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类固醇激素信号对秀丽隐杆线虫胰岛素样信号控制寿命的影响。

Influence of steroid hormone signaling on life span control by Caenorhabditis elegans insulin-like signaling.

机构信息

Graduate Program in Cellular and Molecular Biology, University of Michigan, Ann Arbor, Michigan 48109, USA.

出版信息

G3 (Bethesda). 2013 May 20;3(5):841-50. doi: 10.1534/g3.112.005116.

DOI:10.1534/g3.112.005116
PMID:23550118
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3656731/
Abstract

Sterol-sensing nuclear receptors and insulin-like growth factor signaling play evolutionarily conserved roles in the control of aging. In the nematode Caenorhabditis elegans, bile acid-like steroid hormones known as dafachronic acids (DAs) influence longevity by binding to and regulating the activity of the conserved nuclear receptor DAF-12, and the insulin receptor (InsR) ortholog DAF-2 controls life span by inhibiting the FoxO transcription factor DAF-16. How the DA/DAF-12 pathway interacts with DAF-2/InsR signaling to control life span is poorly understood. Here we specifically investigated the roles of liganded and unliganded DAF-12 in life span control in the context of reduced DAF-2/InsR signaling. In animals with reduced daf-2/InsR activity, mutations that either reduce DA biosynthesis or fully abrogate DAF-12 activity shorten life span, suggesting that liganded DAF-12 promotes longevity. In animals with reduced DAF-2/InsR activity induced by daf-2/InsR RNAi, both liganded and unliganded DAF-12 promote longevity. However, in daf-2/InsR mutants, liganded and unliganded DAF-12 act in opposition to control life span. Thus, multiple DAF-12 activities influence life span in distinct ways in contexts of reduced DAF-2/InsR signaling. Our findings establish new roles for a conserved steroid signaling pathway in life span control and elucidate interactions among DA biosynthetic pathways, DAF-12, and DAF-2/InsR signaling in aging.

摘要

固醇感应核受体和胰岛素样生长因子信号在衰老控制中发挥着进化保守的作用。在秀丽隐杆线虫中,被称为达法克罗酸(DA)的胆酸样甾体激素通过与保守核受体 DAF-12 结合并调节其活性,影响寿命,而胰岛素受体(InsR)同源物 DAF-2 通过抑制 FoxO 转录因子 DAF-16 来控制寿命。DA/DAF-12 途径如何与 DAF-2/InsR 信号相互作用以控制寿命尚不清楚。在这里,我们专门研究了配体结合和非配体结合的 DAF-12 在降低 DAF-2/InsR 信号的情况下控制寿命的作用。在降低 daf-2/InsR 活性的动物中,降低 DA 生物合成或完全消除 DAF-12 活性的突变会缩短寿命,这表明配体结合的 DAF-12 促进长寿。在由 daf-2/InsR RNAi 诱导的降低 DAF-2/InsR 活性的动物中,配体结合和非配体结合的 DAF-12 都促进了寿命的延长。然而,在 daf-2/InsR 突变体中,配体结合和非配体结合的 DAF-12 以相反的方式控制寿命。因此,在降低 DAF-2/InsR 信号的情况下,多种 DAF-12 活性以不同的方式影响寿命。我们的发现确立了保守的类固醇信号通路在寿命控制中的新作用,并阐明了 DA 生物合成途径、DAF-12 和 DAF-2/InsR 信号之间在衰老过程中的相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed5e/3656731/600ea6443d49/841f3.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed5e/3656731/600ea6443d49/841f3.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed5e/3656731/600ea6443d49/841f3.jpg

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