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细胞外囊泡在器官纤维化中的作用:机制、治疗策略和诊断。

Extracellular Vesicles in Organ Fibrosis: Mechanisms, Therapies, and Diagnostics.

机构信息

Center for Clinical and Translational Research, The Research Institute at Nationwide Children's Hospital, Columbus, OH 43205, USA.

Department of Surgery, Division of Pediatric Surgery, The Ohio State University Wexner Medical Center, Columbus, OH 43212, USA.

出版信息

Cells. 2021 Jun 25;10(7):1596. doi: 10.3390/cells10071596.

Abstract

Fibrosis is the unrelenting deposition of excessively large amounts of insoluble interstitial collagen due to profound matrigenic activities of wound-associated myofibroblasts during chronic injury in diverse tissues and organs. It is a highly debilitating pathology that affects millions of people globally and leads to decreased function of vital organs and increased risk of cancer and end-stage organ disease. Extracellular vesicles (EVs) produced within the chronic wound environment have emerged as important vehicles for conveying pro-fibrotic signals between many of the cell types involved in driving the fibrotic response. On the other hand, EVs from sources such as stem cells, uninjured parenchymal cells, and circulation have in vitro and in vivo anti-fibrotic activities that have provided novel and much-needed therapeutic options. Finally, EVs in body fluids of fibrotic individuals contain cargo components that may have utility as fibrosis biomarkers, which could circumvent current obstacles to fibrosis measurement in the clinic, allowing fibrosis stage, progression, or regression to be determined in a manner that is accurate, safe, minimally-invasive, and conducive to repetitive testing. This review highlights the rapid and recent progress in our understanding of EV-mediated fibrotic pathogenesis, anti-fibrotic therapy, and fibrosis staging in the lung, kidney, heart, liver, pancreas, and skin.

摘要

纤维化是由于慢性损伤时与创伤相关的肌成纤维细胞在基质生成方面的深刻活性,导致大量不可溶的细胞外间质胶原过度沉积。它是一种高度衰弱的病理学,影响着全球数百万人,导致重要器官功能下降,癌症风险增加和终末期器官疾病。在慢性创面环境中产生的细胞外囊泡(EVs)已成为在许多参与驱动纤维化反应的细胞类型之间传递促纤维化信号的重要载体。另一方面,来自干细胞、未受伤的实质细胞和循环等来源的 EVs 具有体外和体内的抗纤维化活性,为纤维化治疗提供了新的急需的治疗选择。最后,纤维化个体的体液中的 EV 包含可能作为纤维化生物标志物有用的货物成分,这可以避免目前临床纤维化测量中的障碍,使纤维化分期、进展或消退能够以准确、安全、微创和有利于重复测试的方式确定。本综述重点介绍了我们在理解 EV 介导的纤维化发病机制、抗纤维化治疗以及肺、肾、心、肝、胰腺和皮肤纤维化分期方面的快速和最新进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1056/8305303/b70b36f77913/cells-10-01596-g001.jpg

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