit{\"a}re Expression der Tyrosinase f{\"u}hrt in der transformierten Zelle zur Melaninproduktion. Das Tyrosinase-Helferprotein 1 ist an der Prozessierung und Stabilisierung der Tyrosinase beteiligt. Bereits in verschiedenen Studien konnte gezeigt werden, dass Melanin als Reportermolek{\"u}l f{\"u}r die Magnetresonanz sowie f{\"u}r die multispektrale optoakustische Tomographie einsetzbar ist. Es wurde deswegen angestrebt, die Kombination aus dem therapeutischen Potential des onkolytischen Vaccinia-Virus und der diagnostischen Anwendung des Melanins als Reporter auszunutzen. S{\"a}mtliche in dieser Arbeit aufgef{\"u}hrten rekombinanten Vaccinia-Viren (rVACV) wurden von der Firma Genelux Corporation zur Verf{\"u}gung gestellt und in dieser Arbeit hinsichtlich der therapeutischen Effizienz und des diagnostischen Potentials untersucht. In ersten Zellkultur-Versuchen wurde anhand verschiedener konstitutiv melanogener rVACV-Konstrukte festgestellt, dass die Kombination aus dem Vaccinia-Virus-spezifischen synthetic early/late Promotor und dem Enzym Tyrosinase (GLV-1h327) bzw. den Enzymen Tyrosinase und Tyrosinase-Helferprotein 1 (GLV-1h324) die h{\"o}chste Melaninsynthese-Rate zeigte. Anschließend wurde mittels der Bestimmung der spektralen Absorption und der Enzymaktivit{\"a}t der viral kodierten Melanin synthetisierenden Enzyme sowie mikroskopischer Analysen gezeigt, dass es mit diesen auf 8 Vaccinia-Virus-basierenden melanogenen Reportersystemen m{\"o}glich ist, die Melaninsynthese in nicht-melanogenen Zellen zu induzieren. Anhand elektronenmikroskopischer Untersuchungen in Zellkultur und ex vivo konnte gezeigt werden, dass die nach rVACV-Infektion stattfindende Melaninsynthese in den Lysosomen der Wirtszelle abl{\"a}uft. Eine Analyse der atomaren Zusammensetzung des viral vermittelten Melanins ergab, dass es sich um eine Mischform aus Eu- und Ph{\"a}omelanin handelt. Dieser Melanin-Mix {\"a}hnelte dem Melanin aus Haut und Augen, jedoch lagen an Melanin-gebundene Metallionen in erh{\"o}htem Maß vor...}, subject = {Melanin}, language = {de} } @phdthesis{SalinasSegura2016, author = {Salinas Segura, Alexander}, title = {The Internet of Things: Business Applications, Technology Acceptance, and Future Prospects}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-131605}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2016}, abstract = {This dissertation explores the Internet of Things from three different perspectives for which three individual studies were conducted. The first study presents a business application within supply chain management. The second study addresses user acceptance of pervasive information systems, while the third study covers future prospects of the Internet of Things. The first study is about wireless sensor technologies and their possibilities for optimizing product quality in the cold chain. The processing of sensor data such as temperature information allows for the construction of novel issuing policies in distribution centers. The objective of the study was to investigate the possible economic potential of sensor-based issuing policies in a cold chain. By means of simulation, we analyzed a three-echelon supply chain model, including a manufacturer, a distribution center, and a retail store. Our analysis shows that sensor-based issuing policies bear the potential to become an effective complement to conventional issuing policies. However, the results also indicate that important trade-offs must be taken into account in the selection of a specific issuing policy. The second study deals with the increasing emergence of pervasive information systems and user acceptance. Based on the integration of the extended "Unified Theory of Acceptance and Use of Technology" (UTAUT2) and three pervasiveness constructs, we derived a comprehensive research model to account for pervasive information systems. Data collected from 346 participants in an online survey was analyzed to test the developed research model using structural equation modeling and taking into account multi-group and mediation analysis. The results confirm the applicability of the integrated UTAUT2 model to measure pervasiveness. The third study addresses future prospects of the Internet of Things within the retail industry. We employed a research framework to explore the macro- as well as microeconomic perspective. First, we developed future projections for the retail industry containing IoT aspects. Second, a two-round Delphi study with an expert panel of 15 participants was conducted to evaluate the projections. Third, we used scenario development to create scenarios of the most relevant projections evaluated by the participants.