TY - GEN A1 - Schwarzenberger, Anke A1 - Christjani, Mark A1 - Wacker, Alexander T1 - Longevity of Daphnia and the attenuation of stress responses by melatonin N2 - The widespread occurrence of melatonin in prokaryotes as well as eukaryotes indicates that this indoleamine is considerably old. This high evolutionary age has led to the development of diverse functions of melatonin in different organisms, such as the detoxification of reactive oxygen species and anti-stress effects. In insects, i.e. Drosophila, the addition of melatonin has also been shown to increase the life span of this arthropod, probably by reducing age-related increasing oxidative stress. Although the presence of melatonin was recently found to exist in the ecological and toxicological model organism Daphnia, its function in this cladoceran has thus far not been addressed. Therefore, we challenged Daphnia with three different stressors in order to investigate potential stress-response attenuating effects of melatonin. i) Female and male daphnids were exposed to melatonin in a longevity experiment, ii) Daphnia were confronted with stress signals from the invertebrate predator Chaoborus sp., and iii) Daphnia were grown in high densities, i.e. under crowding-stress conditions. Results In our experiments we were able to show that longevity of daphnids was not affected by melatonin. Therefore, age-related increasing oxidative stress was probably not compensated by added melatonin. However, melatonin significantly attenuated Daphnia’ s response to acute predator stress, i.e. the formation of neckteeth which decrease the ability of the gape-limited predator Chaoborus sp. to handle their prey. In addition, melatonin decreased the extent of crowding-related production of resting eggs of Daphnia. Conclusions Our results confirm the effect of melatonin on inhibition of stress-signal responses of Daphnia. Until now, only a single study demonstrated melatonin effects on behavioral responses due to vertebrate kairomones, whereas we clearly show a more general effect of melatonin: i) on morphological predator defense induced by an invertebrate kairomone and ii) on life history characteristics transmitted by chemical cues from conspecifics. Therefore, we could generally confirm that melatonin plays a role in the attenuation of responses to different stressors in Daphnia. T3 - Zweitveröffentlichungen der Universität Potsdam : Mathematisch-Naturwissenschaftliche Reihe - 405 KW - Daphnia KW - chaoborus kairomone KW - melatonin KW - crowding KW - longevity KW - stress response Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-401476 ER - TY - GEN A1 - Liesenjohann, Monique A1 - Liesenjohann, Thilo A1 - Palme, Rupert A1 - Eccard, Jana T1 - Differential behavioural and endocrine responses of common voles (Microtus arvalis) to nest predators and resource competitors N2 - Background: Adaptive behavioural strategies promoting co-occurrence of competing species are known to result from a sympatric evolutionary past. Strategies should be different for indirect resource competition (exploitation, e.g., foraging and avoidance behaviour) than for direct interspecific interference (e.g., aggression, vigilance, and nest guarding). We studied the effects of resource competition and nest predation in sympatric small mammal species using semi-fossorial voles and shrews, which prey on vole offspring during their sensitive nestling phase. Experiments were conducted in caged outdoor enclosures. Focus common vole mothers (Microtus arvalis) were either caged with a greater white-toothed shrew (Crocidura russula) as a potential nest predator, with an herbivorous field vole (Microtus agrestis) as a heterospecific resource competitor, or with a conspecific resource competitor. Results: We studied behavioural adaptations of vole mothers during pregnancy, parturition, and early lactation, specifically modifications of the burrow architecture and activity at burrow entrances. Further, we measured pre- and postpartum faecal corticosterone metabolites (FCMs) of mothers to test for elevated stress hormone levels. Only in the presence of the nest predator were prepartum FCMs elevated, but we found no loss of vole nestlings and no differences in nestling body weight in the presence of the nest predator or the heterospecific resource competitor. Although the presence of both the shrew and the field vole induced prepartum modifications to the burrow architecture, only nest predators caused an increase in vigilance time at burrow entrances during the sensitive nestling phase. Conclusion: Voles displayed an adequate behavioural response for both resource competitors and nest predators. They modified burrow architecture to improve nest guarding and increased their vigilance at burrow entrances to enhance offspring survival chances. Our study revealed differential behavioural adaptations to resource competitors and nest predators. T3 - Zweitveröffentlichungen der Universität Potsdam : Mathematisch-Naturwissenschaftliche Reihe - 402 KW - behavioural adaptations KW - small mammals KW - interspecific interactions KW - nest predation KW - stress response KW - faecal corticosterone metabolites KW - burrow system KW - shrews KW - voles Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-401184 ER - TY - THES A1 - Mauri, Marco T1 - A model for sigma factor competition in bacterial cells N2 - Bacteria respond to changing environmental conditions by switching the global pattern of expressed genes. In response to specific environmental stresses the cell activates several stress-specific molecules such as sigma factors. They reversibly bind the RNA polymerase to form the so-called holoenzyme and direct it towards the appropriate stress response genes. In exponentially growing E. coli cells, the majority of the transcriptional activity is carried out by the housekeeping sigma factor, while stress responses are often under the control of alternative sigma factors. Different sigma factors compete for binding to a