TY - THES A1 - Lambour, Benjamin T1 - Regulation of sphingolipid long-chain bases during cell death reactions and abiotic stress in \(Arabidopsis\) \(thaliana\) T1 - Regulation von Sphingobasen während der Zelltodreaktion und abiotischem Stress in \(Arabidopsis\) \(thaliana\) N2 - Sphingobasen (LCBs) sind die Bausteine der Biosynthese von Sphingolipiden. Sie werden als Strukturelemente der pflanzlichen Zellmembran definiert und spielen eine wichtige Rolle für das Schicksal der Zellen. Komplexe Ceramide machen einen wesentlichen Teil der gesamten Sphingolipide aus, die einen großen Teil der eukaryotischen Membranen bilden. Gleichzeitig sind LCBs bekannte Signalmoleküle für zelluläre Prozesse in Eukaryonten und sind an Signalübertragungswegen in Pflanzen beteiligt. Es hat sich gezeigt, dass hohe LCB-Konzentrationen mit der Induktion des programmierten Zelltods sowie mit dem durch Pathogene ausgelösten Zelltod in Verbindung stehen. Mehrere Studien haben die regulierende Funktion der Sphingobasen beim programmierten Zelltod (PCD) in Pflanzen bestätigt: (i) Spontaner PCD und veränderte Zelltodreaktionen, die durch mutierte verwandte Gene des Sphingobasen-Stoffwechsels verursacht werden. (ii) Zelltodbedingungen erhöhen den Gehalt an LCBs. (iii) PCD aufgrund eines gestörten Sphingolipid-Stoffwechsels, der durch von nekrotrophen Krankheitserregern produzierte Toxine wie Fumonisin B1 (FB1) hervorgerufen wird. Um den Zelltod zu verhindern und die Zelltodreaktion zu kontrollieren, kann daher die Regulierung des Gehalts an freien LCBs entscheidend sein. Die Ergebnisse der vorliegenden Studie stellten das Verständnis der Sphingobasen und Sphingolipidspiegel während der PCD in Frage. Wir lieferten eine detaillierte Analyse der Sphingolipidspiegel, die Zusammenhänge zwischen bestimmten Sphingolipidarten und dem Zelltod aufzeigte. Darüber hinaus ermöglichte uns die Untersuchung der Sphingolipid-Biosynthese ein Verständnis des Fluxes nach Akkumulation hoher LCB-Konzentrationen. Weitere Analysen von Abbauprodukten oder Sphingolipid-Mutantenlinien wären jedoch erforderlich, um vollständig zu verstehen, wie die Pflanze mit hohen Mengen an Sphingobasen umgeht. N2 - Sphingolipid long-chain bases (LCBs) are the building blocks of the biosynthesis of sphingolipids. They are defined as structural elements of the plant cell membrane and play an important role determining the fate of the cells. Complex ceramides represent a substantial fraction of total sphingolipids which form a major part of eukaryotic membranes. At the same time, LCBs are well known signaling molecules of cellular processes in eukaryotes and are involved in signal transduction pathways in plants. High levels of LCBS have been shown to be associated with the induction of programmed cell death as well as pathogen-derived toxin-induced cell death. Indeed, several studies confirmed the regulatory function of sphingobases in plant programmed cell death (PCD): (i) Spontaneous PCD and altered cell death reaction caused by mutated related genes of sphingobase metabolism. (ii) Cell death conditions increases levels of LCBs. (iii) PCD due to interfered sphingolipid metabolism provoked by toxins produced from necrotrophic pathogens, such as Fumonisin B1 (FB1). Therefore, to prevent cell death and control cell death reaction, the regulation of levels of free LCBs can be crucial. The results of the present study challenged the comprehension of sphingobases and sphingolipid levels during PCD. We provided detailed analysis of sphingolipids levels that revealed correlations of certain sphingolipid species with cell death. Moreover, the investigation of sphingolipid biosynthesis allowed us to understand the flux after the accumulation of high LCB levels. However, further analysis of degradation products or sphingolipid mutant lines, would be required to fully understand how high levels of sphingobases are being treated by the plant. KW - PCD KW - Sphingolipids KW - LCB KW - Ackerschmalwand KW - programmed cell death KW - arabidopsis thaliana KW - abiotic stress Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-325916 ER - TY - JOUR A1 - Barres, B. A. A1 - Schmid, R. A1 - Sendtner, Michael A1 - Raff, Martin C. T1 - Multiple extracellular signals are required for long-term oligodendrocyte survival N2 - We showed previously that oligodendrocytes and their precursors require continuous signalling by protein trophic factors to avoid programmed cell death in culture. Here we show that three classes of such trophic factors promote oligodendrocyte survival in vitro: (1) insulin and insulin-like growth factors (IGFs), (2) neurotrophins, particularly neurotrophin-3 (NT -3), and (3) ciliary-neurotrophic factor (CNTF), leukemia inhibitory factor (LIF) and interleukin 6 (IL-6). A single factor, or combinations of factors within the same class, promote only short-term survival of oligodendrocytes and their precursors, while combinations of factors from different classes promote survival additively. Long-term survival of oligodendrocytes in vitro requires at least one factor from each class, suggesting that multiple signals may be required for long-term oligodendrocyte survival in vivo. We also show that CNTF promotes oligodendrocyte survival in vivo, that platelet-derived growth factor (PDGF) can promote the survival of oligodendrocyte precursors in vitro by acting on a novel, very high affinity PDGF receptor, and that, in addition to its effect on survival, NT-3 is a potent mitogen for oligodendrocyte precursor cells. KW - neurotrophins KW - programmed cell death KW - apoptosis KW - ciliary-neurotrophic factor KW - interleukin 6 KW - insulin KW - insulin-likegrowth factor I Y1 - 1993 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-42644 ER -