}, subject = {Internet der Dinge}, language = {en} } @phdthesis{Schiebel2013, author = {Schiebel, Johannes}, title = {Structure-Based Drug Design on Enzymes of the Fatty Acid Biosynthesis Pathway}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-69239}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2013}, abstract = {W{\"a}hrend die Wirkung der meisten gebr{\"a}uchlichen Antibiotika auf einer Beeintr{\"a}chtigung wichtiger bakterieller Prozesse beruht, wirken manche Substanzen durch die St{\"o}rung der Zellmembran-Struktur. Da Fetts{\"a}uren ein essentieller Bestandteil von Membran-Phospholipiden sind, stellt die bakterielle Fetts{\"a}urebiosynthese II (FAS-II) einen relativ wenig erforschten, aber dennoch vielversprechenden Angriffspunkt f{\"u}r die Entwicklung neuer Antibiotika dar. Das wichtige Antituberkulotikum Isoniazid blockiert die mykobakterielle Fetts{\"a}urebiosynthese und ruft dadurch morphologische {\"A}nderungen sowie letztlich die Lyse des Bakteriums hervor. Eine wichtige Erkenntnis war, dass Isoniazid den letzten Schritt des FAS-II Elongationszyklus inhibiert, der durch die Enoyl-ACP Reduktase katalysiert wird. Darauf aufbauend wurden mehrere Programme ins Leben gerufen, die sich zum Ziel gesetzt hatten, neue Molek{\"u}le zu entwickeln, welche dieses Protein verschiedener Pathogene hemmen. Die S. aureus Enoyl-ACP Reduktase (saFabI) ist von besonders großem Interesse, da drei vielversprechende Inhibitoren dieses Proteins entwickelt werden konnten, die momentan in klinischen Studien eingehend untersucht werden. Trotz dieser Erfolgsaussichten waren zum Zeitpunkt, als die vorliegenden Arbeiten aufgenommen wurden, keine Kristallstrukturen von saFabI {\"o}ffentlich verf{\"u}gbar. Daher war es eines der Hauptziele dieser Doktorarbeit, auf der Basis von kristallographischen Experimenten atomar aufgel{\"o}ste Modelle f{\"u}r dieses wichtige Protein zu erzeugen. Durch die Entwicklung einer verl{\"a}sslichen Methode zur Kristallisation von saFabI im Komplex mit NADP+ und Diphenylether-Inhibitoren konnten Kristallstrukturen von 17 verschiedenen tern{\"a}ren Komplexen gel{\"o}st werden. Weitere kristallographische Experimente ergaben zwei apo-Strukturen sowie zwei Strukturen von saFabI im Komplex mit NADPH und 2-Pyridon-Inhibitoren. Basierend auf der nun bekannten saFabI-Struktur konnten Molekulardynamik-Simulationen durchgef{\"u}hrt werden, um zus{\"a}tzliche Erkenntnisse {\"u}ber die Flexibilit{\"a}t dieses Proteins zu erhalten. Die so gewonnenen Informationen {\"u}ber die Struktur und Beweglichkeit des Enzyms dienten in Folge als ideale Grundlage daf{\"u}r, den Erkennungsprozess von Substrat und Inhibitor zu verstehen. Besonders bemerkenswert dabei ist, dass die verschiedenen saFabI Kristallstrukturen Momentaufnahmen entlang der Reaktionskoordinate der Ligandenbindung und des Hydrid-Transfers repr{\"a}sentieren. Dabei verschließt der so genannte Substratbindungsloop das aktive Zentrum des Enzyms allm{\"a}hlich. Die außergew{\"o}hnlich hohe Mobilit{\"a}t von saFabI konnte durch molekulardynamische Simulationen best{\"a}tigt werden. Dies legt nahe, dass die beobachteten {\"A}nderungen der Konformation tats{\"a}chlich an der Aufnahme und Umsetzung des Substrates beteiligt sind. Eine Kette von Wassermolek{\"u}len zwischen dem aktiven Zentrum und einer wassergef{\"u}llten Kavit{\"a}t im Inneren des Tetramers scheint f{\"u}r die Beweglichkeit des Substratbindungsloops und somit f{\"u}r die katalysierte Reaktion von entscheidender Bedeutung zu sein. Außerdem wurde die erstaunliche Beobachtung gemacht, dass der adaptive Substratbindungsprozess mit einem Dimer-Tetramer {\"U}bergang gekoppelt ist, welcher die beobachtete positive Kooperativit{\"a}t der Ligandenbindung erkl{\"a}ren kann. Alles in allem weist saFabI im Vergleich zu FabI Proteinen aus anderen Organismen mehrere außergew{\"o}hnliche Eigenschaften auf, die f{\"u}r die Synthese von verzweigten Fetts{\"a}uren n{\"o}tig sein k{\"o}nnten, welche wiederum f{\"u}r die {\"U}berlebensf{\"a}higkeit von S. aureus im Wirt von Bedeutung sind. Diese Erkenntnis k{\"o}nnte erkl{\"a}ren, warum S. aureus selbst bei Anwesenheit von exogenen Fetts{\"a}uren von FAS-II Inhibitoren abget{\"o}tet werden kann. Somit k{\"o}nnen die gewonnenen atomaren saFabI Modelle einen entscheidenden Beitrag zur Entwicklung neuer Hemmstoffe dieses validierten Angriffszieles leisten. Tats{\"a}chlich konnten die neuen Strukturen genutzt werden, um die Bindungsst{\"a}rken sowie die Verweilzeiten verschiedener saFabI Inhibitoren molekular zu erkl{\"a}ren. Die Struktur von saFabI im Komplex mit dem 2-Pyridon Inhibitor CG400549 hingegen enth{\"u}llte spezifische Wechselwirkungen in der geweiteten Bindetasche des S. aureus Enzyms, welche das geringe Aktivit{\"a}tsspektrum dieses derzeit klinisch erprobten Inhibitors erkl{\"a}ren. Diese Studien schaffen somit eine ideale Voraussetzung f{\"u}r die Entwicklung neuer wirksamer saFabI Inhibitoren, was am Beispiel des 4-Pyridons PT166 belegt werden kann. Im Rahmen der vorliegenden Dissertation konnten außerdem die Strukturen des Enzyms KasA im Komplex mit mehreren Derivaten des Naturstoffs Thiolactomycin gel{\"o}st werden.