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miR-192 在糖尿病肾病中的作用:临床应用和作用机制。

Roles of microRNA-192 in diabetic nephropathy: the clinical applications and mechanisms of action.

机构信息

Department of Nephrology, Taizhou Central Hospital (Taizhou University Hospital), Taizhou, Zhejiang, China.

Department of Nephrology, Jiaxing Hospital of Traditional Chinese Medicine, Jiaxing, Zhejiang, China.

出版信息

Front Endocrinol (Lausanne). 2023 Jun 15;14:1179161. doi: 10.3389/fendo.2023.1179161. eCollection 2023.

Abstract

Diabetic nephropathy (DN) is one of the most common and intractable microvascular complications of diabetes worldwide, serving as the main cause of terminal renal disease. Due to the lack of early specific symptoms and diagnostic markers, DN severely threatens the sufferer's life. MicroRNA-192 (miR-192) was early identified in human renal cortical tissue and stored and excreted in urine as microvesicles. MiR-192 was found to be involved in the development of DN. For the first time, the present review summarized all the current evidence on the topic of the roles of miR-192 in DN. Finally, 28 studies (ten clinical trials and eighteen experimental studies) were eligible for thorough reviewing. Most of the clinical trials (7/10, 70%) indicated miR-192 might be a protective factor for DN development and progression, while the majority of experimental studies (14/18, 78%) suggested miR-192 might be a pathogenic factor for DN. Mechanistically, miR-192 interacts with various direct targeted proteins (i.e., ZEB1, ZEB2, SIP1, GLP1R, and Egr1) and signaling cascades (i.e., SMAD/TGF-β and PTEN/PI3K/AKT), together contribute to the pathogenesis of DN through epithelial-to-mesenchymal transition (EMT), extracellular matrix deposition, and fibrosis formation. The current review highlights the dual role of miR-192 in the development of DN. Low serum miR-192 expression could be applied for the early prediction of DN (the early stage of DN), while the high miR-192 level in renal tissues and urine may imply the progression of DN (the late stage of DN). Further investigations are still warranted to illustrate this inconsistent phenomenon, which may facilitate promoting the therapeutic applications of miR-192 in predicting and treating DN.

摘要

糖尿病肾病(DN)是全球范围内糖尿病最常见和最顽固的微血管并发症之一,也是终末期肾病的主要病因。由于缺乏早期特异性症状和诊断标志物,DN 严重威胁着患者的生命。微小 RNA-192(miR-192)最早在人肾皮质组织中被发现,并以微泡的形式在尿液中储存和排泄。研究发现 miR-192 参与了 DN 的发生。本综述首次总结了 miR-192 在 DN 中的作用的所有现有证据。最后,有 28 项研究(10 项临床试验和 18 项实验研究)符合深入审查的条件。大多数临床试验(7/10,70%)表明 miR-192 可能是 DN 发展和进展的保护因素,而大多数实验研究(14/18,78%)表明 miR-192 可能是 DN 的致病因素。从机制上讲,miR-192 与各种直接靶向蛋白(即 ZEB1、ZEB2、SIP1、GLP1R 和 Egr1)和信号通路(即 SMAD/TGF-β 和 PTEN/PI3K/AKT)相互作用,通过上皮-间充质转化(EMT)、细胞外基质沉积和纤维化形成共同导致 DN 的发病机制。本综述强调了 miR-192 在 DN 发病机制中的双重作用。血清中 miR-192 表达水平降低可用于早期预测 DN(DN 的早期阶段),而肾脏组织和尿液中高 miR-192 水平可能意味着 DN 的进展(DN 的晚期阶段)。进一步的研究仍有必要阐明这种不一致的现象,这可能有助于促进 miR-192 在预测和治疗 DN 中的治疗应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dda5/10309560/1293c0cd1a0f/fendo-14-1179161-g001.jpg

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