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胰岛素对衰老果蝇心脏功能的调节作用。

Insulin regulation of heart function in aging fruit flies.

作者信息

Wessells Robert J, Fitzgerald Erin, Cypser James R, Tatar Marc, Bodmer Rolf

机构信息

The Burnham Institute, Center for Neuroscience and Aging, 10901 Torrey Pines Road, La Jolla, California 92037, USA.

出版信息

Nat Genet. 2004 Dec;36(12):1275-81. doi: 10.1038/ng1476. Epub 2004 Nov 21.

Abstract

Insulin-IGF receptor (InR) signaling has a conserved role in regulating lifespan, but little is known about the genetic control of declining organ function. Here, we describe progressive changes of heart function in aging fruit flies: from one to seven weeks of a fly's age, the resting heart rate decreases and the rate of stress-induced heart failure increases. These age-related changes are minimized or absent in long-lived flies when systemic levels of insulin-like peptides are reduced and by mutations of the only receptor, InR, or its substrate, chico. Moreover, interfering with InR signaling exclusively in the heart, by overexpressing the phosphatase dPTEN or the forkhead transcription factor dFOXO, prevents the decline in cardiac performance with age. Thus, insulin-IGF signaling influences age-dependent organ physiology and senescence directly and autonomously, in addition to its systemic effect on lifespan. The aging fly heart is a model for studying the genetics of age-sensitive organ-specific pathology.

摘要

胰岛素-胰岛素样生长因子受体(InR)信号传导在调节寿命方面具有保守作用,但对于器官功能衰退的基因控制却知之甚少。在此,我们描述了衰老果蝇心脏功能的渐进性变化:从果蝇1周龄到7周龄,静息心率下降,应激诱导的心力衰竭发生率增加。当胰岛素样肽的全身水平降低以及唯一受体InR或其底物chico发生突变时,这些与年龄相关的变化在长寿果蝇中最小化或不存在。此外,通过过度表达磷酸酶dPTEN或叉头转录因子dFOXO专门干扰心脏中的InR信号传导,可防止心脏功能随年龄下降。因此,胰岛素-IGF信号传导除了对寿命具有全身性影响外,还直接且自主地影响年龄依赖性器官生理学和衰老。衰老果蝇的心脏是研究年龄敏感型器官特异性病理学遗传学的模型。

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