}, subject = {Staphylococcus aureus}, language = {en} } @phdthesis{Becker2015, author = {Becker, Johannes}, title = {Development and implementation of new simulation possibilities in the CAST program package}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-132032}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2015}, abstract = {The aim of the present work is the development and implementation of new simulation possibilities for the CAST program package. Development included, among other things, the partial parallelization of the already existing force fields, extension of the treatment of electrostatic interactions and implementation of molecular dynamics and free energy algorithms. The most time consuming part of force field calculations is the evaluation of the nonbonded interactions. The calculation of these interactions has been parallelized and it could be shown to yield a significant speed up for multi-core calculations compared to the serial execution on only one CPU. For both, simple energy/gradient as well as molecular dynamics simulations the computational time could be significantly reduced. To further increase the performance of calculations employing a cutoff radius, a linkedcell algorithm was implemented which is able to build up the non-bonded interaction list up to 7 times faster than the original algorithm. To provide access to dynamic properties based on the natural time evolution of a system, a molecular dynamics code has been implemented. The MD implementation features two integration schemes for the equations of motion which are able to generate stable trajectories. The basic MD algorithm as described in Section 1.2 leads to the sampling in the microcanonical (NVE) ensemble. The practical use of NVE simulations is limited though because it does not correspond to any experimentally realistic situation. More realistic simulation conditions are found in the isothermal (NVT) and isothermalisobaric (NPT) ensembles. To generate those ensembles, temperature and pressure control has been implemented. The temperature can be controlled in two ways: by direct velocity scaling and by a Nose-Hoover thermostat which produces a real canonical ensemble. The pressure coupling is realized by implementation of a Berendsen barostat. The pressure coupling can be used for isotropic or anisotropic box dimensions with the restriction that the angles of the box need to be 90� . A crucial simulation parameter in MD simulations is the length of the timestep. The timestep is usually in the rang of 1fs. Increasing the timestep beyond 1fs can lead to unstable trajectories since the fastest motion in the system, usually the H-X stretch vibration can not be sampled anymore. A way to allow for bigger timesteps is the use of a constraint algorithm which constrains the H-X bonds to the equilibrium distance. For this the RATTLE algorithm has been implemented in the CAST program. The velocity Verlet algorithm in combination with the RATTLE algorithm has been shown to yield stable trajectories for an arbitrary length of simulation time. In a first application the MD implementation is used in conjunction with the MOPAC interface for the investigation of PBI sidechains and their rigidity. The theoretical investigations show a nice agreement with experimentally obtained results. Based on the MD techniques two algorithms for the determination of free energy differences have been implemented. The umbrella sampling algorithm can be used to determine the free energy change along a reaction coordinate based on distances or dihedral angles. The implementation was tested on the stretching of a deca-L-alanine and the rotation barrier of butane in vacuum. The results are in nearly perfect agreement with literature values. For the FEP implementation calculations were performed for a zero-sum transformation of ethane in explicit solvent, the charging of a sodium ion in explicit solvent and the transformations of a tripeptide in explicit solvent. All results are in agreement with benchmark calculations of the NAMD program as well as literature values. The FEP formalism was then applied to determine the relative binding free energies between two inhibitors in an inhibitor-protein complex. Next to force fields, ab-initio methods can be used for simulations and global optimizations. Since the performance of such methods is usually significantly poorer than force field applications, the use for global optimizations is limited. Nevertheless significant progress has been made by porting these codes to GPUs. In order to make use of these developments a MPI interface has been implemented into CAST for communication with the DFT code TeraChem. The CAST/TeraChem combination has been tested on the \$H_2 O_{10}\$ cluster as well as the polypeptide met-Enkephalin. The pure ab-initio calculations showed a superior behavior compared to the standard procedure where the force field results are usually refined using quantum chemical methods.