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网络分析揭示了从真菌到动物进化上保守的与衰老相关的途径。

Network analyses unveil ageing-associated pathways evolutionarily conserved from fungi to animals.

机构信息

Institut de Systématique, Evolution, Biodiversité (ISYEB), Sorbonne Université, CNRS, Museum National d'Histoire Naturelle, EPHE, Université Des Antilles, Paris, France.

Département de Sciences Biologiques, Complexe Des Sciences, Université de Montréal, Montréal, QC, Canada.

出版信息

Geroscience. 2023 Apr;45(2):1059-1080. doi: 10.1007/s11357-022-00704-2. Epub 2022 Dec 12.

Abstract

The genetic roots of the diverse paces and shapes of ageing and of the large variations in longevity observed across the tree of life are poorly understood. Indeed, pathways associated with ageing/longevity are incompletely known, both in terms of their constitutive genes/proteins and of their molecular interactions. Moreover, there is limited overlap between the genes constituting these pathways across mammals. Yet, dedicated comparative analyses might still unravel evolutionarily conserved, important pathways associated with longevity or ageing. Here, we used an original strategy with a double evolutionary and systemic focus to analyse protein interactions associated with ageing or longevity during the evolution of five species of Opisthokonta. We ranked these proteins and interactions based on their evolutionary conservation and centrality in past and present protein-protein interaction (PPI) networks, providing a big systemic picture of the evolution of ageing and longevity pathways that identified which pathways emerged in which Opisthokonta lineages, were conserved, and/or central. We confirmed that longevity/ageing-associated proteins (LAPs), be they pro- or anti-longevity, are highly central in extant PPI, consistently with the antagonistic pleiotropy theory of ageing, and identified key antagonistic regulators of ageing/longevity, 52 of which with homologues in humans. While some highly central LAPs were evolutionarily conserved for over a billion years, we report a clear transition in the functionally important components of ageing/longevity within bilaterians. We also predicted 487 novel evolutionarily conserved LAPs in humans, 54% of which are more central than mTOR, and 138 of which are druggable, defining new potential targets for anti-ageing treatments in humans.

摘要

遗传因素是导致衰老速度和模式以及生物多样性寿命存在巨大差异的主要原因,但目前对此知之甚少。事实上,与衰老/长寿相关的途径在其组成基因/蛋白质及其分子相互作用方面都知之甚少。此外,构成这些途径的基因在哺乳动物之间的重叠非常有限。然而,专门的比较分析可能仍然可以揭示与长寿或衰老相关的进化保守的重要途径。在这里,我们使用了一种原始的策略,具有双重进化和系统焦点,来分析五个后生动物物种进化过程中与衰老或长寿相关的蛋白质相互作用。我们根据它们的进化保守性以及在过去和现在的蛋白质-蛋白质相互作用(PPI)网络中的中心性对这些蛋白质和相互作用进行了排名,提供了一个与衰老和长寿途径进化相关的大型系统图,确定了哪些途径出现在哪些后生动物谱系中,哪些途径是保守的,哪些途径是中心的。我们证实,长寿/衰老相关蛋白(LAPs),无论是促进长寿还是抗长寿,在现存的 PPI 中都具有高度的中心性,这与衰老的拮抗多效性理论一致,并确定了衰老/长寿的关键拮抗调节剂,其中 52 个在人类中有同源物。虽然一些高度中心的 LAPs 已经进化保守了超过 10 亿年,但我们报告了在两侧对称动物中,衰老/长寿的功能重要组成部分发生了明显的转变。我们还预测了人类 487 个新的进化保守 LAPs,其中 54%的 LAPs比 mTOR 更中心,其中 138 个是可药用的,为人类抗衰老治疗定义了新的潜在靶点。

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