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Metabolic changes associated with the long winter fast dominate the liver proteome in 13-lined ground squirrels

机译:与漫长的冬季相关的代谢变化快速控制着13排地松鼠的肝脏蛋白质组

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摘要

Small-bodied hibernators partition the year between active homeothermy and hibernating heterothermy accompanied by fasting. To define molecular events underlying hibernation that are both dependent and independent of fasting, we analyzed the liver proteome among two active and four hibernation states in 13-lined ground squirrels. We also examined fall animals transitioning between fed homeothermy and fasting heterothermy. Significantly enriched pathways differing between activity and hibernation were biased toward metabolic enzymes, concordant with the fuel shifts accompanying fasting physiology. Although metabolic reprogramming to support fasting dominated these data, arousing (rewarming) animals had the most distinct proteome among the hibernation states. Instead of a dominant metabolic enzyme signature, torpor-arousal cycles featured differences in plasma proteins and intracellular membrane traffic and its regulation. Phosphorylated NSFL1C, a membrane regulator, exhibited this torpor-arousal cycle pattern; its role in autophagosome formation may promote utilization of local substrates upon metabolic reactivation in arousal. Fall animals transitioning to hibernation lagged in their proteomic adjustment, indicating that the liver is more responsive than preparatory to the metabolic reprogramming of hibernation. Specifically, torpor use had little impact on the fall liver proteome, consistent with a dominant role of nutritional status. In contrast to our prediction of reprogramming the transition between activity and hibernation by gene expression and then within-hibernation transitions by posttranslational modification (PTM), we found extremely limited evidence of reversible PTMs within torpor-arousal cycles. Rather, acetylation contributed to seasonal differences, being highest in winter (specifically in torpor), consistent with fasting physiology and decreased abundance of the mitochondrial deacetylase, SIRT3.
机译:小体型冬眠者在活跃的同温和休眠的异性间伴有禁食之间划分年份。为了定义冬眠既依赖于又不依赖于禁食的分子事件,我们分析了在13个内衬的松鼠中处于两个活跃和四个冬眠状态的肝脏蛋白质组。我们还检查了秋季动物在摄食同温和禁食异温之间的转换。活动和冬眠之间差异显着的丰富途径偏向于代谢酶,这与禁食生理伴随的燃料转移是一致的。尽管支持空腹的代谢重编程在这些数据中占主导地位,但在冬眠状态下,唤醒(重新武装)动物的蛋白质组最为不同。代替显性代谢酶的特征,环状循环引起血浆蛋白和细胞内膜运输及其调节的差异。磷酸化的NSFL1C(一种膜调节剂)表现出这种环-铁环循环模式。其在自噬小体形成中的作用可能会在唤醒中通过代谢激活来促进局部底物的利用。秋季过渡到冬眠的动物的蛋白质组调整滞后,表明肝脏比冬眠的代谢重编程更具反应性。具体来说,使用玉米粥对秋季肝脏蛋白质组几乎没有影响,这与营养状况的主要作用相一致。与我们通过基因表达重新编程活动和休眠之间的转换以及然后通过翻译后修饰(PTM)重新进入休眠状态的转换的预测相反,我们发现在圆孔循环内可逆PTM的证据非常有限。而是,乙酰化导致季节差异,在冬季最高(特别是在玉米粥中),这与空腹生理和线粒体脱乙酰基酶SIRT3的丰度降低相一致。

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