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伤口愈合和纤维化过程中的成纤维细胞分化

Fibroblast differentiation in wound healing and fibrosis.

作者信息

Darby Ian A, Hewitson Tim D

机构信息

School of Medical Sciences, RMIT University, Melbourne, Australia.

出版信息

Int Rev Cytol. 2007;257:143-79. doi: 10.1016/S0074-7696(07)57004-X.

Abstract

The contraction of granulation tissue from skin wounds was first described in the 1960s. Later it was discovered that during tissue repair, fibroblasts undergo a change in phenotype from their normal relatively quiescent state in which they are involved in slow turnover of the extracellular matrix, to a proliferative and contractile phenotype termed myofibroblasts. These cells show some of the phenotypic characteristics of smooth muscle cells and have been shown to contract in vitro. In the 1990s, a number of researchers in different fields showed that myofibroblasts are present during tissue repair or response to injury in a variety of other tissues, including the liver, kidney, and lung. During normal repair processes, the myofibroblastic cells are lost as repair resolves to form a scar. This cell loss is via apoptosis. In pathological fibroses, myofibroblasts persist in the tissue and are responsible for fibrosis via increased matrix synthesis and for contraction of the tissue. In many cases this expansion of the extracellular matrix impedes normal function of the organ. For this reason much interest has centered on the derivation of myofibroblasts and the factors that influence their differentiation, proliferation, extracellular matrix synthesis, and survival. Further understanding of how fibroblast differentiation and myofibroblast phenotype is controlled may provide valuable insights into future therapies that can control fibrosis and scarring.

摘要

皮肤伤口处肉芽组织的收缩最早在20世纪60年代被描述。后来发现,在组织修复过程中,成纤维细胞的表型会发生变化,从它们正常相对静止的状态(此时它们参与细胞外基质的缓慢更新)转变为一种增殖性和收缩性的表型,即肌成纤维细胞。这些细胞表现出一些平滑肌细胞的表型特征,并且已被证明在体外能够收缩。在20世纪90年代,不同领域的一些研究人员表明,在包括肝脏、肾脏和肺在内的多种其他组织的组织修复或对损伤的反应过程中都存在肌成纤维细胞。在正常修复过程中,随着修复形成瘢痕,肌成纤维细胞会消失。这种细胞消失是通过凋亡实现的。在病理性纤维化中,肌成纤维细胞持续存在于组织中,并通过增加基质合成导致纤维化以及引起组织收缩。在许多情况下,这种细胞外基质的扩张会阻碍器官的正常功能。因此,人们的许多兴趣都集中在肌成纤维细胞的来源以及影响其分化、增殖、细胞外基质合成和存活的因素上。对成纤维细胞分化和肌成纤维细胞表型如何被控制的进一步理解可能会为未来控制纤维化和瘢痕形成的治疗方法提供有价值的见解。

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