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Identification of MFGE8 in mesenchymal stem cell secretome as an anti-fibrotic factor in liver fibrosis

机译:鉴定间充质干细胞分泌物中的MFGE8作为肝纤维化的抗纤维化因子

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摘要

The beneficial paracrine roles of mesenchymal stem cells (MSCs) in tissue repair have potential in therapeutic strategies against various diseases. However, the key therapeutic factors secreted from MSCs and their exact molecular mechanisms of action remain unclear. In this study, the cell-free secretome of umbilical cord-derived MSCs showed significant anti-fibrotic activity in the mouse models of liver fibrosis. The involved action mechanism was the regulation of hepatic stellate cell activation by direct inhibition of the TGFβ/Smad-signaling. Antagonizing the milk fat globule-EGF factor 8 (MFGE8) activity blocked the anti-fibrotic effects of the MSC secretome in vitro and in vivo. Moreover, MFGE8 was secreted by MSCs from the umbilical cord as well as other tissues, including teeth and bone marrow. Administration of recombinant MFGE8 protein alone had a significant anti-fibrotic effect in two different models of liver fibrosis. Additionally, MFGE8 downregulated TGFβ type I receptor expression by binding to αvβ3 integrin on HSCs. These findings revealed the potential role of MFGE8 in modulating TGFβ-signaling. Thus, MFGE8 could serve as a novel therapeutic agent for liver fibrosis.
机译:间充质干细胞(MSCs)在组织修复中的有益旁分泌作用在针对各种疾病的治疗策略中具有潜力。然而,尚不清楚MSC分泌的关键治疗因子及其确切的分子作用机制。在这项研究中,脐带来源的MSC的无细胞分泌组在肝纤维化的小鼠模型中显示出显着的抗纤维化活性。参与的作用机制是通过直接抑制TGFβ/ Smad信号传导来调节肝星状细胞的活化。拮抗乳脂球EGF因子8(MFGE8)的活性在体外和体内阻断了MSC分泌组的抗纤维化作用。而且,MFGE8是由MSC从脐带以及其他组织(包括牙齿和骨髓)分泌的。在两种不同的肝纤维化模型中,单独施用重组MFGE8蛋白具有显着的抗纤维化作用。另外,MFGE8通过与HSC上的αvβ3整联蛋白结合而下调了TGFβI型受体的表达。这些发现揭示了MFGE8在调节TGFβ信号中的潜在作用。因此,MFGE8可以作为肝纤维化的新型治疗剂。

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