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Activin-mediated alterations of the fibroblast transcriptome and matrisome control the biomechanical properties of skin wounds

机译:激活素介导的成纤维细胞转录组和矩阵的改变控制皮肤伤口的生物力学性质

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Matrix deposition is essential for wound repair, but when excessive, leads to hypertrophic scars and fibrosis. The factors that control matrix deposition in skin wounds have only partially been identified and the consequences of matrix alterations for the mechanical properties of wounds are largely unknown. Here, we report how a single diffusible factor, activin A, affects the healing process across scales. Bioinformatics analysis of wound fibroblast transcriptome data combined with biochemical and histopathological analyses of wounds and functional in vitro studies identify that activin promotes pro-fibrotic gene expression signatures and processes, including glycoprotein and proteoglycan biosynthesis, collagen deposition, and altered collagen cross-linking. As a consequence, activin strongly reduces the wound and scar deformability, as identified by a non-invasive in vivo method for biomechanical analysis. These results provide mechanistic insight into the roles of activin in wound repair and fibrosis and identify the functional consequences of alterations in the wound matrisome at the biomechanical level.
机译:基质沉积对于伤口修复至关重要,但在过度时,导致肥厚疤痕和纤维化。仅部分鉴定了皮肤伤害中的基质沉积的因素,并且基质改变伤口力学性能的后果在很大程度上是未知的。在这里,我们报告了单一扩散因素如何激活素A,影响跨尺度的愈合过程。伤口成纤维细胞的生物信息分析与伤口生物化学和组织病理学分析相结合的伤口和功能性在体外研究鉴定该激活素促进促蛋白酶诱导的基因表达签名和方法,包括糖蛋白和蛋白多糖生物合成,胶原沉积和改变的胶原蛋白交联。因此,激活素强烈降低伤口和瘢痕可变形性,如通过体内生物力学分析的非侵入性的非侵入性鉴定。这些结果提供了机械洞察激活素在伤口修复和纤维化中的作用,并在生物力学水平处鉴定伤口矩阵中的改变的功能后果。

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