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Effect of Hypoxia-Induced MicroRNA-210 Expression on Cardiovascular Disease and the Underlying Mechanism

机译:缺氧诱导的microRNA-210表达对心血管疾病的影响及根本机制

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Cardiovascular diseases have high morbidity and mortality rates worldwide, and their treatment and prevention are challenging. MicroRNAs are a series of noncoding RNAs with highly conserved sequences and regulate gene expression by inhibiting mRNA transcription or degrading targeting proteins. MicroRNA-210 is significantly upregulated during hypoxia and plays a protective role by inhibiting apoptosis and regulating cell proliferation, differentiation, migration, mitochondrial metabolism, and angiogenesis in hypoxic cells. MicroRNA-210 expression is altered in cardiovascular diseases such as atherosclerosis, acute myocardial infarction, preeclampsia, aortic stenosis, and heart failure, and overexpression of microRNA-210 in some of these diseases exerts protective effects on target organs. Furthermore, chronically upregulated miR-210 potentially plays a marked pathogenic role in specific situations. This review primarily focuses on the upstream pathways, downstream targets, clinical progress in cardiovascular disease, and potential applications of microRNA-210.
机译:心血管疾病具有全球性高的发病率和死亡率,以及他们的治疗和预防挑战。 MicroRNA是一系列具有高度保守序列的非沉积RNA,并通过抑制mRNA转录或降解靶向蛋白来调节基因表达。 MicroRNA-210在缺氧期间显着上调,通过抑制细胞凋亡和调节细胞增殖,分化,迁移,线粒体代谢和缺氧细胞血管生成起到保护作用。 MicroRNA-210表达在动脉粥样硬化,急性心肌梗死,先兆子痫,主动脉狭窄和心力衰竭等心血管疾病中改变,并且在一些这些疾病中的MicroRNA-210的过度表达对靶器官产生了保护作用。此外,长期上调的miR-210可能在特定情况下发挥明显的致病作用。本综述主要集中在上游途径,下游目标,心血管疾病中的临床进展以及MicroRNA-210的潜在应用。

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