TY - JOUR A1 - Makoah Nigel, Animake A1 - Arndt, Hans-Dieter A1 - Pradel, Gabriele T1 - The proteasome of malaria parasites: A multi-stage drug target for chemotherapeutic intervention? JF - International Journal for Parasitology: Drugs and Drug Resistance N2 - The ubiquitin/proteasome system serves as a regulated protein degradation pathway in eukaryotes, and is involved in many cellular processes featuring high protein turnover rates, such as cell cycle control, stress response and signal transduction. In malaria parasites, protein quality control is potentially important because of the high replication rate and the rapid transformations of the parasite during life cycle progression. The proteasome is the core of the degradation pathway, and is a major proteolytic complex responsible for the degradation and recycling of non-functional ubiquitinated proteins. Annotation of the genome for Plasmodium falciparum, the causative agent of malaria tropica, revealed proteins with similarity to human 26S proteasome subunits. In addition, a bacterial ClpQ/hslV threonine peptidase-like protein was identified. In recent years several independent studies indicated an essential function of the parasite proteasome for the liver, blood and transmission stages. In this review, we compile evidence for protein recycling in Plasmodium parasites and discuss the role of the 26S proteasome as a prospective multi-stage target for antimalarial drug discovery programs. KW - plasmodium falciparum KW - proteasome KW - ubiquitin KW - inhibitor Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-137777 VL - 2 ER - TY - THES A1 - Cook, Mandy T1 - The neurodegenerative Drosophila melanogaster AMPK mutant loechrig T1 - The neurodegenerative Drosophila melanogaster AMPK Mutante loechrig N2 - In dieser Doktorarbeit wird die Drosophila Mutante loechrig (loe), die progressive Degeneration des Nervensystems aufweist, weiter beschrieben. In der loe Mutante fehlt eine neuronale Isoform der γ- Untereinheit der Proteinkinase AMPK (AMP-activated protein kinase). Die heterotrimere AMPK (auch als SNF4Aγ bekannt) kontrolliert das Energieniveau der Zelle, was ständiges Beobachten des ATP/AMP- Verhältnis erfordert. AMPK wird durch niedrige Energiekonzentrationen und Beeinträchtigungen im Metabolismus, wie zum Beispiel Sauerstoffmangel, aktiviert und reguliert mehrere wichtige Signaltransduktionswege, die den Zellmetabolismus kontrollieren. Jedoch ist die Rolle von AMPK im neuronalen Überleben noch unklar. Eines der Proteine, dass von AMPK reguliert wird, ist HMGR (hydroxymethylglutaryl-CoA- reductase), ein Schlüsselenzym in der Cholesterin- und Isoprenoidsynthese. Es wurde gezeigt, dass wenn die Konzentration von HMGR manipuliert wird, auch der Schweregrad des neurodegenerativen Phänotyps in loe beeinflusst wird. Obwohl die regulatorische Rolle von AMPK auf HMGR in Drosophila konserviert ist, können Insekten Cholesterin nicht de novo synthetisieren. Dennoch ist der Syntheseweg von Isoprenoiden zwischen Vertebraten und Insekten evolutionär konserviert. Isoprenylierung von Proteinen, wie zum Beispiel von kleinen G-Proteinen, stellt den Proteinen einen hydophobischen Anker bereit, mit denen sie sich an die Zellmembran binden können, was in anschließender Aktivierung resultieren kann. In dieser Doktorarbeit wird gezeigt, dass die loe Mutation die Prenylierung von Rho1 und den LIM-Kinasesignalweg beeinflusst, was eine wichtige Rolle im Umsatz von Aktin und axonalem Auswachsen spielt. Die Ergebnisse weisen darauf hin, dass die Mutation in LOE, Hyperaktivität des Isoprenoidsynthesewegs verursacht, was zur erhöhten Farnesylierung von Rho1 und einer dementsprechend höheren Konzentration von Phospho- Cofilin führt. Eine Mutation in Rho1 verbessert den neurodegenerativen Phänotyp und die Lebenserwartung von loe. Der Anstieg vom inaktiven Cofilin in loe führt zu einer Zunahme von filamentösen Aktin. Aktin ist am Auswachen von Neuronen beteiligt und Experimente in denen loe Neurone analysiert wurden, gaben wertvolle Einblicke in eine mögliche Rolle die AMPK, und dementsprechend Aktin, im Neuronenwachstum spielt. Des Weiteren wurde demonstriert, dass Neurone, die von der loe Mutante stamen, einen verlangsamten axonalen Transport aufweisen, was darauf hinweist dass Veränderungen, die durch den Einfluss von loe auf den Rho1 Signalweg im Zytoskelettnetzwerk hervorgerufen wurden, zur Störung des axonalen Transports und anschließenden neuronalen Tod führen. Es zeigte außerdem, dass Aktin nicht nur am neuronalen Auswachsen beteiligt ist, sondern auch wichtig für die Aufrechterhaltung von Neuronen ist. Das bedeutet, dass Änderungen der Aktindynamik zur progressiven Degeneration von Neuronen führen kann. Zusammenfassend unterstreichen diese Ergebnisse die wichtige Bedeutung von AMPK in den Funktionen und im Überleben von Neuronen und eröffnen einen neuartigen funktionellen Mechanismus in dem Änderungen in AMPK neuronale Degeneration hervorrufen kann. N2 - In this thesis the Drosophila mutant loechrig (loe), that shows progressive degeneration of the nervous system, is further described. Loe is missing a neuronal isoform of the protein kinase AMPK γ subunit (AMP-activated protein kinase- also known as SNF4Aγ) The heterotrimeric AMPK controls the energy level of the cell, which requires constant monitoring of the ATP/AMP levels. It is activated by low energy levels and metabolic insults like oxygen starvation and regulates multiple important signal pathways that control cell metabolism. Still, its role in neuronal survival is unclear. One of AMPK’s downstream targets is HMGR (hydroxymethylglutaryl-CoA- reductase), a key enzyme in cholesterol and isoprenoid synthesis. It has been shown that manipulating the levels of HMGR affects the severity of the neurodegenerative phenotype in loe. Whereas the regulatory role of AMPK on HMGR is conserved in Drosophila, insects cannot synthesize cholesterol de novo. However, the synthesis of isoprenoids is a pathway that is evolutionarily conserved between vertebrates and insects. Isoprenylation of target proteins like small G-proteins provides a hydrophobic anchor that allows the association of these proteins with membranes and following activation. This thesis shows that the loe mutation interferes with the prenylation of Rho1 and the regulation of the LIM kinase pathway, which plays an important role in actin turnover and axonal outgrowth. The results suggest that the mutation in LOE, causes hyperactivity of the isoprenoid synthesis pathway, which leads to increased farnesylation of RHO1 and therefore higher levels of phospho-cofilin. A mutation in Rho1 improves the neurodegenerative phenotype and life span. The increased inactive cofilin amount in loe leads to an up regulation of filamentous actin. Actin is involved in neuronal outgrowth and experiments analyzing loe neurons gave valuable insights into a possible role of AMPK and accordingly actin on neurite growth and stability. It was demonstrated that neurons derived from loe mutants exhibit reduces axonal transport suggesting that changes in the cytoskeletal network caused by the effect of loe on the Rho1 pathway lead to disruptions in axonal transport and subsequent neuronal death. It also shows that actin is not only involved in neuronal outgrowth, its also important in maintenance of neurons, suggesting that interference with actin dynamics leads to progressive degeneration of neurons. Together, these results further support the importance of AMPK in neuronal function and survival and provide a novel functional mechanisms how alterations in AMPK can cause neuronal degeneration KW - Taufliege KW - Nervendegeneration KW - AMP KW - Proteinkinasen KW - Molekulargenetik KW - Drosophila KW - Neurodegeneration KW - AMPK KW - Drosophila KW - Neurodegeneration KW - Rho Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-72027 ER - TY - JOUR A1 - Merget, Benjamin A1 - Koetschan, Christian A1 - Hackl, Thomas A1 - Förster, Frank A1 - Dandekar, Thomas A1 - Müller, Tobias A1 - Schultz, Jörg A1 - Wolf, Matthias T1 - The ITS2 Database JF - Journal of Visual Expression N2 - The internal transcribed spacer 2 (ITS2) has been used as a phylogenetic marker for more than two decades. As ITS2 research mainly focused on the very variable ITS2 sequence, it confined this marker to low-level phylogenetics only. However, the combination of the ITS2 sequence and its highly conserved secondary structure improves the phylogenetic resolution1 and allows phylogenetic inference at multiple taxonomic ranks, including species delimitation. The ITS2 Database presents an exhaustive dataset of internal transcribed spacer 2 sequences from NCBI GenBank accurately reannotated. Following an annotation by profile Hidden Markov Models (HMMs), the secondary structure of each sequence is predicted. First, it is tested whether a minimum energy based fold (direct fold) results in a correct, four helix conformation. If