MicroRNAs Inducing Proliferation of Quiescent Adult Cardiomyocytes.

Raghav Pandey, Rafeeq P H Ahmed
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引用次数: 18

Abstract

In the United States, each year over 700,000 people suffer from a heart attack and over 25% of deaths are related to heart disease, making it the leading cause of death. Following ischemic injury a part of the heart muscle is replaced by a scar tissue, reducing its functioning capacity. Recent advancements in surgical intervention and pharmacotherapy only provide symptomatic relief and do not address the root cause of the problem which is the massive loss of cardiomyocytes (CM). Therefore, the development of novel therapeutic intervention for the repair and regeneration of ischemic myocardium remains an area of intense research. While existing CM in zebra fish and neonatal mice are known to proliferate and replenish the infarcted heart, it has been shown that adult mammalian CM lose this ability, thus preventing regeneration of the scar tissue. There have been many attempts to facilitate regeneration of ischemic heart but have met with limited success. Micro-RNAs (miRNAs) are one of the promising candidates towards this goal as they are known to play important regulatory roles during differentiation and tissue regeneration, and regulate genetic information by post-transcriptional modification as well as regulation of other miRNAs. While previous work by Eulalio et al., showed miRNAs inducing proliferation in neonatal CM (NCM), we here identify miRNAs inducing proliferation of rat adult-CM (ACM). This commentary while analyses recent work by Eulalio et al[1] also shows some new data with microRNAs in rat adult-CMs. Further work into the mechanism of these miRNAs can determine their therapeutic potential towards regenerating cardiac tissue post ischemic injury.

诱导静止心肌细胞增殖的microrna。
在美国,每年有超过70万人患有心脏病,超过25%的死亡与心脏病有关,使其成为死亡的主要原因。缺血性损伤后,一部分心肌被疤痕组织所取代,降低了其功能。外科手术和药物治疗的最新进展只能提供症状缓解,而不能解决问题的根本原因,即大量心肌细胞(CM)的损失。因此,开发用于缺血心肌修复和再生的新型治疗干预措施仍然是一个研究热点。虽然已知斑马鱼和新生小鼠的CM能够增殖并补充梗死的心脏,但研究表明,成年哺乳动物的CM失去了这种能力,从而阻止了疤痕组织的再生。已有许多促进缺血心脏再生的尝试,但收效甚微。微rna (miRNAs)是实现这一目标的有希望的候选者之一,因为它们在分化和组织再生过程中发挥重要的调节作用,并通过转录后修饰以及其他miRNAs的调控来调节遗传信息。Eulalio等人之前的研究表明,miRNAs可诱导新生儿CM (NCM)的增殖,而我们在此发现了诱导成年大鼠CM (ACM)增殖的miRNAs。这篇评论在分析了Eulalio等人最近的工作的同时,也显示了大鼠成年cm中microrna的一些新数据。对这些mirna机制的进一步研究可以确定它们对缺血损伤后心脏组织再生的治疗潜力。
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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