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人牙髓干细胞在周围神经再生中表达 STRO-1、c-kit 和 CD34 标志物。

Human dental pulp stem cells expressing STRO-1, c-kit and CD34 markers in peripheral nerve regeneration.

机构信息

Department of Surgery, Medicine, Dentistry and Morphological Sciences with interest in Transplant, Oncology and Regenerative Medicine, University of Modena and Reggio Emilia, Modena, Italy.

Department of Obstetrics and Gynecology, IRCCS Arcispedale Santa Maria Nuova, Reggio Emilia, Italy.

出版信息

J Tissue Eng Regen Med. 2018 Feb;12(2):e774-e785. doi: 10.1002/term.2378. Epub 2017 Mar 2.

DOI:10.1002/term.2378
PMID:27943583
Abstract

Peripheral nerve injuries are a commonly encountered clinical problem and often result in long-term functional defects. The application of stem cells able to differentiate in Schwann cell-like cells in vitro and in vivo, could represent an attractive therapeutic approach for the treatment of nerve injuries. Further, stem cells sources sharing the same embryological origin as Schwann cells might be considered a suitable tool. The aim of this study was to demonstrate the ability of a neuroectodermal subpopulation of human STRO-1 /c-Kit /CD34 DPSCs, expressing P75 , nestin and SOX-10, to differentiate into Schwann cell-like cells in vitro and to promote axonal regeneration in vivo, which led to functional recovery as measured by sustained gait improvement, in animal rat model of peripheral nerve injury. Transplanted human dental pulp stem cells (hDPSCs) engrafted into sciatic nerve defect, as revealed by the positive staining against human nuclei, showed the expression of typical Schwann cells markers, S100b and, noteworthy, a significant number of myelinated axons was detected. Moreover, hDPSCs promoted axonal regeneration from proximal to distal stumps 1 month after transplantation. This study demonstrates that STRO-1 /c-Kit /CD34 hDPSCs, associated with neural crest derivation, represent a promising source of stem cells for the treatment of demyelinating disorders and might provide a valid alternative tool for future clinical applications to achieve functional recovery after injury or peripheral neuropathies besides minimizing ethical issues. Copyright © 2016 John Wiley & Sons, Ltd.

摘要

周围神经损伤是一种常见的临床问题,常导致长期的功能缺陷。体外和体内能分化为许旺细胞样细胞的干细胞的应用,可能代表一种有吸引力的治疗神经损伤的方法。此外,与许旺细胞具有相同胚胎起源的干细胞来源可能被认为是一种合适的工具。本研究旨在证明表达 P75、巢蛋白和 SOX-10 的人 STRO-1/c-Kit/CD34 DPSCs 的神经外胚层亚群在体外分化为许旺细胞样细胞的能力,并促进体内轴突再生,从而导致功能恢复,如动物大鼠周围神经损伤模型中持续步态改善所测量的。移植的人牙髓干细胞(hDPSCs)在坐骨神经缺损中被移植,如人核的阳性染色所显示的,表现出典型的许旺细胞标志物 S100b 的表达,值得注意的是,检测到大量有髓轴突。此外,hDPSCs 促进了从近端到远端残端的轴突再生,在移植后 1 个月。这项研究表明,与神经嵴起源相关的 STRO-1/c-Kit/CD34 hDPSCs 代表了治疗脱髓鞘疾病的有前途的干细胞来源,并且可能为未来的临床应用提供有效的替代工具,以实现损伤或周围神经病变后的功能恢复,同时最小化伦理问题。版权所有 © 2016 约翰威立父子公司

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