this is not the case, the structure is predicted by homology modeling. In homology modeling, an already known secondary structure is transferred to another ITS2 sequence, whose secondary structure was not able to fold correctly in a direct fold. The ITS2 Database is not only a database for storage and retrieval of ITS2 sequence-structures. It also provides several tools to process your own ITS2 sequences, including annotation, structural prediction, motif detection and BLAST search on the combined sequence-structure information. Moreover, it integrates trimmed versions of 4SALE and ProfDistS for multiple sequence-structure alignment calculation and Neighbor Joining tree reconstruction. Together they form a coherent analysis pipeline from an initial set of sequences to a phylogeny based on sequence and secondary structure. In a nutshell, this workbench simplifies first phylogenetic analyses to only a few mouse-clicks, while additionally providing tools and data for comprehensive large-scale analyses. KW - homology modeling KW - molecular systematics KW - internal transcribed spacer 2 KW - alignment KW - genetics KW - secondary structure KW - ribosomal RNA KW - phylogenetic tree KW - phylogeny Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-124600 VL - 61 IS - e3806 ER - TY - JOUR A1 - Isaias, Ioannis U. A1 - Volkmann, Jens A1 - Marzegan, Alberto A1 - Marotta, Giorgio A1 - Cavallari, Paolo A1 - Pezzoli, Gianni T1 - The Influence of Dopaminergic Striatal Innervation on Upper Limb Locomotor Synergies JF - PLoS One N2 - To determine the role of striatal dopaminergic innervation on upper limb synergies during walking, we measured arm kinematics in 13 subjects with Parkinson disease. Patients were recruited according to several inclusion criteria to represent the best possible in vivo model of dopaminergic denervation. Of relevance, we included only subjects with normal spatio-temporal parameters of the stride and gait speed to avoid an impairment of upper limbs locomotor synergies as a consequence of gait impairment per se. Dopaminergic innervation of the striatum was measured by FP-CIT and SPECT. All patients showed a reduction of gait-associated arms movement. No linear correlation was found between arm ROM reduction and contralateral dopaminergic putaminal innervation loss. Still, a partition analysis revealed a 80% chance of reduced arm ROM when putaminal dopamine content loss was >47%. A significant correlation was described between the asymmetry indices of the swinging of the two arms and dopaminergic striatal innervation. When arm ROM was reduced, we found a positive correlation between upper-lower limb phase shift modulation ( at different gait velocities) and striatal dopaminergic innervation. These findings are preliminary evidence that dopaminergic striatal tone plays a modulatory role in upper-limb locomotor synergies and upper-lower limb coupling while walking at different velocities. KW - pet KW - Parkinsons disease KW - basal ganglia KW - spinal-cord KW - walking KW - gait KW - arm KW - coordination KW - movements Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-133976 VL - 7 IS - 12 ER - TY - THES A1 - Schmidt, Gerald T1 - The Influence of Anticipation and Warnings on Collision Avoidance Behavior of Attentive Drivers T1 - Einfluss von Antizipation und Warnung auf das Kollisionsvermeidungsverhalten aufmerksamer Fahrer N2 - This thesis deals with collision avoidance. Focus is on the question of under which conditions collision avoidance works well for humans and if drivers can be supported by a Forward Collision Warning (FCW) System when they do not react appropriately. Forward Collision Warning systems work in a way that tries to focus the driver's attention in the direction of the hazard and evoke an avoidance reaction by some sort of alert (e.g., tone or light). Research on these warning systems generally focuses on inattention and distraction as the cause for crashes. If the driver is inattentive, the results of a crash are thought to be worse as the driver‘s reaction is belated or might not mitigate the crash at all. To ensure effectiveness in the worst case, most of the experiments studying FCW systems have been conducted with visually distracted drivers. Research on the cause and possible countermeasures for crashes of attentive drivers are hardly available, although crash databases and field operational test data show that 40-60% of the drivers look at the forward scene shortly before they crash. Hence, only a few studies elaborated on ideas about the reasons for crashes with attentive drivers. On the basis of the literature, it is worked out that one reason for delayed avoidance behavior can be an incorrect allocation of attention. It is further elaborated that high level attention processes are strongly influenced by interpretation of the situation and the anticipation of future status. Therefore, it is hypothesized that alert drivers react later when they can not foresee a potential threat or even when they misinterpret the situation. If the lack of threat anticipation or incorrect anticipation is a reason for crashes, a FCW system could be a great help, when the FCW is easily comprehensible. It is hypothesized that a FCW can compensate for missing threat anticipation in the driver. The results of the experiments show that the level of threat anticipation has the largest influence on driver behavior in an imminent crash situation. The results further suggest that FCW systems - especially warnings of audible or haptic modality - can help attentive drivers who do not anticipate a threat or misinterpret a situation. The negative influence of missing or mislead threat anticipation on objective measures was small when the threat appeared suddenly. This is thought to be due to the visual appearance of the introduced threat. It is assumed that this type of stimulus triggers a lower level attentional process, as opposed to a top-down attention process controlled by an anticipatory process. In the other scenario types such a lower level process may not be triggered. An important result of the second study is that (Forward) Collision Warnings have to be learned. Participants with warnings reacted slower than participants without any FCW in the first critical event. Participants with a visual warning reacted particularly slow. Later in the experiment, the probands with warnings were constantly faster than their counterparts without them. Hence, the results of this study suggest that a haptic or audible modality should be used as a primary warning to the driver. The characteristic of visual warnings to draw the visual attention is both a blessing and a curse. It is suggested to use the visual warning component for only a short period of time to attract the driver's attention to the forward scene, but then end the display to not further distract him. Car manufacturers try to avoid as many unnecessary alarms as possible. If driver monitoring would be available, it is often planned to suppress warnings when the driver is looking through the windshield. The results suggest not to do so. If a driver reaches a critical situation represented by a low Time-to-collision (TTC) or a high need to decelerate, he should always get a warning, unless he is already braking or steering. The most important arguments for this are: - Looking at the street does not mean that the driver has the correct situational awareness. - The driver has to learn the meaning of the warning. - The driver will not be annoyed by a warning when the situation is considered critical. N2 - Die vorliegende Arbeit beschäftigt sich mit Kollisionsvermeidungsverhalten im Straßenverkehr. Die Hauptfragestellung der Arbeit erforscht die Bedingungen, unter welchen Menschen Kollisionsvermeidung gut beherrschen, und stellt dabei den Anteil der Antizipation in den Vordergrund. Ein weiterer Hauptpunkt der Arbeit ist die Frage, ob in den Situationen, in denen Fahrer kein angemessenes Verhalten zeigen, ein Frontkollisionswarnsystem unterstützend wirkt. Der Begriff Frontkollisionswarnung wird im Folgenden von dem Englischen Begriff "Front Collision Warning" als FCW abgekürzt. Anhand der Literatur wird herausgearbeitet, dass eine Hauptursache für verspätete Vermeidungsreaktionen eine falsche Aufmerksamkeitsausrichtung des Fahrers ist. Des Weiteren wird dargestellt, dass höhere Aufmerksamkeitsprozesse stark von der Situationsinterpretation und -antizipation beeinflusst werden. Daraus wird die Hypothese abgeleitet, dass aufmerksame Fahrer dann verspätet reagieren, wenn es ihnen entweder nicht möglich ist, die Gefahr vorherzusehen oder der Fahrer die Situation falsch einschätzt. Falls dies zutrifft und eine fehlende oder fehlgeleitete Antizipation die Ursache für Unfälle darstellt, müsste eine FCW vorteilhaft wirken, wenn diese schnell und leicht verständlich ist. Eine so gestaltete FCW könnte die Situationswahrnehmung des Fahrers