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Comparative transcriptional profiling identifies takeout as a gene that regulates life span

机译:比较转录谱分析表明外卖是一个基因 调节寿命

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摘要

A major challenge in translating the positive effects of dietary restriction (DR) for the improvement of human health is the development of therapeutic mimics. One approach to finding DR mimics is based upon identification of the proximal effectors of DR life span extension. Whole genome profiling of DR in Drosophila shows a large number of changes in gene expression, making it difficult to establish which changes are involved in life span determination as opposed to other unrelated physiological changes. We used comparative whole genome expression profiling to discover genes whose change in expression is shared between DR and two molecular genetic life span extending interventions related to DR, increased dSir2 and decreased Dmp53 activity. We find twenty-one genes shared among the three related life span extending interventions. One of these genes, takeout, thought to be involved in circadian rhythms, feeding behavior and juvenile hormone binding is also increased in four other life span extending conditions: Rpd3, Indy, chico and methuselah. We demonstrate takeout is involved in longevity determination by specifically increasing adult takeout expression and extending life span. These studies demonstrate the power of comparative whole genome transcriptional profiling for identifying specific downstream elements of the DR life span extending pathway.
机译:转化饮食限制(DR)对改善人类健康的积极作用的主要挑战是治疗模拟物的发展。查找DR拟态的一种方法是基于DR寿命延长的近端效应器的识别。果蝇中DR的全基因组图谱显示了基因表达的大量变化,与其他不相关的生理变化相比,很难确定哪些变化涉及寿命确定。我们使用比较的全基因组表达谱来发现基因,其表达变化在DR和两个与DR相关的分子遗传学寿命延长干预措施,增加dSir2和降低Dmp53活性之间共享。我们发现在延长寿命的三个相关寿命之间共有二十一个基因。这些基因之一,外卖,被认为与昼夜节律,进食行为和幼年激素结合有关,在其他四个寿命延长条件下也增加了:Rpd3,Indy,chico和methuselah。我们证明外卖通过具体增加成年外卖的表达量和延长寿命来参与长寿的确定。这些研究证明了比较性全基因组转录谱分析对鉴定特定基因的能力 DR寿命延长途径的下游元素。

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