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分化因子可诱导小鼠多能间充质干细胞克隆中肌肉、脂肪、软骨和骨的表达。

Differentiation factors induce expression of muscle, fat, cartilage, and bone in a clone of mouse pluripotent mesenchymal stem cells.

作者信息

Rogers J J, Young H E, Adkison L R, Lucas P A, Black A C

机构信息

Department of Surgery, Mercer University School of Medicine, Medical Center of Central Georgia, Macon.

出版信息

Am Surg. 1995 Mar;61(3):231-6.

PMID:7887536
Abstract

Growth factors have been used experimentally to accelerate wound healing by increasing scar tissue formation at a wound site. These studies suggest that stimulation of fibroblastic differentiation and proliferation are essential components of adult tissue repair. Recent studies report the presence of mesenchymal stem cells within granulation tissue and as connective tissue-resident stem cells. This suggests that mesenchymal stem cells as well as fibroblasts may contribute to wound healing and repair. To determine the potential for mesenchymal stem cells to contribute to nonfibrogenic tissue repair, a clonal population of murine mesenchymal stem cells was examined with dexamethasone, a general differentiation agent, and muscle morphogenetic protein, a specific differentiation-inducing agent. Dexamethasone induced the expression of phenotypic markers for fat, cartilage, and bone in the stem cells. Muscle morphogenetic protein induced the expression of mRNAs for the muscle specific regulatory genes MyoD1 and myogenin in these cells. These results suggest that pluripotent mesenchymal stem cells within connective tissue compartments and granulation tissue have the potential to contribute to functional tissue restoration, rather than contributing solely to fibrogenic scar tissue formation during tissue repair.

摘要

生长因子已被用于实验,通过增加伤口部位的瘢痕组织形成来加速伤口愈合。这些研究表明,刺激成纤维细胞分化和增殖是成人组织修复的重要组成部分。最近的研究报告称,肉芽组织中存在间充质干细胞,且其作为结缔组织驻留干细胞。这表明间充质干细胞和成纤维细胞可能都有助于伤口愈合和修复。为了确定间充质干细胞对非纤维化组织修复的潜在作用,用一种通用分化剂地塞米松和一种特定分化诱导剂肌肉形态发生蛋白对小鼠间充质干细胞的克隆群体进行了检测。地塞米松诱导干细胞中脂肪、软骨和骨的表型标志物表达。肌肉形态发生蛋白诱导这些细胞中肌肉特异性调节基因MyoD1和肌细胞生成素的mRNA表达。这些结果表明,结缔组织隔室和肉芽组织中的多能间充质干细胞有可能促进功能性组织修复,而不是仅在组织修复过程中促进纤维化瘢痕组织形成。

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