H₂S-mediated blockage of protein acetylation and oxidative stress attenuates lipid overload-induced cardiac senescence.

IF 2.5 4区医学 Q3 ENDOCRINOLOGY & METABOLISM

Archives of Physiology and Biochemistry Pub Date : 2024-02-01 Epub Date: 2021-09-11 DOI:10.1080/13813455.2021.1976209

Ruihuan Yu, Yuehong Wang, Jiechun Zhu, Guangdong Yang

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引用次数: 0

Abstract

Hydrogen sulphide (H₂S), a newly identified gasotransmitter, can be endogenously produced by cystathionine gamma-lyase (CSE) in the cardiovascular system. This study investigated the role of the CSE/H₂S system on lipid overload-induced lipotoxicity and cardiac senescence. Lipid overload in rat cardiomyocyte cells (H9C2) promoted intracellular accumulation of lipid, oxidative stress, mitochondrial dysfunctions, lipid peroxidation and inhibited cell viability, all of which could be reversed by exogenously applied H₂S. Further data revealed that H₂S protected H9C2 cells from lipid overload-induced senescence by altering the expressions of lipid metabolism-related genes and inhibiting cellular acetyl-CoA and global protein acetylation. Enhancement of protein acetylation abolished the protective role of H₂S on cardiac senescence. In vivo, knockout of the CSE gene strengthened cardiac lipid accumulation, protein acetylation, and cellular ageing in high fat diet-fed mice. Taken together, the CSE/H₂S system is capable of maintaining lipid homeostasis and cellular senescence in heart cells under lipid overload.

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H2S 介导的蛋白质乙酰化和氧化应激阻断可减轻脂质超载诱导的心脏衰老。

硫化氢（H2S）是一种新发现的气体递质，可由心血管系统中的胱硫醚γ-裂解酶（CSE）内源性产生。本研究探讨了 CSE/H2S 系统对脂质超载诱导的脂毒性和心脏衰老的作用。在大鼠心肌细胞（H9C2）中，脂质超载会促进细胞内脂质积累、氧化应激、线粒体功能障碍、脂质过氧化和抑制细胞活力，而外源施加的 H2S 可逆转所有这些现象。进一步的数据显示，H2S 通过改变脂质代谢相关基因的表达，抑制细胞乙酰-CoA 和全局蛋白质乙酰化，保护 H9C2 细胞免受脂质过载诱导的衰老。蛋白质乙酰化的增强消除了 H2S 对心脏衰老的保护作用。在体内，敲除 CSE 基因会加强高脂饮食喂养小鼠的心脏脂质积累、蛋白质乙酰化和细胞衰老。综上所述，CSE/H2S 系统能够在脂质超载的情况下维持心脏细胞的脂质平衡和细胞衰老。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Archives of Physiology and Biochemistry ENDOCRINOLOGY & METABOLISM-PHYSIOLOGY

CiteScore

6.90

自引率

3.30%

发文量

期刊介绍： Archives of Physiology and Biochemistry: The Journal of Metabolic Diseases is an international peer-reviewed journal which has been relaunched to meet the increasing demand for integrated publication on molecular, biochemical and cellular aspects of metabolic diseases, as well as clinical and therapeutic strategies for their treatment. It publishes full-length original articles, rapid papers, reviews and mini-reviews on selected topics. It is the overall goal of the journal to disseminate novel approaches to an improved understanding of major metabolic disorders. The scope encompasses all topics related to the molecular and cellular pathophysiology of metabolic diseases like obesity, type 2 diabetes and the metabolic syndrome, and their associated complications. Clinical studies are considered as an integral part of the Journal and should be related to one of the following topics: -Dysregulation of hormone receptors and signal transduction -Contribution of gene variants and gene regulatory processes -Impairment of intermediary metabolism at the cellular level -Secretion and metabolism of peptides and other factors that mediate cellular crosstalk -Therapeutic strategies for managing metabolic diseases Special issues dedicated to topics in the field will be published regularly.