ergänzen. Es wird die Hypothese aufgestellt, dass FCW fehlende oder fehlgeleitete Gefahrenantizipation des Fahrers kompensieren können. Hauptuntersuchungsgegenstand der Experimente ist die Interaktion zwischen verschiedenen Gütestufen der Gefahrenantizipation und der An- bzw. Abwesenheit von FCW in verschiedenen Fahrsituationen. Um die verschiedenen Gütestufen der Antizipation zu realisieren, wurden komplexe Stadtszenarien im Fahrsimulator umgesetzt. Das Verhalten des umgebenden Verkehrs wurde in einer Weise modifiziert, dass es das Situationsbewusstsein des Fahrers beeinflusste. Der umgebende Verkehr erlaubte es dem Fahrer, (1) die Gefahr vorherzusehen, (2) die Gefahr nicht vorherzusehen oder leitete (3) die Antizipation des Fahrers dadurch fehl, dass ein weiterer, irrelevanter Verkehrsteilnehmer eingeführt wurde. Die Ergebnisse bestätigen die Hypothese, dass die Güte der Gefahrenantizipation den größten Einfluss auf das Fahrerverhalten in einer drohenden Unfallsituation hat. Die Ergebnisse deuten weiter darauf hin, dass FCW-Systeme aufmerksamen Fahrern messbar helfen, wenn diese die Gefahr nicht antizipieren oder sogar die Situation falsch einschätzen. Die positive Wirkung ist bei der getesteten akustischen und haptischen Warnung besonders ausgeprägt. Auffällig war, dass der negative Einfluss der fehlenden oder fehlgeleiteten Antizipation bei plötzlich auftauchenden Gefahrenobjekten deutlich geringer war, als wenn diese längere Zeit sichtbar waren, bevor sie zur Gefahr wurden. Es wird davon ausgegangen, dass dieser Effekt aufgrund visueller Eigenschaften der Gefahrenobjekte ausgelöst wird. Bei den plötzlich auftauchenden Gefahren wird davon ausgegangen, dass diese einen lower-level Aufmerksamkeitsprozess auslösen, welcher im Konflikt zu top-down Aufmerksamkeitsprozessen steht, die die Antizipation steuern. Ein wichtiges Ergebnis der zweiten Studie ist, dass (Front-) Kollisionswarnungen erst vom Fahrer gelernt werden müssen, damit sie sich positiv auf die Kollisionsvermeidung auswirken können. Die Teilnehmer mit Warnung reagierten beim ersten kritischen Ereignis langsamer als die Teilnehmer ohne Warnung. Dieser Zusammenhang war bei Probanden mit visueller Warnung besonders ausgeprägt. Später im Experiment war die Probandengruppe mit Warnung konstant schneller als die Gruppe ohne und zeigte einen klaren Vorteil einer gelernten FCW. Die Ergebnisse der Simulatorstudien legen u.a. nahe, haptische oder akustische Warnungen als primäre Warnmodalitäten in drohenden Auffahrsituationen zu verwenden, da bei diesen die negativen Auswirkungen der ersten Warnung geringer ausfallen. KW - Zusammenstoss KW - Verkehrsunfall KW - Fahrerassistenz KW - Frontkollisionswarnung KW - Warnung KW - Antizipation KW - Driver Assistance System KW - Front Collision Warning KW - Anticipation KW - HMI Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-73789 ER - TY - JOUR A1 - Ermert, Volker A1 - Fink, Andreas H. A1 - Morse, Andrew P. A1 - Paeth, Heiko T1 - The Impact of Regional Climate Change on Malaria Risk due to Greenhouse Forcing and Land-Use Changes in Tropical Africa JF - Environmental Health Perspectives N2 - BACKGROUND: Climate change will probably alter the spread and transmission intensity of malaria in Africa. OBJECTIVES: In this study, we assessed potential changes in the malaria transmission via an integrated weather disease model. METHODS: We simulated mosquito biting rates using the Liverpool Malaria Model (LMM). The input data for the LMM were bias-corrected temperature and precipitation data from the regional model (REMO) on a 0.5 degrees latitude longitude grid. A Plasmodium falciparum infection model expands the LMM simulations to incorporate information on the infection rate among children. Malaria projections were carried out with this integrated weather disease model for 2001 to 2050 according to two climate scenarios that include the effect of anthropogenic land-use and land-cover changes on climate. RESULTS: Model-based estimates for the present climate (1960 to 2000) are consistent with observed data for the spread of malaria in Africa. In the model domain, the regions where malaria is epidemic are located in the Sahel as well as in various highland territories. A decreased spread of malaria over most parts of tropical Africa is projected because of simulated increased surface temperatures and a significant reduction in annual rainfall. However, the likelihood of malaria epidemics is projected to increase in the southern part of the Sahel. In most of East Africa, the intensity of malaria transmission is expected to increase. Projections indicate that highland areas that were formerly unsuitable for malaria will become epidemic, whereas in the lower-altitude regions of the East African highlands, epidemic risk will decrease. CONCLUSIONS: We project that climate changes driven by greenhouse-gas and land-use changes will significantly affect the spread of malaria in tropical Africa well before 2050. The geographic distribution of areas where malaria is epidemic might have to be significantly altered in the coming decades. KW - climate change KW - West Africa KW - highland malaria KW - malaria KW - malaria model KW - malaria projection KW - Sahel KW - transmission KW - model KW - highlands KW - temperatures KW - validation KW - resurgence KW - scenarios KW - epidemic KW - deseases Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-135562 VL - 120 IS - 1 ER - TY - THES A1 - Seida, Ahmed Adel T1 - The Immunomodulatory Role of Endogenous Glucocorticoids in Ovarian Cancer T1 - Die immunmodulatorische Bedeutung der lokalen Aktivierung von endogenem Cortison im Ovarialkarzinom N2 - Ovarian cancer currently causes ~6,000 deaths per year in Germany alone. Since only palliative treatment is available for ovarian carcinomas that have developed resistance against platinum-based chemotherapy and paclitaxel, there is a pressing medical need for the development of new therapeutic approaches. As survival is strongly influenced by immunological parameters, immunotherapeutic strategies appear promising. The research of our group thus aims at overcoming tumour immune escape by counteracting immunosuppressive mechanisms in the tumour microenvironment. In this context, we found that tumour-infiltrating myeloid-derived suppressor cells (MDSC) or tumour associated macrophages (TAM) which are abundant in ovarian cancer express high levels of the enzyme 11β-hydroxysteroid dehydrogenase1 (11-HSD1). This oxido-reductase enzyme is essential for the conversion of biologically inactive cortisone into active cortisol. In line with this observation, high endogenous cortisol levels could be detected in serum, ascitic fluid and tumour exudates from ovarian cancer patients. Considering that cortisol exerts strong anti-inflammatory and immunosuppressive effects on immune cells, it appears likely that high endogenous cortisol levels contribute to immune escape in ovarian cancer. We thus hypothesised that local activation of endogenous glucocorticoids could suppress beneficial immune responses in the tumour microenvironment and thereby prevent a successful immunotherapy. To investigate the in vivo relevance of this postulated immune escape mechanism, irradiated PTENloxP/loxP loxP-Stop-loxP-krasG12D mice were reconstituted with hematopoietic stem cells from either glucocorticoid receptor (GR) expressing mice (GRloxP/loxP) or from mice with a T cell-specific glucocorticoid receptor knock-out (lck-Cre GRloxP/loxP) mice. In the host mice, the combination of a conditional PTEN knock-out with a latent oncogenic kras leads to tumour development when a Cre-encoding adenovirus is injected into the ovarian bursa. Using this model, mice that had been reconstituted with GC-insensitive T cells showed better intratumoural T cell infiltration than control mice that had received functionally unaltered GRloxP/loxP cells via adoptive transfer. However, tumour-infiltrating T cells mostly assumed a Foxp3+ (regulatory) phenotype and survival was even shortened in mice with cortisol-insensitive T cells. Thus, endogenous cortisol seems to inhibit immune cell infiltration in ovarian cancer, but productive anti-tumour immune responses might still be prevented by further factors from the tumour microenvironment. Thus, our data did not provide a sufficiently strong rationale to further pursue the antagonisation of glucocorticoid signalling in ovarian cancer patients, Moreover, glucocorticoids are frequently administered to cancer patients to reduce inflammation and swelling and to prevent chemotherapy-related toxic side effects like nausea or hypersensitivity reactions associated with paclitaxel therapy. Thus, we decided to address the question whether specific signalling pathways in innate immune cells, preferentially in NK cells, could still be activated even in the presence of GC. A careful investigation of the various activating NK cell receptors (i.e. NKp30, NKp44, NKp46), DNAM-1 and NKG2D) was thus performed which revealed that NKp30, NKp44 and NKG2D are all down-regulated by cortisol whereas NKp46 is actually induced by cortisol. Interestingly, NKp46 is the only known receptor that is strictly confined to NK cells. Its activation via crosslinking leads to cytokine release and activation of cytotoxic activity. Stimulation of NK cells via NKp46 may contribute to immune-mediated tumour destruction by triggering the lysis of tumour cells and by altering the cytokine pattern in the tumour microenvironment, thereby generating more favourable conditions for the recruitment of antigen-specific immune cells. Accordingly, our observation that even cortisol-treated NK cells can still be activated via NKp46 and CD2 might become valuable for the design of immunotherapies that can still be applied in the presence of endogenous or therapeutically administered glucocorticoids. N2 - Ovarialkarzinome verursachen allein in Deutschland jährlich ca. 6.000 Todesfälle. Da bei Ovarialkarzinomen, die eine Resistenz gegen eine platinbasierte Chemotherapie mit cis-Platin und gegen Paclitaxel entwickelt haben, nur eine palliative Behandlung möglich ist, gibt esbesteht ein dringenden dringender Bedarf an der Entwicklung von neuen Therapieansätzen. Das Überleben der Patientinnen ist sehr stark von immunologischen Parametern beeinflusst, und somit erscheinensodass immuntherapeutische Strategien als ein vielversprechender Ansatzerscheinen. Das Ziel der Forschung in unserer Gruppe ist daher, dem „Tumor-Immun-Escape“ durch eine Verhinderung von immunosuppressiven Mechanismen in im der Tumormikromilieu-Mikroumgebung entgegenzuwirken. In diesem Zusammenhang haben wir gefundenentdeckt, dass Tumor-infiltrierende Suppressorzellen der myeloiden Ursprungsschen Reihe (MDSC) oder Tumor-assoziierte Makrophagen (TAM), die in Ovarialkarzinomen reichlich vorhanden sind, das Enzym 11β-Hydroxysteroid-Dehydrogenase 1 (11β-HSD1) in großer Menge exprimieren. Diese Oxido-Reduktase ist essentiell bei derfür die Umwandlung von biologisch inaktiven Cortison in biologisch aktives Cortisol. In Übereinstimmung damit, werden hohe endogene Cortisol Spiegel in Seren, Azites und Tumorsekreten von Ovarialkarzinom-Patientinnen gemessen. Unter Berücksichtigung der starken anti-inflammatorischen und immunsuppressiven Eigenschaften von Cortisol, erscheint es sehr wahrscheinlich, dass ein hoher endogener Cortisol-Spiegel zum „Immune-Escape“ von Ovarialkarzinomzellen beiträgt. Unsere Vermutung ist Wir stellten daher die Hypothese auf, dass die lokale Aktivierung von endogenen Glucocorticoiden zu einer Unterdrückung der nützlichen Immunantwort in der Tumor-Mikroumgebung führt und eine erfolgreiche Immuntherapie verhindert. Um die in vivo Relevanz dieses postulierten „Immune-Escape“ Mechanismuses zu untersuchen, wurden bestrahlte PTENloxP/loxP loxP-Stop-loxP-krasG12D Mäuse mit Hämatopoetischen hämatopoietischen Stammzellen entweder aus Glucocoprticoid-Rezeptor (GR) exprimierenden Mäusen (GRloxP/loxP) oder aus Mäusen mit einem T-Zell spezifischen Glucocoprticoid-Rezeptor knock-out (lck-Cre GRloxP/loxP) rekonstituiert. In diesen Mäusen führte die Kombination von konditionellem PTEN knock-out mit einer latenten Expression von oncogenen onkogenen Kras zur Tumorentwicklung sobald ein für Cre-Rekombinase codierendes Adenovirus in die Ovarien-ovarielle Bursa injiziert wurdewird. Mit Hilfe von diesesm Modells wurde gezeigt, dass Mäuse, die mit GC-unempfindlichen T-Zellen rekonstituiert worden waren eine bessere intratumorale T-Zell Infiltration zeigten im Vergleich zu Kontroll-Mäusen, die über einen adaptiven Transfer funktionell unveränderte GRloxP/loxP Zellen erhalten hatten. Tumor-infiltrierende T-Zellen haben aber in der Mehrzahl einen hauptsächlich angenommen Foxp3+ (regulatorischen) Phänotyp angenommen, sodass und das Überleben dieser Zellen war sogar verkürzt in Mäusen mit Cortisol-unempfindlichen T-Zellen sogar eine verkürzte Überlebenszeit aufwiesen. Somit scheint endogenes Cortisol die Infiltration von Immunzellen beim Ovarialkarzinom zu inhibieren, aber eine produktive antitumorale Immunantwort könnte scheint trotzdem verhindert werden durch andere Faktoren aus im Tumormikromilieu verhindert zu werden.der Tumor-Mikroumgebung. Somit bieten unsere Daten keine ausreichend starke Begründung, für eineum das Konzept der Antagonisierung endogener,der durch Glucocorticoide ausgelösten ausgelöster Signale in Ovarialkarzinom-Patientinnen weiter zu verfolgen. Des Weiteren werden Glucocorticoide oft Krebspatienten verabreicht, um Entzündungen und Schwellungen zu reduzieren sowie Chemotherapie. bedingte Nebeneffekte wie Übelkeit oder Überempfindlichkeitsreaktionen, die mit einer Paclitaxel-Therapy einhergehen, zu verhindern. Daher wurde der Frage nachgegangen, ob spezifische Signalwege im angeborenem Immunsystem, insbesondere in NK-Zellen, auch in Anwesenheit von GC noch aktiviert werden können. Eine Untersuchung der verschiedenen NK-Zellen aktivierenden Rezeptoren (NKp30, NKp44, NKp46, DNAM-1 und NKG2D) wurde durchgeführt. Dabei wurde eine Herunterregulation von NKp30, NKp44 und NKG2D sowie eine Induktion von NKp46 durch Cortisol festgestellt. Von besonderem Interesse ist, dass NKp46 der einzige bekannte Rezeptor ist, der nur von NK-Zellen exprimiert wird. Seine Aktivierung bewirkt eine Cytokinfreisetzung Zytokinfreisetzung und eine Aktivierung Induktion der zytotoxischen AktivitätNK Zell-Antwort. Eine Stimulation der NK-Zellen über NKp46 könnte zur immun-vermittelten Tumorzerstörung durch Auslösen der Tumorzell-Lyse und durch eine Veränderung des Cytokinexpressionsmusters Zytokinexpressionsmusters in im Tumormikromilieu der Tumor-Mikroumgebung beitragen. Somit würden verbesserte Bedingungen für die Rekrutierung von antigen-spezifischen Immunzellen generiert. Unsere Beobachtung, dass selbst Cortisol behandelte NK-Zellen immer noch über NKp46 und CD2 aktiviert werden können, könnten nützlich zur Entwicklung von Immuntherapien sein, die in Gegenwart von endogenen oder therapeutisch verabreichten Glucocorticoide angewendet werden sollen. KW - Cortison KW - Eierstockkrebs KW - Cortison KW - Ovarialkarzinom KW - Endogenous Glucocorticoids KW - Ovarian Cancer Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-73901 ER - TY - JOUR A1 - Jaschke, Alexander A1 - Chung, Bomee A1 - Hesse, Deike A1 - Kluge, Reinhart A1 - Zahn, Claudia A1 - Moser, Markus A1 - Petzke, Klaus-Jürgen A1 - Brigelius-Flohé, Regina A1 - Puchkov, Dmytro A1 - Koepsell, Hermann A1 - Heeren, Joerg A1 - Joost, Hans-Georg A1 - Schürmann, Annette T1 - The GTPase ARFRP1 controls the lipidation of chylomicrons in the Golgi of the intestinal epithelium JF - Human Molecular Genetics N2 - The uptake and processing of dietary lipids by the small intestine is a multistep process that involves several steps including vesicular and protein transport. The GTPase ADP-ribosylation factor-related protein 1 (ARFRP1) controls the ARF-like 1 (ARL1)-mediated Golgi recruitment of GRIP domain proteins which in turn bind several Rab-GTPases. Here, we describe the essential role of ARFRP1 and its interaction with Rab2 in the assembly and lipidation of chylomicrons in the intestinal epithelium. Mice lacking Arfrp1 specifically in the intestine \((Arfrp1^{vil−/−})\) exhibit an early post-natal growth retardation with reduced plasma triacylglycerol and free fatty acid concentrations. \(Arfrp1^{vil−/−}\) enterocytes as well as Arfrp1 mRNA depleted Caco-2 cells absorbed fatty acids normally but secreted chylomicrons with a markedly reduced triacylglycerol content. In addition, the release of apolipoprotein A-I (ApoA-I) was dramatically decreased, and ApoA-I accumulated in the \(Arfrp1^{vil−/−}\) epithelium, where it predominantly co-localized with Rab2. The release of chylomicrons from Caco-2 was markedly reduced after the suppression of Rab2, ARL1 and Golgin-245. Thus, the GTPase ARFRP1 and its downstream proteins are required for the lipidation of chylo­microns and the assembly of ApoA-I to these particles in the Golgi of intestinal epithelial cells. KW - ARF Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-125658 VL - 21 IS - 14 ER - TY - JOUR A1 - Franke, B. A1 - Faraone, S. V. A1 - Asherson, P. A1 - Buitelaar, J. A1 - Bau, C. H. D. A1 - Ramos-Quiroga, J. A. A1 - Mick, E. A1 - Grevet, E. H. A1 - Johansson, S. A1 - Haavik, J. A1 - Lesch, K.