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心血管疾病中的环状RNA:诊断与治疗的范式转变

Circular RNAs in cardiovascular disease: A paradigm shift in diagnosis and therapeutics.

作者信息

Parsanathan Rajesh, Sunil Sredha, Byju Rishaba

机构信息

Department of Biotechnology, School of Integrative Biology, Central University of Tamil Nadu, Neelakudi, Thiruvarur 610 005, Tamil Nadu, India.

Department of Biotechnology, School of Integrative Biology, Central University of Tamil Nadu, Neelakudi, Thiruvarur 610 005, Tamil Nadu, India.

出版信息

Life Sci. 2025 Jul 21;379:123877. doi: 10.1016/j.lfs.2025.123877.

Abstract

Cardiovascular diseases (CVDs) remain the leading cause of global mortality, accounting for 32 % of deaths worldwide in 2021. The increasing prevalence of CVDs highlights the urgent need for novel diagnostic and therapeutic approaches. Circular RNAs (circRNAs), a class of single-stranded RNA molecules produced via back-splicing, have gained attention as potential biomarkers and therapeutic targets due to their distinctive features. Unlike linear RNAs, circRNAs lack 5' caps and 3' poly(A) tails, making them highly resistant to exonuclease degradation and granting them an extended half-life of 19-24 h. Their stability, tissue- and disease-specific expression, evolutionary conservation, and responsiveness to pathological stimuli enable them to regulate key biological processes such as apoptosis, metabolism, and inflammation. Growing evidence links circRNAs to CVD pathogenesis: in cardiomyopathies, circHIPK3 and circFndc3b contribute to hypertrophy and diastolic dysfunction through miR-30a sponging and SERCA2a inhibition; in atherosclerosis, circANRIL exhibits protective effects by modulating ribosomal RNA synthesis and vascular smooth muscle cell proliferation; after myocardial infarction, circZNF609 reduces inflammation while circFndc3b helps prevent apoptosis; and in hypertension, downregulation of hsa-circ-0005870 serves as a specific biomarker. This review further explores circRNAs' diagnostic potential in biofluids, such as serum circHIPK3 for myocardial injury, and their therapeutic applications through silencing with antisense oligonucleotides or delivery of protective mimetics. Despite promising advances, challenges remain, including achieving tissue-specific delivery and addressing the complex pleiotropic effects of circRNAs. Successfully integrating circRNA-based tools into clinical practice could transform CVD management by enabling earlier detection and more personalized treatment strategies.

摘要

心血管疾病(CVDs)仍然是全球死亡的主要原因,2021年占全球死亡人数的32%。心血管疾病患病率的不断上升凸显了对新型诊断和治疗方法的迫切需求。环状RNA(circRNAs)是一类通过反向剪接产生的单链RNA分子,由于其独特的特征,作为潜在的生物标志物和治疗靶点受到了关注。与线性RNA不同,circRNAs缺乏5'帽和3'聚(A)尾,这使得它们对外切核酸酶降解具有高度抗性,并赋予它们19 - 24小时的延长半衰期。它们的稳定性、组织和疾病特异性表达、进化保守性以及对病理刺激的反应性使它们能够调节关键的生物学过程,如细胞凋亡、代谢和炎症。越来越多的证据将circRNAs与心血管疾病发病机制联系起来:在心肌病中,circHIPK3和circFndc3b通过海绵吸附miR - 30a和抑制SERCA2a导致心肌肥大和舒张功能障碍;在动脉粥样硬化中,circANRIL通过调节核糖体RNA合成和血管平滑肌细胞增殖发挥保护作用;心肌梗死后,circZNF609减轻炎症,而circFndc3b有助于防止细胞凋亡;在高血压中,hsa - circ - 0005870的下调作为一种特异性生物标志物。本综述进一步探讨了circRNAs在生物流体中的诊断潜力,如血清circHIPK3用于心肌损伤,以及通过反义寡核苷酸沉默或递送保护性模拟物的治疗应用。尽管取得了有前景的进展,但挑战仍然存在,包括实现组织特异性递送和解决circRNAs复杂的多效性影响。成功地将基于circRNA的工具整合到临床实践中,可以通过实现早期检测和更个性化的治疗策略来改变心血管疾病的管理。

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