Understanding myofibroblast origin in the fibrotic lung

Chinese medical journal pulmonary and critical care medicine Pub Date : 2024-09-01 DOI:10.1016/j.pccm.2024.08.003

Mahsa Zabihi , Mahtab Shahriari Felordi , Arun Lingampally , Saverio Bellusci , Xuran Chu , Elie El Agha

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Abstract

Idiopathic pulmonary fibrosis (IPF) is characterized by accumulation of myofibroblasts (MYFs) and extracellular matrix components, which leads to severe distortion and scarring of the gas exchange units of the lung, the alveoli, and ultimately respiratory failure. Fibrosis-associated MYFs are therefore widely regarded as the culprits that compromise the architectural makeup of the lung in fibrotic disease. During the past decade, the cellular source of MYFs has been intensely investigated. The rationale for such studies is that identifying the origin of these cells might help identify novel therapeutic targets and candidates to treat IPF patients. Recent advances in basic and translational research employing lineage tracing and multi-omics approaches have helped address the identity of MYF precursors, highlight the underlying heterogeneity, and to a less extent investigate MYF fate during fibrosis resolution. In this review, we discuss the current understanding of such important aspects of MYF biology as well as recent developments in the treatment of IPF.

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了解纤维化肺中肌成纤维细胞的起源

特发性肺纤维化（IPF）的特点是肌成纤维细胞（MYFs）和细胞外基质成分的积累，这会导致肺部气体交换单元--肺泡--严重变形和瘢痕形成，最终导致呼吸衰竭。因此，纤维化相关的 MYFs 被广泛认为是破坏纤维化疾病中肺部结构组成的罪魁祸首。在过去的十年中，人们对 MYFs 的细胞来源进行了深入研究。进行此类研究的理由是，确定这些细胞的来源可能有助于确定治疗 IPF 患者的新治疗靶点和候选者。最近，基础研究和转化研究取得了进展，采用了系谱追踪和多组学方法，有助于确定 MYF 前体的身份，突出潜在的异质性，并在较小程度上研究纤维化缓解过程中 MYF 的命运。在这篇综述中，我们将讨论目前对 MYF 生物学这些重要方面的理解以及治疗 IPF 的最新进展。

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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来源期刊

Chinese medical journal pulmonary and critical care medicine Critical Care and Intensive Care Medicine, Infectious Diseases, Pulmonary and Respiratory Medicine

CiteScore

0.40

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0.00%

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