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未分化人骨髓间充质干细胞移植对大鼠 6-羟多巴胺神经毒性的保护作用。

Transplantation of undifferentiated human mesenchymal stem cells protects against 6-hydroxydopamine neurotoxicity in the rat.

机构信息

Interdepartmental Research Center for Parkinson's Disease, IRCCS Neurological Institute "C. Mondino," Pavia, Italy.

出版信息

Cell Transplant. 2010;19(2):203-17. doi: 10.3727/096368909X479839. Epub 2009 Nov 10.

DOI:10.3727/096368909X479839
PMID:19906332
Abstract

Stem cells have been increasingly recognized as a potential tool to replace or support cells damaged by the neurodegenerative process that underlies Parkinson's disease (PD). In this frame, human adult mesenchymal stem cells (hMSCs) have been proposed as an attractive alternative to heterologous embryonic or neural precursor cells. To address this issue, in this study we implanted undifferentiated hMSCs into the striatum of rats bearing a lesion of the nigrostriatal pathway induced by local injection of 6-hydroxydopamine (6-OHDA), a widely recognized rodent model of PD. Before grafting, cultured hMSCs expressed markers of both undifferentiated and committed neural cells, including nestin, GAP-43, NSE, beta-tubulin III, and MAP-2, as well as several cytokine mRNAs. No glial or specific neuronal markers were detected. Following transplantation, some hMSCs acquired a glial-like phenotype, as shown by immunoreactivity for glial fibrillary acid protein (GFAP), but only in animals bearing the nigrostriatal lesion. More importantly, rats that received the striatal graft showed increased survival of both cell bodies and terminals of dopaminergic, nigrostriatal neurons, coupled with a reduction of the behavioral abnormalities (apomorphine-induced turning behavior) associated with the lesion. No differentiation of the MSCs toward a neuronal (dopaminergic) phenotype was observed in vivo. In conclusion, our results suggest that grafted hMSCs exert neuroprotective effects against nigrostriatal degeneration induced by 6-OHDA. The mechanisms underlying this effect remain to be clarified, although it is likely that the acquisition of a glial phenotype by grafted hMSCs may lead to the release of prosurvival cytokines within the lesioned striatum.

摘要

干细胞已逐渐被认为是一种潜在的工具,可以替代或支持由帕金森病(PD)所涉及的神经退行性过程所损伤的细胞。在这种情况下,人类成体间充质干细胞(hMSCs)已被提议作为异体胚胎或神经前体细胞的有吸引力的替代品。为了解决这个问题,在这项研究中,我们将未分化的 hMSCs 植入到由局部注射 6-羟多巴胺(6-OHDA)引起的黑质纹状体通路损伤的大鼠纹状体中,6-OHDA 是一种广泛认可的 PD 啮齿动物模型。在移植前,培养的 hMSCs 表达了未分化和定向神经细胞的标志物,包括巢蛋白、GAP-43、NSE、β-微管蛋白 III 和 MAP-2,以及几种细胞因子的 mRNA。未检测到神经胶质或特定神经元标志物。移植后,一些 hMSCs 获得了神经胶质样表型,如胶质纤维酸性蛋白(GFAP)的免疫反应性所示,但仅在患有黑质纹状体损伤的动物中。更重要的是,接受纹状体移植的大鼠显示多巴胺能、黑质纹状体神经元的细胞体和末梢的存活增加,同时与损伤相关的行为异常(阿扑吗啡诱导的旋转行为)减少。在体内未观察到 MSC 向神经元(多巴胺能)表型的分化。总之,我们的结果表明,移植的 hMSCs 对 6-OHDA 诱导的黑质纹状体变性具有神经保护作用。这种作用的机制尚待阐明,尽管移植的 hMSCs 获得神经胶质样表型可能导致损伤纹状体中释放促生存细胞因子。

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