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iPS-Derived Early Oligodendrocyte Progenitor Cells from SPMS Patients Reveal Deficient In Vitro Cell Migration Stimulation

机译:来自SPMS患者的IPS衍生的早期少寡粒细胞祖细胞揭示了体外细胞迁移刺激的缺陷

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摘要

The most challenging aspect of secondary progressive multiple sclerosis (SPMS) is the lack of efficient regenerative response for remyelination, which is carried out by the endogenous population of adult oligoprogenitor cells (OPCs) after proper activation. OPCs must proliferate and migrate to the lesion and then differentiate into mature oligodendrocytes. To investigate the OPC cellular component in SPMS, we developed induced pluripotent stem cells (iPSCs) from SPMS-affected donors and age-matched controls (CT). We confirmed their efficient and similar OPC differentiation capacity, although we reported SPMS-OPCs were transcriptionally distinguishable from their CT counterparts. Analysis of OPC-generated conditioned media (CM) also evinced differences in protein secretion. We further confirmed SPMS-OPC CM presented a deficient capacity to stimulate OPC in vitro migration that can be compensated by exogenous addition of specific components. Our results provide an SPMS-OPC cellular model and encouraging venues to study potential cell communication deficiencies in the progressive form of multiple sclerosis (MS) for future treatment strategies.
机译:继发性多发性硬化症(SPMS)的最具挑战性方面是缺乏对核髓髓鞘产生的有效再生反应,其在适当的激活后通过成人寡酮细胞(OPCS)的内源性群体进行。 OPCs必须增殖和迁移到病变,然后分化为成熟的少寡核细胞。为了研究SPMS中的OPC细胞组分,我们从受影响的SPMS患者和年龄匹配的对照(CT)产生诱导多能干细胞(IPSC)。我们确认了它们的高效和类似的OPC差异化能力,尽管我们报告了SPMS-OPCs与其CT对应物转录可分类。分析OPC产生的条件介质(CM)也表达了蛋白质分泌的差异。我们进一步证实SPMS-OPC CM呈现缺乏刺激OPC体外迁移的能力,这可以通过外源添加特定组分来补偿。我们的结果提供了SPMS-OPC蜂窝模型,并令人振奋的地点以研究多发性硬化症(MS)的逐步形式的潜在细胞通信缺陷,以备将来治疗策略。

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