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首页> 外文期刊>Stem cells translational medicine. >Translating intracarotid artery transplantation of bone marrow‐derived NCS‐01 cells for ischemic stroke: Behavioral and histological readouts and mechanistic insights into stem cell therapy
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Translating intracarotid artery transplantation of bone marrow‐derived NCS‐01 cells for ischemic stroke: Behavioral and histological readouts and mechanistic insights into stem cell therapy

机译:翻译骨髓衍生NCS-01细胞的脑内动脉移植对缺血性脑卒中:行为和组织学读出和机械洞察力探讨干细胞疗法

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The present study used in vitro and in vivo stroke models to demonstrate the safety, efficacy, and mechanism of action of adult human bone marrow‐derived NCS‐01 cells. Coculture with NCS‐01 cells protected primary rat cortical cells or human neural progenitor cells from oxygen glucose deprivation. Adult rats that were subjected to middle cerebral artery occlusion, transiently or permanently, and subsequently received intracarotid artery or intravenous transplants of NCS‐01 cells displayed dose‐dependent improvements in motor and neurological behaviors, and reductions in infarct area and peri‐infarct cell loss, much better than intravenous administration. The optimal dose was 7.5?×?10sup6/sup cells/mL when delivered via the intracarotid artery within 3?days poststroke, although therapeutic effects persisted even when administered at 1 week after stroke. Compared with other mesenchymal stem cells, NCS‐01 cells ameliorated both the structural and functional deficits after stroke through a broad therapeutic window. NCS‐01 cells secreted therapeutic molecules, such as basic fibroblast growth factor and interleukin‐6, but equally importantly we observed for the first time the formation of filopodia by NCS‐01 cells under stroke conditions, characterized by cadherin‐positive processes extending from the stem cells toward the ischemic cells. Collectively, the present efficacy readouts and the novel filopodia‐mediated mechanism of action provide solid lab‐to‐clinic evidence supporting the use of NCS‐01 cells for treatment of stroke in the clinical setting.
机译:本研究在体外和体内卒中模型中使用,以证明成人人骨髓源性NCS-01细胞的安全性,疗效和机制。与NCS-01细胞的共蜂蜜保护原代大鼠皮质细胞或人体神经祖细胞免受氧血糖剥夺的影响。瞬时或永久地进行中脑动脉闭塞的成年大鼠,随后接受NCS-01细胞的脑内动脉或静脉内移植表现出对电动机和神经行为的剂量依赖性改善,并减少梗塞区域和PERI-INFARCT细胞损失,比静脉内给药更好。当通过颅内动脉内递送3.5℃时,最佳剂量为7.5?×10 6 细胞/ ml,尽管即使在中风后1周施用时也持续存在治疗效果。与其他间充质干细胞相比,NCS-01细胞通过广泛的治疗窗中中风后改善了结构和功能性缺陷。 NCS-01细胞分泌治疗分子,例如碱性成纤维细胞生长因子和白细胞介素-6,但同样重要的是,我们首次观察到在卒中条件下的NCS-01细胞形成氟肽,其特征在于从中延伸的钙粘蛋白阳性过程干细胞朝向缺血细胞。统称,目前的疗效读数和新型氟化碳腺癌的作用机制提供了支持使用NCS-01细胞用于治疗临床环境中卒中的固体实验室到临床证据。

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