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鞘内注射间充质干细胞源性神经前体细胞对实验性多发性硬化模型的临床和病理影响。

Clinical and pathological effects of intrathecal injection of mesenchymal stem cell-derived neural progenitors in an experimental model of multiple sclerosis.

机构信息

Multiple Sclerosis Research Center of New York, 521W. 57th St., 4th floor, New York, NY 10019, USA.

出版信息

J Neurol Sci. 2012 Feb 15;313(1-2):167-77. doi: 10.1016/j.jns.2011.08.036. Epub 2011 Oct 1.

DOI:10.1016/j.jns.2011.08.036
PMID:21962795
Abstract

Multiple sclerosis (MS) is associated with irreversible disability in a significant proportion of patients. At present, there is no treatment to halt or reverse the progression of established disability. In an effort to develop cell therapy-based strategies for progressive MS, we investigated the pre-clinical efficacy of bone marrow mesenchymal stem cell-derived neural progenitors (MSC-NPs) as an autologous source of stem cells. MSC-NPs consist of a subpopulation of bone marrow MSCs with neural progenitor and immunoregulatory properties, and a reduced capacity for mesodermal differentiation, suggesting that this cell population may be appropriate for clinical application in the CNS. We investigated whether MSC-NPs could promote repair and recovery after intrathecal injection into mice with EAE. Multiple injections of MSC-NPs starting at the onset of the chronic phase of disease improved neurological function compared to controls, whereas a single injection had no effect on disease scores. Intrathecal injection of MSC-NPs correlated with reduced immune cell infiltration, reduced area of demyelination, and increased number of endogenous nestin-positive progenitor cells in EAE mice. These observations suggest that MSC-NPs may influence the rate of repair through effects on endogenous progenitors in the spinal cord. This study supports the use of autologous MSC-NPs in MS patients as a means of promoting CNS repair.

摘要

多发性硬化症(MS)在很大比例的患者中与不可逆转的残疾相关。目前,尚无治疗方法可以阻止或逆转已确立的残疾进展。为了开发基于细胞治疗的进展性 MS 策略,我们研究了骨髓间充质干细胞源性神经祖细胞(MSC-NPs)作为自体干细胞来源的临床前疗效。MSC-NPs 由骨髓 MSC 的一个亚群组成,具有神经祖细胞和免疫调节特性,并且中胚层分化能力降低,这表明该细胞群可能适合 CNS 的临床应用。我们研究了 MSC-NPs 是否可以在 EAE 小鼠鞘内注射后促进修复和恢复。与对照组相比,疾病慢性期开始时多次注射 MSC-NPs 可改善神经功能,而单次注射对疾病评分无影响。MSC-NPs 的鞘内注射与免疫细胞浸润减少、脱髓鞘面积减少和 EAE 小鼠内源性巢蛋白阳性祖细胞数量增加相关。这些观察结果表明,MSC-NPs 可能通过对脊髓内源性祖细胞的影响来影响修复速度。这项研究支持在 MS 患者中使用自体 MSC-NPs 作为促进 CNS 修复的一种手段。

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