首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Transplanted human fetal neural stem cells survive migrate and differentiate in ischemic rat cerebral cortex
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Transplanted human fetal neural stem cells survive migrate and differentiate in ischemic rat cerebral cortex

机译:移植的人类胎儿神经干细胞在缺血大鼠大脑皮层中存活迁移并分化

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摘要

We characterize the survival, migration, and differentiation of human neurospheres derived from CNS stem cells transplanted into the ischemic cortex of rats 7 days after distal middle cerebral artery occlusion. Transplanted neurospheres survived robustly in naive and ischemic brains 4 wk posttransplant. Survival was influenced by proximity of the graft to the stroke lesion and was negatively correlated with the number of IB4-positive inflammatory cells. Targeted migration of the human cells was seen in ischemic animals, with many human cells migrating long distances (≈1.2 mm) predominantly toward the lesion; in naive rats, cells migrated radially from the injection site in smaller number and over shorter distances (0.2 mm). The majority of migrating cells in ischemic rats had a neuronal phenotype. Migrating cells between the graft and the lesion expressed the neuroblast marker doublecortin, whereas human cells at the lesion border expressed the immature neuronal marker β-tubulin, although a small percentage of cells at the lesion border also expressed glial fibrillary acid protein (GFAP). Thus, transplanted human CNS (hCNS)-derived neurospheres survived robustly in naive and ischemic brains, and the microenvironment influenced their migration and fate.
机译:我们表征了远端中脑动脉闭塞7天后,来自中枢神经系统干细胞的人神经球的存活,迁移和分化。移植后的第4周,已移植的神经球在幼稚和缺血性脑中均能牢固存活。存活率受移植物与中风病灶的接近程度的影响,并且与IB4阳性炎症细胞的数量呈负相关。在缺血动物中可以观察到人类细胞的靶向迁移,许多人类细胞主要向病变迁移长距离(约1.2毫米)。在幼稚大鼠中,细胞从注射部位放射状迁移的数量较少,且距离较短(0.2毫米)。缺血大鼠中的大多数迁移细胞具有神经元表型。移植物和病变之间的迁移细胞表达了神经母细胞标记的双皮质素,而病变边界处的人类细胞表达了未成熟的神经元标记物β-微管蛋白,尽管病变边界处的细胞中有一小部分也表达了神经胶质纤维酸性蛋白(GFAP)。因此,源自人类CNS(hCNS)的移植神经球在幼稚和缺血性脑中均能牢固存活,并且微环境影响了它们的迁移和命运。

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