Exosomes and non-coding RNAs: Exploring their roles in human myocardial dysfunction.

Magdalena Kulus, Maryam Farzaneh, Mohadeseh Sheykhi-Sabzehpoush, Farhoodeh Ghaedrahmati, Fatemeh Mehravar, Małgorzata Józkowiak, Hanna Piotrowska-Kempisty, Dorota Bukowska, Paweł Antosik, Marzenna Podhorska-Okołów, Maciej Zabel, Paul Mozdziak, Piotr Dzięgiel, Bartosz Kempisty
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Abstract

Myocardial dysfunction, characterized by impaired cardiac muscle function, arises from diverse etiologies, including coronary artery disease, myocardial infarction, cardiomyopathies, hypertension, and valvular heart disease. Recent advancements have highlighted the roles of exosomes and non-coding RNAs in the pathophysiology of myocardial dysfunction. Exosomes are small extracellular vesicles released by cardiac and other cells that facilitate intercellular communication through their molecular cargo, including ncRNAs. ncRNAs are known to play critical roles in gene regulation through diverse mechanisms, impacting oxidative stress, fibrosis, and other factors associated with myocardial dysfunction. Dysregulation of these molecules correlates with disease progression, presenting opportunities for therapeutic interventions. This review explores the mechanistic interplay between exosomes and ncRNAs, underscoring their potential as biomarkers and therapeutic agents in myocardial dysfunction. Emerging evidence supports the use of engineered exosomes and modified ncRNAs to enhance cardiac repair by targeting signaling pathways associated with fibrosis, apoptosis, and angiogenesis. Despite promising preclinical results, delivery, stability, and immunogenicity challenges remain. Further research is needed to optimize clinical translation. Understanding these intricate mechanisms may drive the development of innovative strategies for diagnosing and treating myocardial dysfunction, ultimately improving patient outcomes.

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外泌体和非编码rna:探索它们在人类心肌功能障碍中的作用。
心肌功能障碍以心肌功能受损为特征,病因多样,包括冠状动脉疾病、心肌梗死、心肌病、高血压和瓣膜性心脏病。最近的进展突出了外泌体和非编码rna在心肌功能障碍病理生理中的作用。外泌体是由心脏和其他细胞释放的小细胞外囊泡,通过包括ncrna在内的分子货物促进细胞间通讯。众所周知,ncRNAs通过多种机制在基因调控中发挥关键作用,影响氧化应激、纤维化和其他与心肌功能障碍相关的因素。这些分子的失调与疾病进展相关,为治疗干预提供了机会。这篇综述探讨了外泌体和ncrna之间的相互作用机制,强调了它们作为心肌功能障碍生物标志物和治疗剂的潜力。新出现的证据支持使用工程外泌体和修饰的ncrna通过靶向与纤维化、细胞凋亡和血管生成相关的信号通路来增强心脏修复。尽管有很好的临床前结果,但递送、稳定性和免疫原性方面的挑战仍然存在。优化临床翻译需要进一步的研究。了解这些复杂的机制可能会推动诊断和治疗心肌功能障碍的创新策略的发展,最终改善患者的预后。
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