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Myofibroblasts

机译:肌成纤维细胞

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Purpose of Review: Interest in the myofibroblast as a key player in propagation of chronic progressive fibrosis continues to elicit many publications, with focus on its cellular origins and the mechanisms underpinning their differentiation and/or transition. The objective of the review is to highlight this recent progress. Recent Findings: The epithelial origin of the myofibroblast in fibrosis has been challenged by recent studies, with the pericyte suggested as a possible precursor instead. Additional signaling pathways, including Notch, Wnt, and hedgehog, are implicated in myofibroblast differentiation. The importance of NADPH oxidase 4 was highlighted recently to suggest a potential link between cellular/oxidative stress and the genesis of the myofibroblast. Recent observations on the importance of lysophosphatidic acid in fibrosis suggest that this may be due, in part, to its ability to regulate myofibroblast differentiation. Finally, there is increasing evidence for the role of epigenetic mechanisms in regulating myofibroblast differentiation, including DNA methylation and miRNA regulation of gene expression. Summary: These recent discoveries open up a whole new array of potential targets for novel antifibrotic therapies. This is of special importance given the current bleak outlook for chronic progressive fibrotic diseases, such as scleroderma, due to lack of effective therapies.
机译:综述的目的:对肌成纤维细胞作为慢性进行性纤维化传播的关键参与者的兴趣继续引起许多出版物的关注,重点是其细胞起源以及支持其分化和/或转变的机制。审查的目的是强调这一最新进展。最新发现:纤维化中成肌纤维细胞的上皮起源已受到近期研究的挑战,建议将周细胞作为可能的前体。其他信号传导途径,包括Notch,Wnt和Hedgehog,与成肌纤维细胞分化有关。最近强调了NADPH氧化酶4的重要性,表明细胞/氧化应激与成肌纤维细胞的发生之间存在潜在的联系。关于溶血磷脂酸在纤维化中的重要性的最新观察表明,这可能部分是由于其调节成纤维细胞分化的能力。最后,越来越多的证据表明表观遗传机制在调节成纤维细胞分化中的作用,包括DNA甲基化和基因表达的miRNA调控。简介:这些最新发现为新型抗纤维化疗法开辟了一系列全新的潜在靶标。考虑到由于缺乏有效的治疗方法,目前对于慢性进行性纤维化疾病(例如硬皮病)的前景黯淡,因此,这一点特别重要。

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