VPO1通过上调CYLD促进慢性心力衰竭大鼠心肌细胞的程序性坏死。
VPO1 Promotes Programmed Necrosis of Cardiomyocytes in Rats with Chronic Heart Failure by Upregulating CYLD.
作者信息
Zhang Yinzhuang, Shen Zhijie, Mao Zhuoni, Huang Dan, Lou Chengyu, Fang Li
机构信息
Department of Cardiovascular Medicine, The Affiliated Changsha Hospital of Xiangya School of Medicine, Central South University, 410008 Changsha, Hunan, China.
出版信息
Front Biosci (Landmark Ed). 2024 Dec 24;29(12):425. doi: 10.31083/j.fbl2912425.
BACKGROUND
Chronic heart failure (CHF) is a serious cardiovascular condition. Vascular peroxidase 1 (VPO1) is associated with various cardiovascular diseases, yet its role in CHF remains unclear. This research aims to explore the involvement of VPO1 in CHF.
METHODS
CHF was induced in rats using adriamycin, and the expression levels of VPO1 and cylindromatosis (CYLD) were assessed. In parallel, the effects of VPO1 on programmed necrosis in H9c2 cells were evaluated through cell viability assays, lactate dehydrogenase (LDH) level measurements, and analysis of receptor-interacting protein kinase 1/receptor-interacting protein kinase 3/mixed lineage kinase domain-like protein (RIPK1/RIPK3/MLKL) pathway-related proteins. The impact of CYLD on RIPK1 protein stability and ubiquitination was also investigated, along with the interaction between VPO1 and CYLD. Additionally, cardiac structure and function were assessed using echocardiography, Hematoxylin-eosin (HE) staining, Masson staining, and measurements of myocardial injury-related factors, including N-terminal prohormone of brain natriuretic peptide (NT-proBNP), Aspartate aminotransferase (AST), LDH, and creatine kinase-myocardial band (CK-MB).
RESULTS
VPO1 expression was upregulated in CHF rats and in H9c2 cells treated with adriamycin. In cellular experiments, VPO1 knockdown improved cell viability, inhibited necrosis and the expression of proteins associated with the RIPK1/RIPK3/MLKL pathway. Mechanistically, VPO1 promoted cardiomyocyte programmed necrosis by interacting with the deubiquitinating enzyme CYLD, which enhanced RIPK1 ubiquitination and degradation, leading to activation of the RIPK1/RIPK3/MLKL signaling pathway. At animal level, overexpression of CYLD counteracted the cardiac failure, cardiac hypertrophy, myocardial injury, myocardial fibrosis, and tissue necrosis caused by VPO1 knockdown.
CONCLUSIONS
VPO1 exacerbates cardiomyocyte programmed necrosis in CHF rats by upregulating CYLD, which activates the RIPK1/RIPK3/MLKL signaling pathway. Thus, VPO1 may represent a potential therapeutic target for CHF.
背景
慢性心力衰竭(CHF)是一种严重的心血管疾病。血管过氧化物酶1(VPO1)与多种心血管疾病相关,但其在CHF中的作用仍不清楚。本研究旨在探讨VPO1在CHF中的作用。
方法
使用阿霉素诱导大鼠发生CHF,并评估VPO1和圆柱瘤蛋白(CYLD)的表达水平。同时,通过细胞活力测定、乳酸脱氢酶(LDH)水平测量以及对受体相互作用蛋白激酶1/受体相互作用蛋白激酶3/混合谱系激酶结构域样蛋白(RIPK1/RIPK3/MLKL)途径相关蛋白的分析,评估VPO1对H9c2细胞程序性坏死的影响。还研究了CYLD对RIPK1蛋白稳定性和泛素化的影响,以及VPO1与CYLD之间的相互作用。此外,使用超声心动图、苏木精-伊红(HE)染色、Masson染色以及测量心肌损伤相关因子,包括脑钠肽前体N末端(NT-proBNP)、天冬氨酸转氨酶(AST)、LDH和肌酸激酶同工酶(CK-MB),评估心脏结构和功能。
结果
VPO1在CHF大鼠和用阿霉素处理的H9c2细胞中表达上调。在细胞实验中,敲低VPO1可提高细胞活力,抑制坏死以及与RIPK1/RIPK3/MLKL途径相关的蛋白表达。机制上,VPO1通过与去泛素化酶CYLD相互作用促进心肌细胞程序性坏死,CYLD增强了RIPK1的泛素化和降解,导致RIPK1/RIPK3/MLKL信号通路激活。在动物水平,CYLD的过表达抵消了敲低VPO1所导致的心力衰竭、心脏肥大、心肌损伤、心肌纤维化和组织坏死。
结论
VPO1通过上调CYLD加重CHF大鼠心肌细胞程序性坏死,CYLD激活RIPK1/RIPK3/MLKL信号通路。因此,VPO1可能是CHF的一个潜在治疗靶点。
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