}, subject = {Molekulardynamik}, language = {en} } @book{KiesewetterGromMenzeletal.2016, author = {Kiesewetter, Dirk and Grom, Michael and Menzel, Moritz and Tschinkl, Dominik}, title = {Optimierungsm{\"o}glichkeiten bei den bestehenden steuer- und sozialversicherungsrechtlichen F{\"o}rderregelungen der betrieblichen Altersversorgung}, publisher = {W{\"u}rzburg University Press}, address = {W{\"u}rzburg}, isbn = {978-3-95826-030-6 (print)}, doi = {10.25972/WUP-978-3-95826-031-3}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-128597}, publisher = {W{\"u}rzburg University Press}, pages = {300}, year = {2016}, abstract = {Germany's old-age retirement system is based on three pillars: the statutory pension scheme, company pension schemes (CPS), and private retirement funds. The current government's coalition agreement expressly foresees a strengthening of CPS since its popularity has heavily stagnated in recent years. The intention is to optimize the fiscal and social insurance-related framework for CPS in an attempt to encourage its wider use. The present expert opinion is a contribution towards this effort. There is considerable potential for this especially among small and medium-sized enterprises (SMEs) and earners of low and very low incomes, since these groups are disproportionately under-represented when it comes to CPS takeup. In light of this, this opinion gives priority to these target groups. The study is structured as follows. First, a comprehensive literature review is provided and guided interviews with experts performed in order to identify obstacles to the continued spread of CPS among the target groups under review. Then, interviews are held with employers in the SME category as well as earners of low and very low incomes in order to verify the obstacles identified during the first step and consider any additional insights. On this basis, the authors consider which reforms may prove effective in addressing the identified obstacles. Here, as instructed, any potential reforms should endeavor not to create a financial burden on Germany's tax and social insurance authorities. We then subject these reform ideas to an empirical review that involves interviews with SME tax advisers and again with earners of low and very low incomes. Having analyzed these interviews and discussing additional practical considerations, we explicitly recommend the implementation of selected reforms. In doing so, the authors propose the following two concrete recommendations. Recommendation 1 suggests introducing a mandatory employer contribution on top of deferred compensation that corresponds to the amount of social insurance contributions that are saved as a result, of which employees would be the obvious beneficiaries. This would result in an increase in employers' financial burden compared to the status quo. To compensate, a "CPS deduction" would be introduced as a tax incentive for small enter-prises that decide to introduce a CPS for their employees. This deduction would function similarly to the investment deduction option afforded under Section 7g of the German Income Tax Act, resulting in a positive liquidity and tax deferment effect for small enterprises. Recommendation 2 aims at incentivizing employees to participate in a CPS. Two alternatives are offered. Either Germany's existing Riester subsidy system could be better integrated into CPS schemes by eliminating the duplication of contributions that exists under the status quo. Alternatively, a "CPS subsidy" could be introduced. This would involve granting a statutory subsidy to employers that contribute a certain minimum amount to the CPS on behalf of their employees. As a consequence, employees would be able to participate in a CPS without having to make a contribution of their own, which would have the desired effect especially for earners of low and very low incomes. In connection with Recommendation 2, the authors mention two additional aspects that ought to be implemented for the benefit of employees. One, a restriction should be placed on the extent to which CPS payments are set off against basic social security payments. Two, the acquisition costs of insurance-based CPS solutions should be spread across the entire term of the agreement, meaning that no commission fees can be retained that relate to contributions that haven't yet been made. Finally, the authors recommend two measures that serve to flexibilize and simplify the legal framework surrounding CPS: an increase in the tax- and social insurance contribution-exempt total outlay in the presence of insurance-based external funding and, related to this, a switch from an annualized to a lifetime- or length-of-service-based approach.