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首页> 外文期刊>Philosophical Transactions of the Royal Society of London, Series B. Biological Sciences >Spatial protein quality control and the evolution of lineage-specific ageing
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Spatial protein quality control and the evolution of lineage-specific ageing

机译:空间蛋白质质量控​​制和特定谱系衰老的演变

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摘要

Propagation of a species requires periodic cell renewal to avoid clonal extinction. Sexual reproduction and the separation of germ cells from the soma provide a mechanism for such renewal, but are accompanied by an apparently mandatory ageing of the soma. Data obtained during the last decade suggest that a division of labour exists also between cells of vegetatively reproducing unicellular organisms, leading to the establishment of a soma-like and germ-like lineage with distinct fitness and longevity characteristics. This division of labour in both bacteria and yeast entails segregation of damaged and aggregated proteins such that the germ-like lineage is kept free of damage to the detriment of the soma-like lineage. In yeast, this spatial protein quality control (SQC) encompasses a CCT-chaperonin-dependent translocation and merging of cytotoxic protein aggregates. This process is regulated by Sir2, a protein deacetylase that modulates the rate of ageing in organisms ranging from yeast to worms and flies. Recent data also demonstrate that SQC is intimately integrated with the machinery establishing proper cell polarity and that this machinery is required for generating a soma-like and germ-like lineage in yeast. Deciphering the details of the SQC network may increase our understanding of the development of age-related protein folding disorders and shed light on the selective forces that paved the way for polarity and lineage-specific ageing to evolve.
机译:一个物种的繁殖需要定期更新细胞以避免克隆灭绝。有性生殖和生殖细胞与躯体的分离为这种更新提供了一种机制,但伴随着躯体的明显强制衰老。在过去十年中获得的数据表明,在营养繁殖的单细胞生物的细胞之间也存在分工,导致建立了具有明显适应性和寿命特征的类索马氏和类细菌谱系。细菌和酵母菌的这种分工需要将受损的蛋白质和聚集的蛋白质隔离开,从而使细菌样谱系不受损害,不会损害索马样谱系。在酵母中,这种空间蛋白质量控制(SQC)包括CCT-伴侣蛋白依赖的易位和细胞毒性蛋白聚集体的合并。该过程由Sir2调节,Sir2是一种蛋白质脱乙酰基酶,可调节从酵母到蠕虫和果蝇等生物体的衰老速率。最近的数据还表明,SQC与建立正确细胞极性的机制紧密集成,并且该机制对于在酵母中产生类似体细胞和类似细菌的谱系是必需的。解读SQC网络的细节可能会增加我们对与年龄有关的蛋白质折叠障碍的发展的了解,并阐明为极性和谱系特异性老化发展铺平道路的选择力。

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