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FOXO3:人类长寿的主要基因——一篇综述短文

FOXO3: A Major Gene for Human Longevity--A Mini-Review.

作者信息

Morris Brian J, Willcox Donald Craig, Donlon Timothy A, Willcox Bradley J

机构信息

Department of Geriatric Medicine, John A. Burns School of Medicine, University of Hawaii, Honolulu, Hawaii, USA.

出版信息

Gerontology. 2015;61(6):515-25. doi: 10.1159/000375235. Epub 2015 Mar 28.

Abstract

BACKGROUND

The gene FOXO3, encoding the transcription factor forkhead box O-3 (FoxO3), is one of only two for which genetic polymorphisms have exhibited consistent associations with longevity in diverse human populations.

OBJECTIVE

Here, we review the multitude of actions of FoxO3 that are relevant to health, and thus healthy ageing and longevity.

METHODS

The study involved a literature search for articles retrieved from PubMed using FoxO3 as keyword.

RESULTS

We review the molecular genetics of FOXO3 in longevity, then current knowledge of FoxO3 function relevant to ageing and lifespan. We describe how FoxOs are involved in energy metabolism, oxidative stress, proteostasis, apoptosis, cell cycle regulation, metabolic processes, immunity, inflammation and stem cell maintenance. The single FoxO in Hydra confers immortality to this fresh water polyp, but as more complex organisms evolved, this role has been usurped by the need for FoxO to control a broader range of specialized pathways across a wide spectrum of tissues assisted by the advent of as many as 4 FoxO subtypes in mammals. The major themes of FoxO3 are similar, but not identical, to other FoxOs and include regulation of cellular homeostasis, particularly of stem cells, and of inflammation, which is a common theme of age-related diseases. Other functions concern metabolism, cell cycle arrest, apoptosis, destruction of potentially damaging reactive oxygen species and proteostasis.

CONCLUSIONS

The mechanism by which longevity-associated alleles of FOXO3 reduce age-related mortality is currently of great clinical interest. The prospect of optimizing FoxO3 activity in humans to increase lifespan and reduce age-related diseases represents an exciting avenue of clinical investigation. Research strategies directed at developing therapeutic agents that target FoxO3, its gene and proteins in the pathway(s) FoxO3 regulates should be encouraged and supported.

摘要

背景

基因FOXO3编码转录因子叉头框O-3(FoxO3),它是在不同人群中,其基因多态性与长寿呈现出一致关联的仅有的两个基因之一。

目的

在此,我们综述了与健康相关的FoxO3的多种作用,以及与健康衰老和长寿相关的作用。

方法

该研究涉及使用FoxO3作为关键词在PubMed上检索文章的文献搜索。

结果

我们综述了FOXO3在长寿方面的分子遗传学,以及目前有关FoxO3与衰老和寿命相关功能的知识。我们描述了FoxO如何参与能量代谢、氧化应激、蛋白质稳态、细胞凋亡、细胞周期调控、代谢过程、免疫、炎症和干细胞维持。水螅中的单个FoxO赋予这种淡水水螅永生能力,但随着更复杂的生物体进化,由于哺乳动物中多达4种FoxO亚型的出现,FoxO需要控制更广泛的组织中的多种专门途径,这一角色被取代。FoxO3的主要主题与其他FoxO相似但不完全相同,包括细胞内稳态的调节,特别是干细胞的内稳态调节,以及炎症调节,炎症是与年龄相关疾病的一个共同主题。其他功能涉及代谢、细胞周期停滞、细胞凋亡、破坏潜在有害的活性氧和蛋白质稳态。

结论

FOXO3与长寿相关的等位基因降低与年龄相关死亡率的机制目前具有重大临床意义。在人类中优化FoxO3活性以延长寿命并减少与年龄相关疾病的前景代表了一个令人兴奋的临床研究途径。应鼓励和支持旨在开发靶向FoxO3及其在FoxO3调节途径中的基因和蛋白质的治疗药物的研究策略。

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