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Mesenchymal progenitor cells derived from traumatized muscle enhance neurite growth

机译:来自受创伤的肌肉的间充质祖细胞增强神经突生长

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The success of peripheral nerve regeneration is governed by the rate and quality of axon bridging and myelination that occurs across the damaged region. Neurite growth and the migration of Schwann cells is regulated by neurotrophic factors produced as the nerve regenerates, and these processes can be enhanced by mesenchymal stem cells (MSCs), which also produce neurotrophic factors and other factors that improve functional tissue regeneration. Our laboratory has recently identified a population of mesenchymal progenitor cells (MPCs) that can be harvested from traumatized muscle tissue debrided and collected during orthopaedic reconstructive surgery. The objective of this study was to determine whether the traumatized muscle-derived MPCs exhibit neurotrophic function equivalent to that of bone marrow-derived MSCs. Similar gene- and protein-level expression of specific neurotrophic factors was observed for both cell types, and we localized neurogenic intracellular cell markers (brain-derived neurotrophic factor and nestin) to a subpopulation of both MPCs and MSCs. Furthermore, we demonstrated that the MPC-secreted factors were sufficient to enhance in vitro axon growth and cell migration in a chick embryonic dorsal root ganglia (DRG) model. Finally, DRGs in co-culture with the MPCs appeared to increase their neurotrophic function via soluble factor communication. Our findings suggest that the neurotrophic function of traumatized muscle-derived MPCs is substantially equivalent to that of the well-characterized population of bone marrow-derived MPCs, and suggest that the MPCs may be further developed as a cellular therapy to promote peripheral nerve regeneration.
机译:周围神经再生的成功取决于在受损区域发生的轴突桥接和髓鞘形成的速度和质量。神经再生过程中神经营养因子调节神经突的生长和雪旺细胞的迁移,而间充质干细胞(MSCs)可以增强神经营养因子和其他改善功能性组织再生的因子,从而促进这些过程。我们的实验室最近确定了可以从整形外科手术中清理和收集的受创伤肌肉组织中收获的间充质祖细胞(MPC)群体。这项研究的目的是确定受创伤的肌肉来源的MPC是否表现出与骨髓MSC相同的神经营养功能。两种细胞类型均观察到特定神经营养因子的相似基因和蛋白质水平表达,并且我们将神经原性细胞内细胞标记物(脑源性神经营养因子和巢蛋白)定位于MPC和MSC的亚群。此外,我们证明了MPC分泌的因子足以增强鸡胚背根神经节(DRG)模型中的体外轴突生长和细胞迁移。最后,与MPCs共培养的DRGs似乎通过可溶性因子通讯增加了其神经营养功能。我们的发现表明,受创伤的肌肉来源的MPC的神经营养功能与骨髓来源的MPC的特征明确的人群的神经营养功能基本相同,并且表明MPC可能会进一步发展为细胞疗法,以促进周围神经再生。

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