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A metabolic switch regulates the transition between growth and diapause in C. elegans

机译:代谢交换机调节C.秀丽隐杆线的生长和延展之间的过渡

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摘要

Abstract Background Metabolic activity alternates between high and low states during different stages of an organism’s life cycle. During the transition from growth to quiescence, a major metabolic shift often occurs from oxidative phosphorylation to glycolysis and gluconeogenesis. We use the entry of Caenorhabditis elegans into the dauer larval stage, a developmentally arrested stage formed in response to harsh environmental conditions, as a model to study the global metabolic changes and underlying molecular mechanisms associated with growth to quiescence transition. Results Here, we show that the metabolic switch involves the concerted activity of several regulatory pathways. Whereas the steroid hormone receptor DAF-12 controls dauer morphogenesis, the insulin pathway maintains low energy expenditure through DAF-16/FoxO, which also requires AAK-2/AMPKα. DAF-12 and AAK-2 separately promote a shift in the molar ratios between competing enzymes at two key branch points within the central carbon metabolic pathway diverting carbon atoms from the TCA cycle and directing them to gluconeogenesis. When both AAK-2 and DAF-12 are suppressed, the TCA cycle is active and the developmental arrest is bypassed. Conclusions The metabolic status of each developmental stage is defined by stoichiometric ratios within the constellation of metabolic enzymes driving metabolic flux and controls the transition between growth and quiescence.
机译:在有机体的生命周期的不同阶段高和低状态之间的抽象背景代谢活性交替。在从增速平静的过渡,一个主要的代谢转变往往是从氧化磷酸化糖酵解和糖异生发生。我们使用秀丽隐杆线虫的进入持久幼虫阶段,形成以应对苛刻的环境条件下发育逮捕阶段,作为一个模型来研究与增长转型静止相关联的全球代谢变化和潜在的分子机制。结果在这里,我们表明,代谢开关涉及到几个调控途径的共同行为。而类固醇激素受体DAF-12控制持久形态发生,所述胰岛素通路通过DAF-16 /的FoxO,这也需要AAK-2 /AMPKα保持低能量消耗。 DAF-12和AAK-2分别促进中心碳代谢途径从TCA循环转向个碳原子和它们引导到糖异生中的两个关键的分支点在竞争的酶之间的摩尔比的换档。当两个AAK-2和DAF-12被抑制,TCA循环中是活动的和发育停滞被旁路。结论每个发育阶段的代谢状态由化学计量比的代谢酶驱动代谢通量和控制生长和静止之间的过渡的星座中定义的。

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