-P. A1 - Cormand, B. A1 - Reif, A. T1 - The genetics of attention deficit/hyperactivity disorder in adults, a review JF - Molecular Psychiatry N2 - The adult form of attention deficit/hyperactivity disorder (aADHD) has a prevalence of up to 5% and is the most severe long-term outcome of this common neurodevelopmental disorder. Family studies in clinical samples suggest an increased familial liability for aADHD compared with childhood ADHD (cADHD), whereas twin studies based on self-rated symptoms in adult population samples show moderate heritability estimates of 30–40%. However, using multiple sources of information, the heritability of clinically diagnosed aADHD and cADHD is very similar. Results of candidate gene as well as genome-wide molecular genetic studies in aADHD samples implicate some of the same genes involved in ADHD in children, although in some cases different alleles and different genes may be responsible for adult versus childhood ADHD. Linkage studies have been successful in identifying loci for aADHD and led to the identification of LPHN3 and CDH13 as novel genes associated with ADHD across the lifespan. In addition, studies of rare genetic variants have identified probable causative mutations for aADHD. Use of endophenotypes based on neuropsychology and neuroimaging, as well as next-generation genome analysis and improved statistical and bioinformatic analysis methods hold the promise of identifying additional genetic variants involved in disease etiology. Large, international collaborations have paved the way for well-powered studies. Progress in identifying aADHD risk genes may provide us with tools for the prediction of disease progression in the clinic and better treatment, and ultimately may help to prevent persistence of ADHD into adulthood. KW - IMpACT KW - persistent ADHD KW - molecular genetics KW - heritability KW - endophenotype Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-124677 VL - 17 ER - TY - THES A1 - Koetschan, Christian T1 - The Eukaryotic ITS2 Database - A workbench for modelling RNA sequence-structure evolution T1 - Die Eukaryotische ITS2 Datenbank - Eine Plattform zur Modellierung von RNA Sequenzstruktur Evolution N2 - In den vergangenen Jahren etablierte sich der Marker „internal transcribed spacer 2" (ITS2) zu einem häufig genutzten Werkzeug in der molekularen Phylogenetik der Eukaryoten. Seine schnell evolvierende Sequenz eignet sich bestens für den Einsatz in niedrigeren phylogenetischen Ebenen. Die ITS2 faltet jedoch auch in eine sehr konservierte Sekundärstruktur. Diese ermöglicht die Unterscheidung weit entfernter Arten. Eine Kombination aus beiden in einer Sequenzstrukturanalyse verbessert die Auflösung des Markers und ermöglicht die Rekonstruktion von robusteren Bäumen auf höherer taxonomischer Breite. Jedoch war die Durchführung solch einer Analyse, die die Nutzung unterschiedlichster Programme und Datenbanken vorraussetzte, für den klassischen Biologen nicht einfach durchführbar. Um diese Hürde zu umgehen, habe ich den „ITS2 Workbench“ entwickelt, eine im Internet nutzbare Arbeitsplattform zur automatisierten sequenzstrukturbasierten phylogenetischen Analyse basierend auf der ITS2 (http://its2.bioapps.biozentrum.uni-wuerzburg.de). Die Entwicklung begann mit der Längenoptimierung unterschiedlicher „Hidden Markov Model“ (HMM)-Topologien, die erfolgreich auf ein Modell zur Sequenzstrukturvorhersage der ITS2 angewandt wurden. Hierbei wird durch die Analyse von Sequenzbestandteilen in Kombination mit der Längenverteilung verschiedener Helixregionen die Struktur vorhergesagt. Anschließend konnte ich HMMs auch bei der Sequenzstrukturgenerierung einsetzen um die ITS2 innerhalb einer gegebenen Sequenz zu lokalisieren. Dieses neu implementierte Verfahren verdoppelte die Anzahl vorhergesagter Strukturen und verkürzte die Laufzeit auf wenige Tage. Zusammen mit weiteren Optimierungen des Homologiemodellierungsprozesses kann ich nun erschöpfend Sekundärstrukturen in mehreren Interationen vorhersagen. Diese Optimierungen liefern derzeit 380.000 annotierte Sequenzen einschließlich 288.000 Strukturvorhersagen. Um diese Strukturen für die Berechnung von Alignments und phylogenetischen Bäumen zu verwenden hab ich das R-Paket „treeforge“ entwickelt. Es ermöglicht die Generierung von Sequenzstrukturalignments auf bis zu vier unterschiedlich kodierten Alphabeten. Damit können erstmals auch strukturelle Basenpaarungen in die Alignmentberechnung mit einbezogen werden, die eine Schätzung neuer Scorematrizen vorraussetzten. Das R-Paket ermöglicht zusätzlich die Rekonstruktion von „Maximum Parsimony“, „Maximum Likelihood“ und „Neighbour Joining“ Bäumen auf allen vier Alphabeten mittels weniger Zeilen Programmcode. Das Paket wurde eingesetzt, um die noch umstrittene Phylogenie der „chlorophyceae“ zu rekonstruieren und könnte in zukünftigen Versionen des ITS2 workbench verwendet werden. Die ITS2 Plattform basiert auf einer modernen und sehr umfangreichen Web 2.0 Oberfläche und beinhaltet neuste AJAX und Web-Service Technologien. Sie umfasst die HMM basierte Sequenzannotation, Strukturvorhersage durch Energieminimierung bzw. Homologiemodellierung, Alignmentberechnung und Baumrekonstruktion basierend auf einem flexiblen Datenpool, der Änderungen am Datensatz automatisch aktualisiert. Zusätzlich wird eine Detektion von Sequenzmotiven ermöglicht, die zur Kontrolle von Annotation und Strukturvorhersage dienen kann. Eine BLAST basierte Suche auf Sequenz- und Strukturebene bietet zusätzlich eine Vereinfachung des Taxonsamplings. Alle Funktionen sowie die Nutzung der ITS2 Webseite sind in einer kurzen Videoanleitung dargestellt. Die Plattform lässt jedoch nur eine bestimmte Größe von Datensätzen zu. Dies liegt vor allem an der erheblichen Rechenleistung, die bei diesen Berechnungen benötigt wird. Um die Funktion dieses Verfahrens auch auf großen Datenmengen zu demonstrieren, wurde eine voll automatisierte Rekonstruktion des Grünalgenbaumes (Chlorophyta) durchgeführt. Diese erfolgreiche, auf dem ITS2 Marker basierende Studie spricht für die Sequenz-Strukturanalyse auf weiteren Daten in der Phylogenetik. Hier bietet der ITS2 Workbench den idealen Ausgangspunkt. N2 - During the past years, the internal transcribed spacer 2 (ITS2) was established as a commonly used molecular phylogenetic marker for the eukaryotes. Its fast evolving sequence is predestinated for the use in low-level phylogenetics. However, the ITS2 also consists of a very conserved secondary structure. This enables the discrimination between more distantly related species. The combination of both in a sequence-structure based analysis increases the resolution of the marker and enables even more robust tree reconstructions on a broader taxonomic range. But, performing such an analysis required the application of different programs and databases making the use of the ITS2 non trivial for the typical biologist. To overcome this hindrance, I have developed the ITS2 Workbench, a completely web-based tool for automated phylogenetic sequence-structure analyses using the ITS2 (http://its2.bioapps.biozentrum.uni-wuerzburg.de). The development started with an optimization of length modelling topologies for Hidden Markov Models (HMMs), which were successfully applied on a secondary structure prediction model of the ITS2 marker. Here, structure is predicted by considering the sequences' composition in combination with the length distribution of different helical regions. Next, I integrated HMMs into the sequence-structure generation process for the delineation of the ITS2 within a given sequence. This re-implemented pipeline could more than double the number of structure predictions and reduce the runtime to a few days. Together with further optimizations of the homology modelling process I can now exhaustively predict secondary structures in several iterations. These modifications currently provide 380,000 annotated sequences including 288,000 structure predictions. To include these structures in the calculation of alignments and phylogenetic trees, I developed the R-package "treeforge". It generates sequence-structure alignments on up to four different coding alphabets. For the first time also structural bonds were considered in alignments, which required the estimation of new scoring matrices. Now, the reconstruction of Maximum Parsimony, Maximum Likelihood as well as Neighbour Joining trees on all four alphabets requires just a few lines of code. The package was used to resolve the controversial chlorophyceaen dataset and could be integrated into future versions of the ITS2 workbench. The platform is based on a modern, feature-rich Web 2.0 user interface equipped with the latest AJAX and Web-service technologies. It performs HMM-based sequence annotation, structure prediction by energy minimization or homology modelling, alignment calculation and tree reconstruction on a flexible data pool that repeats calculations according to data changes. Further, it provides sequence motif detection to control annotation and structure prediction and a sequence-structure based BLAST search, which facilitates the taxon sampling process. All features and the usage of the ITS2 workbench are explained in a video tutorial. However, the workbench bears some limitations regarding the size of datasets. This is caused mainly due to the immense computational power needed for such extensive calculations. To demonstrate the validity of the approach also for large-scale