}, subject = {Betriebliche Altersversorgung}, language = {de} } @misc{GalloDunkelTravničeketal.2015, author = {Gallo, Lorenzo and Dunkel, Franz and Tr{\´a}vn{\´i}ček, Bohumil and Meierott, Lenz and Žila, Vojtěch}, title = {Forum Geobotanicum Vol. 6 (2012/2015)}, volume = {6(2012/2015)}, editor = {Meierott, Lenz and Drenckhahn, Detlev and Dunkel, Franz G. and Ewald, J{\"o}rg and Schuhwerk, Franz}, issn = {1867-9315}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-131950}, year = {2015}, abstract = {Forum Geobotanicum is an electronic journal devoted to disseminate information concerning geographical distribution, ecology, morphology, taxonomy and conservation of vascular plants in the European Union with a main focus on middle Europe. It covers from molecular biology to environmental aspects. The focus is to publish original papers, reviews and announcements for the educated generalist as well as the specialist in this broad field. Forum Geobotanicum does not aim to supplant existing paper journals, but will be much more flexible in format, publication time and world-wide distribution than paper journals. Many important studies are being currently published in local journals and booklets and some of them are published privately. Hence, these studies will become aware to only a limited readership. Forum Geobotanicum will encourage authors of such papers to submit them as special issues of the journal. Moreover, the journal is planning to build up an E-mail-address section to support communication between geobotanists in Europe. The editors are optimistic that this electronic journal will develop to a widely used communication forum that will help to stimulate activities in the entire field of geobotany in middle Europe. To overcome problems of long term archivation and effective taxonomic publication of articles published electronically in Forum Geobotanicum, print versions of each volume of the journal and appropriate digital storage devices will be delivered freely to selected university libraries and state libraries in middle Europe.}, subject = {Geobotanik}, language = {de} } @misc{GottschlichTisonMalecotetal.2011, author = {Gottschlich, G{\"u}nter and Tison, Jean-Marc and Malecot, Val{\´e}ry and Rouillard, Thomas}, title = {Forum Geobotanicum Vol. 5 (2011)}, volume = {5(2011)}, editor = {Meierott, Lenz and Drenckhahn, Detlev and Dunkel, Franz G. and Ewald, J{\"o}rg and Schuhwerk, Franz}, issn = {1867-9315}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-131940}, year = {2011}, abstract = {Forum geobotanicum is an electronic journal devoted to disseminate information concerning geographical distribution, ecology, morphology, taxonomy and conservation of vascular plants in the European Union with a main focus on middle Europe. It covers from molecular biology to environmental aspects. The focus is to publish original papers, reviews and announcements for the educated generalist as well as the specialist in this broad field. Forum geobotanicum does not aim to supplant existing paper journals, but will be much more flexible in format, publication time and world-wide distribution than paper journals. Many important studies are being currently published in local journals and booklets and some of them are published privately. Hence, these studies will become aware to only a limited readership. Forum geobotanicum will encourage authors of such papers to submit them as special issues of the journal. Moreover, the journal is planning to build up an E-mail-address section to support communication between geobotanists in Europe. The editors are optimistic that this electronic journal will develop to a widely used communication forum that will help to stimulate activities in the entire field of geobotany in middle Europe. To overcome problems of long term archivation and effective taxonomic publication of articles published electronically in Forum geobotanicum, print versions of each volume of the journal and appropriate digital storage devices will be delivered freely to selected university libraries and state libraries in middle Europe.}, subject = {Geobotanik}, language = {de} } @misc{OPUS4-13197, title = {einBlick - Ausgabe 14 - 12. April 2016}, volume = {14/2016}, organization = {Julius-Maximilians-Universit{\"a}t W{\"u}rzburg}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-131975}, year = {2016}, abstract = {Nachrichten aus der Julius-Maximilians-Universit{\"a}t W{\"u}rzburg}, subject = {W{\"u}rzburg}, language = {de} } @misc{OPUS4-13196, title = {einBlick - Ausgabe 13 - 05. April 2016}, volume = {13/2016}, organization = {Julius-Maximilians-Universit{\"a}t W{\"u}rzburg}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-131960}, year = {2016}, abstract = {Nachrichten aus der Julius-Maximilians-Universit{\"a}t W{\"u}rzburg}, subject = {W{\"u}rzburg}, language = {de} } @phdthesis{Kesetovic2016, author = {Kesetovic, Diana}, title = {Synthesis and biological testing of potential anti-tuberculosis drugs targeting the β-ketoacyl ACP synthase}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-131301}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2016}, abstract = {With 9.6 million new cases and 1.5 million deaths in 2014, tuberculosis (TB) is alongside with AIDS the most deadly infection.