Proteomics reveals crosstalk between calcium disturbance and multiple stresses facilitating lethal ventricular arrhythmias-sudden cardiac death under the co-morbidity of acute myocardial ischemia and type II diabetes mellitus

IF 5.1 2区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

Life sciences Pub Date : 2025-07-02 DOI:10.1016/j.lfs.2025.123826

Ye Zhang , Xiaojun Zhang , Huishan Liang , Haiyan Li , Wei Zhang , Mengxuan Zhang , Danya Zhou , Mengting Zhu , Xudong Xiao , Junyao Lv , Guanghui Zhu , Xiaojun Yu , Minchao Lai , Dian Wang

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引用次数: 0

Abstract

Aims

Diabetes mellitus (DM) often co-exists with myocardial ischemia (MI). Whether DM increases sudden cardiac death (SCD) susceptibility in early MI remains unclear, and the underlying mechanism needs to be further explored.

Materials and methods

We induced type II DM in mice to produce a co-morbidity model of DM and MI. Proteomic analysis was conducted to identify proteomic features associated with DM-SCD and MI. Additionally, a neonatal rat ventricular myocyte (NRVM) model was established under conditions of hypoxia and high glucose (HG) to elucidate the interplay between oxidative stress and endoplasmic reticulum (ER) stress in MI co-morbid with DM.

Key findings

Our findings revealed that DM increased the incidence of lethal ventricular arrhythmia (LVA)-SCD in early MI. Proteomic data indicate that Ca²⁺-mediated oxidative stress and ER stress may synergistically contribute to the increased SCD incidence. SCD mice exhibited increased mitochondrial ROS (mROS) and cytosolic ROS (cytoROS), decreased mitochondrial membrane potential (MMP) and reduced/oxidized glutathione ratio, upregulation of RyR2-S2814 phosphorylation, and increased expression of ER stress-related proteins in the ischemic myocardium. NRVMs subjected to hypoxia and HG showed cytosolic and mitochondrial Ca²⁺ overload, excessive ROS production, and reduced intracellular K⁺ levels. Treatment with MitoTEMPO to scavenge mROS and 4-PBA to inhibit ER stress normalized SCD-associated alterations in mice and hypoxia- and HG-associated alterations in NRVMs, preventing LVA-SCD.

Significance

Our study uncovers that DM increases the incidence of LVA-SCD in early MI, which is associated with the crosstalk between calcium dysregulation and multiple stresses.

Abstract Image

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蛋白质组学揭示了钙干扰与多重应激之间的串扰，促进了急性心肌缺血和II型糖尿病合并症下致死性室性心律失常-心源性猝死

目的糖尿病（DM）常与心肌缺血（MI）共存。糖尿病是否会增加心肌梗死早期心源性猝死（SCD）易感性尚不清楚，其潜在机制有待进一步探讨。材料和方法我们在小鼠中诱导II型糖尿病，建立糖尿病和心肌梗死共发病模型，并进行蛋白质组学分析，以确定与DM- scd和心肌梗死相关的蛋白质组学特征。在缺氧和高糖（HG）条件下，建立了新生大鼠心室肌细胞（NRVM）模型，以阐明氧化应激和内质网（ER）应激在心肌梗死合并DM时的相互作用。研究结果表明，DM增加了心肌梗死早期致死性室性心律失常(LVA)-SCD的发生率。蛋白质组学数据表明，Ca2+介导的氧化应激和内质网应激可能协同促进SCD发生率的增加。SCD小鼠表现为线粒体ROS （mROS）和细胞质ROS （cytoROS）升高，线粒体膜电位（MMP）降低，谷胱甘肽/氧化谷胱甘肽比值降低，RyR2-S2814磷酸化上调，缺血心肌内质网应激相关蛋白表达增加。缺氧和汞胁迫下的nrvm表现为胞质和线粒体Ca2+超载，ROS产生过多，细胞内K+水平降低。用MitoTEMPO清除mROS和4-PBA抑制小鼠内质网应激正常化scd相关改变和nrvm缺氧和hg相关改变，预防LVA-SCD。我们的研究发现，糖尿病增加了心肌梗死早期LVA-SCD的发生率，这与钙失调和多重应激之间的串扰有关。

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

Life sciences 医学-药学

CiteScore

12.20

自引率

1.60%

发文量

841

审稿时长

6 months

期刊介绍： Life Sciences is an international journal publishing articles that emphasize the molecular, cellular, and functional basis of therapy. The journal emphasizes the understanding of mechanism that is relevant to all aspects of human disease and translation to patients. All articles are rigorously reviewed. The Journal favors publication of full-length papers where modern scientific technologies are used to explain molecular, cellular and physiological mechanisms. Articles that merely report observations are rarely accepted. Recommendations from the Declaration of Helsinki or NIH guidelines for care and use of laboratory animals must be adhered to. Articles should be written at a level accessible to readers who are non-specialists in the topic of the article themselves, but who are interested in the research. The Journal welcomes reviews on topics of wide interest to investigators in the life sciences. We particularly encourage submission of brief, focused reviews containing high-quality artwork and require the use of mechanistic summary diagrams.