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SIR2 and other genes are abundantly expressed in long-lived natural segregants for replicative aging of the budding yeast Saccharomyces cerevisiae

机译:SIR2和其他基因在长寿命的天然分离子中大量表达,用于芽生酵母酿酒酵母的复制性衰老

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摘要

We investigated the mechanism underlying the natural variation in longevity within natural populations using the model budding yeast, Saccharomyces cerevisiae. We analyzed whole-genome gene expression in four progeny of a natural S. cerevisiae strain that display differential replicative aging. Genes with different expression levels in short- and long-lived strains were classified disproportionately into metabolism, transport, development, transcription or cell cycle, and organelle organization (mitochondrial, chromosomal, and cytoskeletal). With several independent validating experiments, we detected 15 genes with consistent differential expression levels between the long- and the short-lived progeny. Among those 15, SIR2, HSP30, and TIM17 were upregulated in long-lived strains, which is consistent with the known effects of gene silencing, stress response, and mitochondrial function on aging. The link between SIR2 and yeast natural life span variation offers some intriguing ties to the allelic association of the human homolog SIRT1 to visceral obesity and metabolic response to lifestyle intervention.
机译:我们使用模型发芽的酵母酿酒酵母调查了自然种群中寿命长寿的自然变化的基本机制。我们分析了天然酿酒酵母菌株的四个子代中的全基因组基因表达,这些菌株显示差异复制性衰老。在短寿命和长寿命菌株中具有不同表达水平的基因不成比例地分类为代谢,转运,发育,转录或细胞周期以及细胞器组织(线粒体,染色体和细胞骨架)。通过几个独立的验证实验,我们检测到了15个基因,它们在长寿和短寿后代之间具有一致的差异表达水平。在这15个中,SIR2,HSP30和TIM17在长寿命菌株中被上调,这与基因沉默,应激反应和线粒体功能对衰老的已知作用一致。 SIR2和酵母自然寿命变化之间的联系为人类同源物SIRT1与内脏肥胖和生活方式干预的代谢反应等位基因关联提供了一些有趣的联系。

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