‎ Foremost, the increased prevalence of resistant strains of M. tuberculosis among the TB-infected population represents a serious thread. Hence, in the last decades, novel drug targets have been investigated worldwide. So far a relatively unexplored target is the cell wall enzyme β-ketoacyl-ACP-synthase "KasA", which plays a crucial role in maintaining the membrane impermeability and hence the cell ability to resist to the immune response and drug therapy. KasA is a key enzyme in the fatty acid synthase "FAS-II" elongation cycle, responsible for the extension of the growing acyl chain within the biosynthesis of precursors for the most hydrophobic constituents of the cell wall - mycolic acids. Design of the novel KasA inhibitors, performed in the research group of Prof. Sotriffer by C. Topf and B. Schaefer, was based on the recently published crystal structure of KasA‎ in complex with its known inhibitor thiolactomycin (TLM). Considering the essential ligand-enzyme interactions, a pharmacophore model was built and applied in the virtual screening of a modified ZINC database. Selected hits with the best in silico affinity data have been reported by Topf‎ and Schaefer‎. In this work, two of the obtained hits were synthesized and their structure was systematically varied. First, a virtual screening hit, chromone-2-carboxamide derivative GS-71, was modified in the amide part. Since the most of the products possessed a very low solubility in the aqueous buffer medium used in biological assays, polar groups (nitro, succinamidyl and trimethyl-amino substituent in position 6 of the chromone ring or hydroxyl group on the benzene ring in the amide part have been inserted to the molecule. Further variations yielded diaryl ketones, diaryl ketone bearing a succinamidyl substituent, carboxamide bearing a methylpiperazinyl-4-oxobutanamido group and methyl-malonyl ester amides. Basically, the essential structural features necessary for the ligand-enzyme interactions have been maintained. The latter virtual screening hit, a pyrimidinone derivative VS-8‎ was synthesized and the structure was modified by substitution in positions 2, 4, 5 and 6 of the pyrimidine ring. Due to autofluorescence, detected in most of the products, this model structure was not further varied. Simultaneously, experiments on solubilization of the first chromone-2-carboxamides with cyclodextrins, cyclic oligosacharides known to form water-soluble inclusion complexes, were performed. Although the assessed solubility of the chromone 3b/DIMEB (1:3) mixture exceeded 14-fold the intrinsic one, the achieved 100 µM solubility was still not sufficient to be used as a stock solution in the binding assay. The experiments with cyclodextrin in combination with DMSO were ineffective. Owing to high material costs necessary for the appropriate cyclodextrin amounts, the aim focused on structural modification of the hydrophobic products. Precise structural data have been obtained from the solved crystal structures of three chromone derivatives: the screening hit GS-71 (3b), its trimethylammonium salt (18) and 6-nitro-substituted N-benzyl-N-methyl-chromone-2-carboxamide (9i). The first two compounds are nearly planar with an anti-/trans-rotamer configuration. In the latter structure, the carboxamide bridge is bent out of the chromone plane, showing an anti-rotamer, too. Considering the relatively low partition coefficient of compound 3b (cLogP = 2.32), the compound planarity and correlating tight molecular packing might be the factors significantly affecting its poor solubility. Regarding the biological results of the chromone-based compounds, similar structure-activity correlations could be drawn from the binding assay and the whole cell activity testing on M. tuberculosis. In both cases, the introduction of a nitro group to position 6 of the chromone ring and the presence of a flexible substituent in the amide part showed a positive effect. In the binding study, the nitro group at position 4 on the N-benzyl residue was of advantage, too. The highest enzyme affinity was observed for N-(4-nitrobenzyl)-chromone-2-carboxamide 4c (KD = 34 µM), 6-nitro substituted N-benzyl-chromone-2-carboxamide 9g (KD = 40 µM) and 6‑nitro-substituted N-(4-nitrobenzyl)-chromone-2-carboxamide 9j (KD = 31 µM), which could not be attributed to the fluorescence quenching potential of the nitro