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Tridermal tumorigenesis of induced pluripotent stem cells transplanted in ischemic brain

机译:诱导多能干细胞移植入缺血性脑的三真皮肿瘤发生

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摘要

Stroke is a major neurologic disorder. Induced pluripotent stem (iPS) cells can be produced from basically any part of patients, with high reproduction ability and pluripotency to differentiate into various types of cells, suggesting that iPS cells can provide a hopeful therapy for cell transplantation. However, transplantation of iPS cells into ischemic brain has not been reported. In this study, we showed that the iPS cells fate in a mouse model of transient middle cerebral artery occlusion (MCAO). Undifferentiated iPS cells (5 × 105) were transplanted into ipsilateral striatum and cortex at 24 h after 30 mins of transient MCAO. Behavioral and histologic analyses were performed at 28 day after the cell transplantation. To our surprise, the transplanted iPS cells expanded and formed much larger tumors in mice postischemic brain than in sham-operated brain. The clinical recovery of the MCAO+iPS group was delayed as compared with the MCAO+PBS (phosphate-buffered saline) group. iPS cells formed tridermal teratoma, but could supply a great number of Dcx-positive neuroblasts and a few mature neurons in the ischemic lesion. iPS cells have a promising potential to provide neural cells after ischemic brain injury, if tumorigenesis is properly controlled.
机译:中风是一种主要的神经系统疾病。诱导的多能干(iPS)细胞基本上可以从患者的任何部位产生,具有高繁殖能力和多能性以分化成各种类型的细胞,这表明iPS细胞可以为细胞移植提供希望的疗法。然而,尚未报道将iPS细胞移植到缺血性脑中。在这项研究中,我们显示了iPS细胞在短暂性大脑中动脉闭塞(MCAO)小鼠模型中的命运。将未分化的iPS细胞(5×10 5 )在短暂MCAO 30分钟后24 h移植到同侧纹状体和皮层。在细胞移植后第28天进行行为和组织学分析。令我们惊讶的是,移植的iPS细胞在缺血后脑部的小鼠中扩张并形成了比假手术脑部更大的肿瘤。与MCAO + PBS(磷酸盐缓冲液)组相比,MCAO + iPS组的临床恢复延迟。 iPS细胞形成了三层皮畸胎瘤,但在缺血性病变中可提供大量Dcx阳性神经母细胞和一些成熟神经元。如果适当地控制肿瘤发生,iPS细胞在缺血性脑损伤后具有提供神经细胞的潜力。

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