analyses, a fully automated reconstruction of the Chlorophyta (Green Algal) Tree of Life was performed. The successful application of the marker even on large datasets underlines the capabilities of ITS2 sequence-structure analysis and suggests its utilization on further datasets. The ITS2 workbench provides an excellent starting point for such endeavours. KW - Ribosomale RNA KW - Datenbank KW - Marker KW - Phylogenie KW - Evolution KW - Sequenz KW - Struktur KW - Hidden Markov Model KW - Evolution KW - ribosomal RNA KW - workbench KW - sequence-structure Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-73128 ER - TY - THES A1 - Waider, Jonas T1 - The effects of serotonin deficiency in mice: Focus on the GABAergic system T1 - Die Effekte einer Serotonindefizienz in der Maus: Das GABAerge System im Blickpunkt N2 - Based on genetic association and functional imaging studies, reduced function of tryptophan hydroxylase-2 (TPH2) has been shown to be critically involved in the pathophysiology of anxiety-disorders and depression. In order to elucidate the impact of a complete neuronal 5-HT deficiency, mice with a targeted inactivation of the gene encoding Tph2 were generated. Interestingly, survival of Tph2-/- mice, the formation of serotonergic neurons and the pathfinding of their projections was not impaired. Within this thesis, I investigated the influence of 5-HT deficiency on the γ-amino butyric acid (GABA) system. The GABAergic system is implicated in the pathophysiology of anxiety disorders. Therefore, measurement of GABA concentrations in different limbic brain regions was carried out. These measurements were combined with immunohistochemical estimation of GABAergic cell subpopulations in the dorsal hippocampus and amygdala. In Tph2-/- mice GABA concentrations were increased exclusively in the dorsal hippocampus. In heterozygous Tph2+/- mice concentrations of GABA were increased in the amygdala compared to Tph2-/- and wt control mice, while the reverse was found in the prefrontal cortex. The changes in GABA concentrations were accompanied by altered cell density of GABAergic neurons within the basolateral complex of the amygdala and parvalbumin (PV) neurons of the dorsal hippocampus and by adaptational changes of 5-HT receptors. Thus, adaptive changes during the development on the GABA system may reflect altered anxiety-like and depressive-like behavior in adulthood. Moreover, chronic mild stress (CMS) rescues the depressive-like effects induced by 5-HT deficiency. In contrast, 5-HT is important in mediating an increased innate anxiety-like behavior under CMS conditions. This is in line with a proposed dual role of 5-HT acting through different mechanisms on anxiety and depressive-like behavior, which is influenced by gene-environment interaction effects. Further research is needed to disentangle these complex networks in the future. N2 - Genomweite Assoziationsstudien in Kombination mit bildgebenden Studien zeigten, dass eine verringerte Funktion der Tryptophanhydroxylase-2 (Tph2) eine zentrale Rolle in der Pathophysiologie von Angststörungen und Depression spielt. Jedoch sind die einer Angststörung oder Depression zugrundeliegenden genauen Mechanismen noch nicht verstanden. Um den Einfluss einer 5-HT Defizienz zu untersuchen, wurden Tph2 ablatierte (Tph2-/-) Mäuse mittels zielgerichteter Mutagenese generiert. Der Verlust des Tph2 Gens hatte interessanterweise keinen Einfluss auf die Entwicklung vormals serotonerger Neurone und das Überleben der Tiere. In vorherigen Untersuchungen konnte gezeigt werden, dass 5-HT das GABAerge System, welches in der Pathophysiologie von Angststörungen eine zentrale Rolle spielt, in seiner Entwicklung beeinflusst. Daher wurden im Rahmen dieser Arbeit in verschiedenen Gehirnregionen des limbischen Systems Konzentrationen von GABA gemessen. Außerdem wurden mittels immunhistologischer Untersuchungen die Auswirkungen einer 5-HT Defizienz auf GABAerge Neuronenpopulationen hin untersucht. In Tph2-/- Mäusen wurden erhöhte Konzentrationen im Vergleich zu Tph2+/- und wt Kontrollen von GABA im Hippocampus festgestellt. In der Amygdala zeigten die Tph2+/- Mäuse dagegen eine erhöhte Konzentration von GABA. Dieser Effekt auf Tph2+/- Mäuse war umgekehrt im PFC Kortex zu finden, der erniedrigte GABA Konzentrationen in Tph2+/- aufwies. Die Veränderungen auf der neurochemischen Ebene wurden begleitet von veränderten GABAergen Zelldichten im basolateralen Komplex der Amygdala und parvalbuminergen GABAergen Neuronen in der CA3 Region des dorsalen hippocampus. Zudem waren 5-HT1A Rezeptoren und ihre Signalwege hochreguliert. Es scheint, dass der Verlust von 5-HT adaptive Veränderungen in der Entwicklung auf das GABAerge System zur Folge hat und die Basis für verändertes angstähnliches und depressionsähnliches Verhalten im Erwachsenenalter darstellt. Zusätzlich scheint eine 5-HT Defizienz den depressiven Phänotyp im Porsolt Test auszugleichen. Demgegenüber scheint 5-HT wichtig für ein erhöhtes angstähnliches Verhalten unter CMS Bedingungen zu sein. Dies unterstützt die Hypothese einer Doppelrolle von 5-HT innerhalb von Signalwegen und Mechanismen des angst- und depressionsähnlichem Verhalten, die durch Umweltfaktoren wie Stress stark beeinflusst werden. Um den Patienten noch besser helfen zu können erfordert dies in der Zukunft weiterhin eine fundierte Entschlüsselung der dahinter verborgenen Mechanismen. KW - Knockout KW - Serotonin KW - Maus KW - Knockout-Maus KW - GABA KW - serotonin deficiency KW - GABA KW - knockout-mice Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-74565 ER - TY - JOUR A1 - Jin, Jing A1 - Allison, Brendan Z. A1 - Kaufmann, Tobias A1 - Kübler, Andrea A1 - Zhang, Yu A1 - Wang, Xingyu A1 - Cichocki, Andrzej T1 - The Changing Face of P300 BCIs: A Comparison of Stimulus Changes in a P300 BCI Involving Faces, Emotion, and Movement JF - PLoS One N2 - Background: One of the most common types of brain-computer interfaces (BCIs) is called a P300 BCI, since it relies on the P300 and other event-related potentials (ERPs). In the canonical P300 BCI approach, items on a monitor flash briefly to elicit the necessary ERPs. Very recent work has shown that this approach may yield lower performance than alternate paradigms in which the items do not flash but instead change in other ways, such as moving, changing colour or changing to characters overlaid with faces. Methodology/Principal Findings: The present study sought to extend this research direction by parametrically comparing different ways to change items in a P300 BCI. Healthy subjects used a P300 BCI across six different conditions. Three conditions were similar to our prior work, providing the first direct comparison of characters flashing, moving, and changing to faces. Three new conditions also explored facial motion and emotional expression. The six conditions were compared across objective measures such as classification accuracy and bit rate as well as subjective measures such as perceived difficulty. In line with recent studies, our results indicated that the character flash condition resulted in the lowest accuracy and bit rate. All four face conditions (mean accuracy >91%) yielded significantly better performance than the flash condition (mean accuracy = 75%). Conclusions/Significance: Objective results reaffirmed that the face paradigm is superior to the canonical flash approach that has dominated P300 BCIs for over 20 years. The subjective reports indicated that the conditions that yielded better performance were not considered especially burdensome. Therefore, although further work is needed to identify which face paradigm is best, it is clear that the canonical flash approach should be replaced with a face paradigm when aiming at increasing bit rate. However, the face paradigm has to be further explored with practical applications particularly with locked-in patients. KW - ERPS KW - communication KW - TO-target interval KW - visual-evoked potentials KW - brain-computer-interface KW - recognition KW - amplitude KW - paradigm KW - systems Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-134173 VL - 7 IS - 11 ER - TY - JOUR A1 - Ramachandran, Vinoy K. A1 - Shearer, Neil A1 - Jacob, Jobin J. A1 - Sharma, Cynthia M. A1 - Thompson, Arthur T1 - The architecture and ppGpp-dependent expression of the primary transcriptome of Salmonella Typhimurium during invasion gene expression JF - BMC Genomics N2 - Background: Invasion of intestinal epithelial cells by Salmonella enterica serovar Typhimurium (S. Typhimurium) requires expression of the extracellular virulence gene expression programme (STEX), activation of which is dependent on the signalling molecule guanosine tetraphosphate (ppGpp). Recently, next-generation transcriptomics (RNA-seq) has revealed the unexpected complexity of bacterial transcriptomes and in this report we use differential RNA sequencing (dRNA-seq) to define the high-resolution