group. The assay interference potential of chromones, due to a covalent binding on the enzyme sulfhydryl groups, was found to be negligible at the assay conditions. Moderate in vivo activity was detected for 6‑nitro-substituted N-benzyl-chromone-2-carboxamide 9g and its N-benzyl-N-methyl-, N‑furylmethyl-, N-cyclohexyl- and N-cyclohexylmethyl derivatives 9i, 9d, 9e, 9f, for which MIC values 20 - 40 µM were assessed. Cytotoxicity was increased in the N‑cyclohexylmethyl derivative only. None of the pyrimidine-based compounds showed activity in vivo. The affinity of the model structure, VS-8, surpassed with KD = 97 µM the assessed affinity of TLM (KD = 142 µM). Since for the model chromone compound GS-71 no reliable KasA binding data could be obtained, a newly synthesized chromone derivative 9i was docked into the KasA binding site, in order to derive correlation between the in silico and in vitro assessed affinity. For the 6‑nitro-derivative 9i a moderate in vivo activity on M. tuberculosis was obtained. The in silico predicted pKi values for TLM and 9i were higher than the corresponding in vitro results, maintaining though a similar tendency, i.e., the both affinity values for compound 9i (pKi predicted = 6.64, pKD experimental = 4.02) surpassed those obtained for TLM (pKi predicted = 5.27, pKD experimental = 3.84). Nevertheless, the experimental pKD values are considered preliminary results. The binding assay method has been improved in order to acquire more accurate data. Owing to the method development, limited enzyme batches and solubility issues, only selected compounds could be evaluated. The best hits, together with the compounds active on the whole cells of M. tuberculosis, will be submitted to the kinetic enzyme assay, in order to confirm the TLM-like binding mechanism. Regarding the in vivo testing results, no correlations could be drawn between the predicted membrane permeability values and the experimental data, as for the most active compounds 9e and 9f, a very low permeability was anticipated (0.4 and 0.7 \%, respectively). Further biological tests would be required to investigate the action- or transport mode.}, subject = {Tuberkelbakterium}, language = {en} } @book{ReindersHoosHaubenthal2016, author = {Reinders, Heinz and Hoos, Olaf and Haubenthal, Gernot}, title = {Fußballspezifische Leistungen bei NFZ-Spielerinnen. Entwicklung und Manual einer Leistungsdiagnostik zur Erfassung der Spielf{\"a}higkeiten im M{\"a}dchenfußball}, isbn = {978-3-945459-07-2}, issn = {2365-2268}, doi = {10.25972/OPUS-13142}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-131429}, publisher = {Universit{\"a}t W{\"u}rzburg}, pages = {49}, year = {2016}, abstract = {Das Nachwuchsf{\"o}rderzentrum f{\"u}r Juniorinnen in Unterfranken f{\"o}rdert talentierte Nachwuchspielerinnen zwischen neun und 15 Jahren. Es ist bayernweit das einzige Nachwuchsf{\"o}rderzentrum nur f{\"u}r Spielerinnen, das {\"u}ber eine wissenschaftliche Begleitung im sportwissenschaftlichen und p{\"a}dagogisch-psychologischen Bereich verf{\"u}gt. Es wurde im Fr{\"u}hjahr 2014 von vier Partnervereinen in der Region gemeinsam mit der Empirischen Bildungsforschung und dem Sportzentrum der Universit{\"a}t W{\"u}rzburg sowie dem 1. FC N{\"u}rnberg M{\"a}dchen- und Frauenfußball gegr{\"u}ndet. Das Ziel ist es, talentierte Spielerinnen nach einem innovativen sportwissenschaftlichen Ansatz zu f{\"o}rdern und auf diese Weise die Chance des {\"U}bergangs in den Leistungssport f{\"u}r jede Spielerin zu erh{\"o}hen. Hierzu werden die Spielerinnen jedes Jahr im Fr{\"u}hsommer f{\"u}r acht Wochen w{\"a}hrend des w{\"o}chentlichen Trainings gesichtet und mittels allgemeiner motorischer Tests einerseits sowie fußballspezifischer Tests andererseits auf ihre Eignung f{\"u}r eine Aufnahme in das NFZ hin gepr{\"u}ft. Im sportartspezifischen Bereich wurden die Spielerinnen des Leistungskaders 2015/16 neben einem neu entwickelten Test, der die F{\"a}higkeiten der Spielerinnen im Spielverlauf abbildet, auch mit Teilaufgaben der Testbatterie des Deutschen Fußball-Bundes konfrontiert (H{\"o}ner \& Roth, 2011, 2015). Dieser Test des DFB dient seit geraumer Zeit dazu, den Leistungsstand der an DFB-St{\"u}tzpunkten gef{\"o}rderten Spielerinnen und Spieler zu {\"u}berpr{\"u}fen und durch den Vergleich mit Normwerttabellen individuelle SpielerInnen-Profile zu erstellen. Dieser Band berichtet die Ergebnisse der Leistungstests im NFZ f{\"u}r Juniorinnen nach den Kriterien des DFB und stellt die im NFZ entwickelte Leistungsdiagnostik NFZ-TestSpiel vor. Drei zentrale Befunde kristallisieren sich dabei heraus. Erstens nimmt die erste Generation der NFZ-Spielerinnen einen heterogenen Leistungsstand gemessen an den DFB-Kriterien ein. Dieser Befund relativiert sich aber zweitens, weil die Testbatterie des DFB durchaus Zweifel an deren Mess-Zuverl{\"a}ssigkeit aufkommen l{\"a}sst und zudem Normwerte f{\"u}r Jahrg{\"a}nge unterhalb der U11-Juniorinnen nicht existieren. Drittens erweist sich der im NFZ gew{\"a}hlte Ansatz vielversprechend, um die Spielf{\"a}higkeiten im M{\"a}dchenfußball {\"u}ber reale Spielsituationen, also als Prozessdiagnostik zu erfassen. Die vorgestellte NFZ-Leistungsdiagnostik erweist sich als in hohem Maße reliabel und ergibt erste Hinweise auf eine valide Messung individueller fußballspezifischer Kompetenzen.