limited pool of RNA polymerase (RNAP) core enzymes, providing a mechanism for cross talk between genes or gene classes via the sharing of expression machinery. To quantitatively analyze the contribution of sigma factor competition to global changes in gene expression, we develop a thermodynamic model that describes binding between sigma factors and core RNAP at equilibrium, transcription, non-specific binding to DNA and the modulation of the availability of the molecular components. Association of housekeeping sigma factor to RNAP is generally favored by its abundance and higher binding affinity to the core. In order to promote transcription by alternative sigma subunits, the bacterial cell modulates the transcriptional efficiency in a reversible manner through several strategies such as anti-sigma factors, 6S RNA and generally any kind of transcriptional regulators (e.g. activators or inhibitors). By shifting the outcome of sigma factor competition for the core, these modulators bias the transcriptional program of the cell. The model is validated by comparison with in vitro competition experiments, with which excellent agreement is found. We observe that transcription is affected via the modulation of the concentrations of the different types of holoenzymes, so saturated promoters are only weakly affected by sigma factor competition. However, in case of overlapping promoters or promoters recognized by two types of sigma factors, we find that even saturated promoters are strongly affected. Active transcription effectively lowers the affinity between the sigma factor driving it and the core RNAP, resulting in complex cross talk effects and raising the question of how their in vitro measure is relevant in the cell. We also estimate that sigma factor competition is not strongly affected by non-specific binding of core RNAPs, sigma factors, and holoenzymes to DNA. Finally, we analyze the role of increased core RNAP availability upon the shut-down of ribosomal RNA transcription during stringent response. We find that passive up-regulation of alternative sigma-dependent transcription is not only possible, but also displays hypersensitivity based on the sigma factor competition. Our theoretical analysis thus provides support for a significant role of passive control during that global switch of the gene expression program and gives new insights into RNAP partitioning in the cell. N2 - Bakterien reagieren auf Aenderungen in ihren Umgebungsbedingungen indem sie global das Genexpressionsprogramm umschalten. Die Zelle aktiviert, als spezifische Reaktion auf Stressbedingungen, mehrere charakteristische Molekuele wie zum Beispiel die Sigmafaktoren. Diese binden reversibel an die RNA Polymerase (RNAP), mit der sie einen Komplex bilden das sogenannte Holoenzym und steuern sie als Reaktion auf den Stress zu den entsprechenden Genen. In exponentiell wachsenden E. Coli Zellen wird das Meiste der Transkription von einem sogenannten Haushaltssigmafaktor organisiert. Wohingegen Stressreaktionen haeufig von alternativen Sigmafaktoren kontrolliert werden. Die verschiedenen Sigmafaktoren konkurrieren um einen begrenzten Pool von RNAP Coreenzymen, womit die Expression einzelner Gene oder Genklassen beeinflusst wird, da sie sich die Maschienerie teilen. Um den Beitrag der Sigmafaktorkonkurrenz an der gesamten Veraenderung der Genexpression quantitativ zu analysieren, haben wir ein theoretisches Modell entwickelt, welches das Binden von Sigmafaktoren mit RNAP Coreenzymen im gleichgewicht, die Transkription, das nichtspezifische Binden an die DNA sowie die Modulation verfuegbarer molekularer Komponenten beschreibt. Normalerweise wird die Assoziation des Haushaltssigmafaktors mit dem RNAP Coreenzym beguenstigt durch dessen grosse Anzahl und die hohe Bindungsaffinitaet. Daher nutzen bakterielle Zellen verschiedene, reversibele Strategien um die Transkription durch alternative Holoenzyme zu foerdern. Dazu gehoeren Anti-Sigmafaktoren, 6S RNA und generell beliebige Transkriptionsregulatoren (z.B.: Aktivatoren oder Repressoren). Sie beeinflussen das Transkriptionsprogramm der Zelle indem sie das Resultat der Sigmafaktorkonkurrenz um die RNAP Coreenzyme zugunsten eines der Sigmafaktoren verschieben. Das Modell kann validiert werden durch Vergleiche mit in vitro Konkurrenzexperimenten, die exzellente uebereinstimmung zeigen. Wir koennen feststellen, dass die Transkription durch Konzentrationsaenderungen der verschiedenen Holoenzyme beeinflusst wird, daher ist der Effekt der Sigmafaktorkonkurrenz klein bei saturierten Promotoren. Was sich jedoch aendert bei sich ueberlappenden Promotoren oder Promotoren, die von zwei verschiedenen Sigmafaktoren erkannt werden. In diesen Faellen sehen wir einen grossen Effekt. Transkription fuehrt zu effektiv abgesekten Affinitaet zwischen den zugehoerigen Sigmafaktoren und den RNAP Coreenzymen, was zu komplizierten Verhalten fuehrt und die Frage aufwirft, inwieweit in vitro gemessenen Effekte in der Zelle wiederzufinden sind. Wir koennen den Einfluss nichtspezifischen Bindens der RNAPs, der Sigmafaktoren und der Holoenzyme an die DNA abschaetzen. Als letztes analysieren wir die Konkurrenz waehrend der "Stringent Response". Hierbei wird die Transkription der ribosomalen RNA unterbrochen was die Anzahl der freien RNAP Coreenzyme stark erhoeht. Wir sehen, dass das passive Hochregeln des alternativen sigmafaktorabhaengigen Transkriptionsprogramms durch Sigmafaktorkokurrenz moeglich und sogar hypersensitiv ist. Unsere theoretische Analyse zeigt, dass die passive Kontrolle in diesem Fall eine signifikante Rolle im globalen umschalten des Transkriptionsprogramms spielt und liefert neue Erkenntnisse zur RNAP Partitionierung in der Zelle. T2 - Ein Modell für die Konkurrenz zwischen Sigmafaktoren in Bakterienzellen KW - biophysics KW - systems biology KW - gene regulation KW - stress response KW - Biophysik KW - Systembiologie KW - Genregulation KW - Stressantwort Y1 - 2014 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-72098 ER -