transcriptomic architecture of wildtype S. Typhimurium and a ppGpp null strain under growth conditions which model STEX. In doing so we show that ppGpp plays a much wider role in regulating the S. Typhimurium STEX primary transcriptome than previously recognised. Results: Here we report the precise mapping of transcriptional start sites (TSSs) for 78% of the S. Typhimurium open reading frames (ORFs). The TSS mapping enabled a genome-wide promoter analysis resulting in the prediction of 169 alternative sigma factor binding sites, and the prediction of the structure of 625 operons. We also report the discovery of 55 new candidate small RNAs (sRNAs) and 302 candidate antisense RNAs (asRNAs). We discovered 32 ppGpp-dependent alternative TSSs and determined the extent and level of ppGpp-dependent coding and non-coding transcription. We found that 34% and 20% of coding and non-coding RNA transcription respectively was ppGpp-dependent under these growth conditions, adding a further dimension to the role of this remarkable small regulatory molecule in enabling rapid adaptation to the infective environment. Conclusions: The transcriptional architecture of S. Typhimurium and finer definition of the key role ppGpp plays in regulating Salmonella coding and non-coding transcription should promote the understanding of gene regulation in this important food borne pathogen and act as a resource for future research. KW - legionella pneumophila KW - growth rate control KW - escherichia coli K-12 KW - pathogenicity island 2 KW - bacterial signal molecule KW - enterica serovar typhimurium KW - messenger RNA KW - protein synthesis KW - sationary phase KW - environmental regulation Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-130625 VL - 13 IS - 25 ER - TY - THES A1 - Schelter, Jörg T1 - The Aharonov-Bohm effect and resonant scattering in graphene T1 - Aharonov-Bohm-Effekt und resonante Streuung in Graphen N2 - In this thesis, the electronic transport properties of mesoscopic condensed matter systems based on graphene are investigated by means of numerical as well as analytical methods. In particular, it is analyzed how the concepts of quantum interference and disorder, which are essential to mesoscopic devices in general, are affected by the unique electronic and transport properties of the graphene material system. We consider the famous Aharonov–Bohm effect in ring-shaped transport geometries, and, besides providing an overview over the recent developments on the subject, we study the signatures of fundamental phenomena such as Klein tunneling and specular Andreev reflection, which are specific to graphene, in the magnetoconductance oscillations. To this end, we introduce and utilize a variant of the well-known recursive Green’s function technique, which is an efficient numerical method for the calculation of transport observables in effectively non-interacting open quantum systems in the framework of a tight binding model. This technique is also applied to study the effects of a specific kind of disorder, namely short-range resonant scatterers, such as strongly bound adatoms or molecules, that can be modeled as vacancies in the graphene lattice. This numerical analysis of the conductance in the presence of resonant scatterers in graphene leads to a non-trivial classification of impurity sites in the graphene lattice and is further substantiated by an independent analytical treatment in the framework of the Dirac equation. The present thesis further contains a formal introduction to the topic of non-equilibrium quantum transport as appropriate for the development of the numerical technique mentioned above, a general introduction to the physics of graphene with a focus on the particular phenomena investigated in this work, and a conclusion where the obtained results are summarized and open questions as well as potential future developments are highlighted. N2 - In dieser Arbeit werden die elektronischen Transporteigenschaften von Graphen-basierten mesoskopischen Festkörpersystemen mittels numerischer und analytischer Methoden untersucht. Im Besonderen wird analysiert, wie Konzepte von Quanteninterferenz und Unordnung, die eine wesentliche Rolle für mesoskopische Systeme spielen, durch die einzigartigen elektronischen und Transporteigenschaften von Graphen beeinflusst werden. Wir betrachten den berühmten Aharonov-Bohm-Effekt in ringförmigen Transportgeometrien, geben einen Überblick über die Entwicklung dieses Themas in den letzten Jahren und befassen uns mit den charakteristischen Merkmalen, die fundamentale Phänomene wie Klein-Tunneln und gerichtete Andreev-Reflexion, welche spezifisch für Graphen sind, in den Magnetooszillationen der elektrischen Leitfähigkeit aufweisen. Dazu führen wir eine Variante der Methode der rekursiven Greenschen Funktionen ein, die ein effizientes numerisches Verfahren zur Berechnung von Transportobservablen in effektiv nicht-wechselwirkenden, offenen Quantensystemen im Rahmen eines „tight binding“-Modells darstellt. Diese Methode wird desweiteren zur Erforschung eines speziellen Typs von Unordnung herangezogen, nämlich kurzreichweitiger, resonanter Streuzentren wie stark gebundene Adatome oder Moleküle, die als Fehlstellen in der Graphen-Gitterstruktur modelliert werden können. Diese numerische Analyse der elektrischen Leitfähigkeit bei Anwesenheit resonanter Streuzentren in Graphen führt zu einer nicht-trivialen Klassifizierung von Fremdatom-Gitterplätzen innerhalb des Graphen-Gitters und wird durch eine unabhängige analytische Behandlung im Rahmen der Dirac-Gleichung bekräftigt. Die vorliegende Arbeit enthält weiterhin eine formale Einführung in das Thema des Nichtgleichgewichts-Quantentransports, wie es für die Entwicklung der genannten numerischen Methode dienlich ist, eine allgemeine Einführung in die Physik von Graphen mit Fokus auf die speziellen Aspekte, die in dieser Arbeit untersucht werden, sowie eine abschließende Darstellung, in der die erhaltenen Ergebnisse zusammengefasst und offene Fragen sowie mögliche zukünftige Entwicklungen hervorgehoben werden. KW - Graphen KW - Aharonov-Bohm-Effekt KW - Resonanzstreuung KW - graphene KW - Aharonov-Bohm effect KW - resonant scattering KW - recursive Green's functions KW - Direkte numerische Simulation KW - Festkörperphysik Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-74662 ER - TY - JOUR A1 - Pils, Stefan A1 - Kopp, Kathrin A1 - Peterson, Lisa A1 - Tascon, Julia Delgado A1 - Nyffenegger-Jann, Naja J. A1 - Hauck, Christof R. T1 - The Adaptor Molecule Nck Localizes the WAVE Complex to Promote Actin Polymerization during CEACAM3-Mediated Phagocytosis of Bacteria JF - PLoS One N2 - Background: CEACAM3 is a granulocyte receptor mediating the opsonin-independent recognition and phagocytosis of human-restricted CEACAM-binding bacteria. CEACAM3 function depends on an intracellular immunoreceptor tyrosine-based activation motif (ITAM)-like sequence that is tyrosine phosphorylated by Src family kinases upon receptor engagement. The phosphorylated ITAM-like sequence triggers GTP-loading of Rac by directly associating with the guanine nucleotide exchange factor (GEF) Vav. Rac stimulation in turn is critical for actin cytoskeleton rearrangements that generate lamellipodial protrusions and lead to bacterial uptake. Principal Findings: In our present study we provide biochemical and microscopic evidence that the adaptor proteins Nck1 and Nck2, but not CrkL, Grb2 or SLP-76, bind to tyrosine phosphorylated CEACAM3. The association is phosphorylation-dependent and requires the Nck SH2 domain. Overexpression of the isolated Nck1 SH2 domain, RNAi-mediated knock-down of Nck1, or genetic deletion of Nck1 and Nck2 interfere with CEACAM3-mediated bacterial internalization and with the formation of lamellipodial protrusions. Nck is constitutively associated with WAVE2 and directs the actin nucleation promoting WAVE complex to tyrosine phosphorylated CEACAM3. In turn, dominant-negative WAVE2 as well as shRNA-mediated knock-down of WAVE2 or the WAVE-complex component Nap1 reduce internalization of bacteria. Conclusions: Our results provide novel mechanistic insight into CEACAM3-initiated phagocytosis. We suggest that the CEACAM3 ITAM-like sequence is optimized to co-ordinate a minimal set of cellular factors needed to efficiently trigger actin-based lamellipodial protrusions and rapid pathogen engulfment. KW - activation KW - neisseria gonorrhoeae KW - human pathogens KW - T cell KW - signal transduction KW - escherichia coli KW - epithelial cells KW - tyrosine kinase KW - receptor KW - adhesion Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-131747 VL - 7 IS - 3 ER - TY - JOUR A1 - Samimi, C. A1 - Fink, A. H. A1 - Paeth, H. T1 - The 2007 flood in the Sahel: causes, characteristics and its presentation in the media and FEWS NET JF - Natural Hazards and Earth System Sciences N2 - During the rainy season in 2007, reports about exceptional