}, subject = {Leistungsdiagnostik}, language = {de} } @phdthesis{Knorr2015, author = {Knorr, Johannes Walter}, title = {Femtosecond spectroscopy of photolysis reactions in the liquid phase}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-131362}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2015}, abstract = {Within the framework of this thesis, photolysis reactions in the liquid phase were investigated by means of ultrafast optical spectroscopy. Apart from molecular studies dealing with the highly spin-dependent reactivity of diphenylcarbene (DPC) in binary solvent mixtures and ligand dissociation reactions of so-called CO-releasing molecules (CORMs), special emphasis was put on the implementation and characterization of methods improving and extending the signal detection in conventional pump-probe transient absorption setups. The assumption of DPC being an archetypal triplet-ground-state arylcarbene was recently questioned by matrix-isolation studies at low temperatures. DPC embedded in argon matrices revealed a hitherto unknown reactivity when the carbene environment was modified by small amounts of methanol dopant molecules. To complement these findings with liquid-phase experiments at room temperature, femtosecond pump-probe transient absorption spectroscopy with probing in the visible and ultraviolet regime was employed to unravel primary reaction processes of DPC in solvent mixtures. Supported by quantum chemical simulations conducted by our collaborators, it was shown that a competition between the reaction pathways occurs that not only depends on the solvent molecule near-by but also on its interaction with other solvent molecules. In-depth analysis of the solvation dynamics and the amount of nascent intermediates corroborates the importance of a hydrogen-bonded complex with a protic solvent molecule, in striking analogy to complexes found at cryogenic temperatures. Probing the transient absorption of molecules in the mid-infrared spectral range benefits from the high chemical specificity of molecules' vibrational signatures. The technique of chirped-pulse upconversion (CPU) constitutes a promising alternative to standard direct multichannel MCT detection when accessing this spectral detection window. Hence, one chapter of this thesis is dedicated to a direct comparison between both detection methods. By conducting an exemplary pump-probe transient absorption experiment, it became evident, that the additional nonlinear interaction step is responsible for increased noise levels when using CPU. However, a correction procedure capable of removing these additional noise contributions—stemming from the fundamental laser radiation used for upconversion—was successfully tested. Perhaps most importantly for various spectroscopic applications, CPU scored with a significantly extended detection bandwidth owing to the high pixel numbers of modern CCD cameras. Transition-metal complexes capable of releasing small molecular messengers upon photoactivation are promising sources of gasotransmitters such as carbon monoxide (CO) or nitric oxide (NO) in biological applications. However, only little is known about the characteristic time scales of ligand dissociation in this class of molecules. For this purpose, two complexes were investigated with femtosecond time resolution: [Mn(CO)3(tpm)]Cl with tpm=tris(2-pyrazolyl)methane, a manganese tricarbonyl complex which has proven to be selective and cytotoxic to cancer cells, and [Mo(CO)2(NO)(iPr3tacn)]PF6 with iPr3tacn=1,4,7-triisopropyl-1,4,7-triazacyclononane, a molybdenum complex containing both carbonyl and nitrosyl ligands. By conducting pump-probe transient absorption measurements in different spectral probing windows supported by quantum chemical calculations and linear absorption spectroscopy, it was shown that both complexes are able to release one CO ligand within the first few picoseconds after UV excitation. The results complement existing studies which focused on the molecules' ligand-releasing properties upon long-term exposure. The additional information gained on an ultrafast time scale provides a comprehensive understanding of individual reaction steps connected with ligand release in this class of molecules. Hence, the studies might create new incentives to develop modified molecules for specific applications.}, subject = {Ultrakurzzeitspektroskopie}, language = {en} }