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核激素受体DAF-12对秀丽隐杆线虫的寿命具有相反的作用,并调控在多种长寿蠕虫中被抑制的基因。

The nuclear hormone receptor DAF-12 has opposing effects on Caenorhabditis elegans lifespan and regulates genes repressed in multiple long-lived worms.

作者信息

Fisher Alfred L, Lithgow Gordon J

机构信息

Division of Geriatrics, Department of Medicine, University of California, San Francisco, 94121, USA.

出版信息

Aging Cell. 2006 Apr;5(2):127-38. doi: 10.1111/j.1474-9726.2006.00203.x.

Abstract

The orphan nuclear hormone receptor gene daf-12 in Caenorhabditis elegans plays a key role in the regulation of development and determination of adult longevity. To understand the effects of daf-12 on aging we characterized the lifespan of loss-of-function and gain-of-function daf-12 alleles that have been identified on the basis of their effects on dauer development. We find that these mutations have opposing effects on longevity and resistance to oxidative and thermal stress which makes daf-12 the first gene with alleles that can extend or shorten lifespan. We find that the shortened lifespan of the loss-of-function mutation is due to accelerated aging in young adulthood rather than an adverse effect of the mutation on development. Microarray analysis of worms carrying the two alleles revealed a relatively small number of genes differentially expressed between the two genotypes. Comparison of the expression profiles with the profiles associated with dauer formation and long-lived daf-2 mutants revealed that while the profiles are largely different, there is significant overlap among the genes down-regulated, but not up-regulated, in all profiles. Several of these genes down-regulated in multiple long-lived worms have known effects on lifespan, and many of the genes belong to a family of poorly characterized genes that are strongly down-regulated in dauers, daf-2 mutants, and long-lived daf-12 mutants. Our results point to daf-12 modulating aging and stress responses in part through the repression of specific genes, and emphasize the role that the repression of genes that curtail maximal lifespan plays in lifespan determination.

摘要

秀丽隐杆线虫中的孤儿核激素受体基因daf-12在发育调控和成虫寿命决定中起关键作用。为了解daf-12对衰老的影响,我们对功能丧失型和功能获得型daf-12等位基因的寿命进行了表征,这些等位基因是根据它们对滞育发育的影响而确定的。我们发现这些突变对寿命以及对氧化应激和热应激的抗性具有相反的影响,这使得daf-12成为第一个具有能延长或缩短寿命等位基因的基因。我们发现功能丧失型突变导致的寿命缩短是由于成年早期衰老加速,而不是该突变对发育产生的不利影响。对携带这两种等位基因的线虫进行微阵列分析发现,两种基因型之间差异表达的基因数量相对较少。将表达谱与滞育形成和长寿daf-2突变体相关的谱进行比较,结果显示虽然这些谱在很大程度上不同,但在所有谱中下调而非上调的基因之间存在显著重叠。在多个长寿线虫中下调的这些基因中有几个对寿命有已知影响,并且许多基因属于一类特征 poorly characterized genes,在滞育线虫、daf-2突变体和长寿daf-12突变体中强烈下调。我们的结果表明,daf-12部分通过抑制特定基因来调节衰老和应激反应,并强调了抑制缩短最大寿命的基因在寿命决定中所起的作用。 (注:“poorly characterized genes”直译为“特征 poorly characterized genes”,可能原英文表述有误,可根据实际情况修正)

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