rains and floodings in the Sahel were published in the media, especially in August and September. Institutions and organizations like the World Food Programme (WFP) and FEWS NET put the events on the agenda and released alerts and requested help. The partly controversial picture was that most of the Sahel faced a crisis caused by widespread floodings. Our study shows that the rainy season in 2007 was exceptional with regard to rainfall amount and return periods. In many areas the event had a return period between 1 and 50 yr with high spatial heterogeneity, with the exception of the Upper Volta basin, which yielded return periods of up to 1200 yr. Despite the strong rainfall, the interpretation of satellite images show that the floods were mainly confined to lakes and river beds. However, the study also proves the difficulties in assessing the meteorological processes and the demarcation of flooded areas in satellite images without ground truthing. These facts and the somewhat vague and controversial reports in the media and FEWS NET demonstrate that it is crucial to thoroughly analyze such events at a regional and local scale involving the local population. KW - prediction KW - satellite rainfall products KW - tropical North-Africa KW - West-Africa KW - climate change KW - summer rainfall KW - variability KW - SST KW - teleconnection KW - validation Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-131790 VL - 12 IS - 2 SP - 313 EP - 325 ER - TY - JOUR A1 - Radermacher, Kim A. A1 - Wingler, Kirstin A1 - Kleikers, Pamela A1 - Altenhöfer, Sebastian A1 - Hermans, Johannes J. R. A1 - Kleinschnitz, Christoph A1 - Schmidt, Harald H. H. W. T1 - The 1027th target candidate in stroke: Will NADPH oxidase hold up? JF - Experimental and Translational Stroke Medicine N2 - As recently reviewed, 1026 neuroprotective drug candidates in stroke research have all failed on their road towards validation and clinical translation, reasons being quality issues in preclinical research and publication bias. Quality control guidelines for preclinical stroke studies have now been established. However, sufficient understanding of the underlying mechanisms of neuronal death after stroke that could be possibly translated into new therapies is lacking. One exception is the hypothesis that cellular death is mediated by oxidative stress. Oxidative stress is defined as an excess of reactive oxygen species (ROS) derived from different possible enzymatic sources. Among these, NADPH oxidases (NOX1-5) stand out as they represent the only known enzyme family that has no other function than to produce ROS. Based on data from different NOX knockout mouse models in ischemic stroke, the most relevant isoform appears to be NOX4. Here we discuss the state-of-the-art of this target with respect to stroke and open questions that need to be addressed on the path towards clinical translation. KW - NADPH oxidases (NOX) KW - stroke therapy KW - oxidative stress Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-124197 VL - 4 IS - 11 ER - TY - JOUR A1 - Jain, Preetesh A1 - Javdan, Mohammad A1 - Feger, Franziska K. A1 - Chiu, Pui Yan A1 - Sison, Cristina A1 - Damle, Rajendra N. A1 - Bhuiya, Tawfiqul A. A1 - Sen, Filiz A1 - Abruzzo, Lynne V. A1 - Burger, Jan A. A1 - Rosenwald, Andreas A1 - Allen, Steven L. A1 - Kolitz, Jonathan E. A1 - Rai, Kanti R. A1 - Chiorazzi, Nicholas A1 - Sherry, Barbara T1 - Th17 and non-Th17 interleukin-17-expressing cells in chronic lymphocytic leukemia: delineation, distribution, and clinical relevance JF - Haematologica N2 - Background The levels and clinical relevance of Th17 cells and other interleukin-17-producing cells have not been analyzed in chronic lymphocytic leukemia. The objective of this study was to quantify blood and tissue levels of Th17 and other interleukin-17-producing cells in patients with this disease and correlate blood levels with clinical outcome. Design and Methods: Intracellular interleukin-17A was assessed in blood and splenic mononuclear cells from patients with chronic lymphocytic leukemia and healthy subjects using flow cytometry. Interleukin-17A-producing cells were analyzed in formalin-fixed, paraffin-embedded spleen and lymph node sections using immunohistochemistry and immunofluorescence. Results: The absolute numbers of Th17 cells in peripheral blood mononuclear cells and the percentages of Th17 cells in spleen cell suspensions were higher in patients with chronic lymphocytic leukemia than in healthy subjects; in six out of eight paired chronic lymphocytic leukemia blood and spleen sample comparisons, Th17 cells were enriched in spleen suspensions. Circulating Th17 levels correlated with better prognostic markers and longer overall survival of the patients. Two "non-Th17" interleukin-17-expressing cells were identified in chronic lymphocytic leukemia spleens: proliferating cells of the granulocytic lineage and mature mast cells. Granulocytes and mast cells in normal spleens did not express interleukin-17. Conversely, both chronic lymphocytic leukemia and healthy lymph nodes contained similar numbers of interleukin-17+ mast cells as well as Th17 cells. Conclusions: Th17 cells are elevated in chronic lymphocytic leukemia patients with better prognostic markers and correlate with longer survival. Furthermore, non-Th17 interleukin-17A-expressing cells exist in chronic lymphocytic leukemia spleens as maturing granulocytes and mature mast cells, suggesting that the microenvironmental milieu in leukemic spleens promotes the recruitment and/or expansion of Th17 and other IL-17-expressing cells. The pathophysiology of Th17 and non-Th17-interleukin-producing cells in chronic lymphocytic leukemia and their distributions and roles in this disease merit further study. KW - disease KW - helper T cells KW - T(H)17 cells KW - tumor microenvironment KW - multiple myeloma KW - up regulation KW - mast cells KW - lineage KW - pathway KW - IL-17 Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-131290 VL - 97 IS - 4 ER - TY - JOUR A1 - Hommers, Wilfried A1 - Lewand, Martin A1 - Ehrmann, Dominic T1 - Testing the moral algebra of two Kohlbergian informers JF - Psícologica N2 - This paper seeks to unify two major theories of moral judgment: Kohlberg's stage theory and Anderson's moral information integration theory. Subjects were told about thoughts of actors in Kohlberg's classic altruistic Heinz dilemma and in a new egoistical dilemma. These actors's thoughts represented Kohlberg's stages I (Personal Risk) and IV (Societal Risk) and had three levels, High, Medium, and Low. They were presented singly and in a 3 x 3 integration design. Subjects judged how many months of prison the actor deserved. The data supported the averaging model of moral integration theory, whereas Kohlberg's theory has no way to handle the integration problem. Following this, subjects ranked statements related to Kohlberg's first four stages in a procedure similar to that of Rest (1975). Higher score went with larger effect of Societal Risk as predicted by Kohlberg's theory. But contrary to Kohlberg's theory, no age trends were found. Also strongly contrary to Kohlberg's theory, effects of Personal Risk (Stage I) and Societal Risk (Stage IV) correlated positively. KW - integration KW - information KW - judgements KW - intent KW - damage KW - rules Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-133917 VL - 33 IS - 3 ER - TY - JOUR A1 - Hintzsche, Henning A1 - Jastrow, Christian A1 - Kleine-Ostmann, Thomas A1 - Kärst, Uwe A1 - Schrader, Thorsten A1 - Stopper, Helga T1 - Terahertz electromagnetic fields (0.106 THz) do not induce manifest genomic damage in vitro N2 - Terahertz electromagnetic fields are non-ionizing electromagnetic fields in the frequency range from 0.1 to 10 THz. Potential applications of these electromagnetic fields include the whole body scanners, which currently apply millimeter waves just below the terahertz range, but future scanners will use higher frequencies in the terahertz range. These and other applications will bring along human exposure to these fields. Up to now, only a limited number of investigations on biological effects of terahertz electromagnetic fields have been performed. Therefore, research is strongly needed to enable reliable risk assessment. Cells were exposed for 2 h, 8 h, and 24 h with different power intensities ranging from 0.04 mW/cm2 to 2 mW/cm2, representing levels below, at, and above current safety limits. Genomic damage on the chromosomal level was measured as micronucleus formation. DNA strand breaks and alkali-labile sites were quantified with the comet assay. No DNA strand breaks or alkali-labile sites were observed as a consequence of exposure to terahertz electromagnetic fields in the comet assay. The fields did not cause chromosomal damage in the form of micronucleus induction. KW - Toxikologie Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-76268 ER -