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Reconsidering movement of eukaryotic mRNAs between polysomes and P bodies.

机译:重新考虑多核糖体与P体之间的真核mRNA的运动。

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摘要

Cell survival in changing environments requires appropriate regulation of gene expression, including posttranscriptional regulatory mechanisms. From reporter gene studies in glucose-starved yeast, it was proposed that translationally silenced eukaryotic mRNAs accumulate in P bodies and can return to active translation. We present evidence contradicting the notion that reversible storage of nontranslating mRNAs is a widespread and general phenomenon. First, genome-wide measurements of mRNA abundance, translation, and ribosome occupancy after glucose withdrawal show that most mRNAs are depleted from the cell coincident with their depletion from polysomes. Second, only a limited subpopulation of translationally repressed transcripts, comprising fewer than 400 genes, can be reactivated for translation upon glucose readdition in the absence of new transcription. This highly selective posttranscriptional regulation could be a mechanism for cells to minimize the energetic costs of reversing gene-regulatory decisions in rapidly changing environments by transiently preserving a pool of transcripts whose translation is rate-limiting for growth.
机译:在不断变化的环境中的细胞存活需要适当调节基因表达,包括转录后调控机制。根据在葡萄糖饥饿的酵母中进行的报告基因研究,有人提出翻译沉默的真核mRNA在P体中积累,并可以恢复为主动翻译。我们目前的证据与非翻译mRNA的可逆存储是一种普遍存在的普遍现象相矛盾。首先,葡萄糖撤除后,全基因组范围内的mRNA丰度,翻译和核糖体占有率的测量结果表明,大多数mRNA从细胞中被消耗掉,同时它们从多核糖体中被消耗掉。第二,只有少于400个基因的翻译抑制的转录子的有限亚群可以在没有新转录的情况下在葡萄糖重新分配后被重新激活进行翻译。这种高度选择性的转录后调控可能是细胞通过暂时保留转录水平受其生长速率限制的转录本来在快速变化的环境中最小化逆转基因调控决定的能量消耗的机制。

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