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The adult CNS retains the potential to direct region-specific differentiation of a transplanted neuronal precursor cell line

机译:成年的中枢神经系统保留了指导移植神经元前体细胞系区域特异性分化的潜力

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摘要

The chronic survival and differentiation of the conditionally immortalized neuronal cell line, RN33B, was examined following transplantation into the adult and neonatal rat hippocampus and cerebral cortex. In clonal culture, differentiated RN33B cells express p75NTR and trkB mRNA and protein, and respond to brain-derived neurotrophic factor treatment by inducing c-fos mRNA. Transplanted cells, identified using immunohistochemistry to detect beta- galactosidase expression, were seen in most animals up to 24 weeks posttransplantation (the latest time point examined). Stably integrated cells with various morphologies consistent with their transplantation site were observed. In the cerebral cortex, many RN33B cells differentiated with morphologies similar to pyramidal neurons and stellate cells. In the hippocampal formation, many RN33B cells assumed morphologies similar to pyramidal neurons characteristic of CA1 and CA3 regions, granular cell layer neurons of the dentate gyrus, and polymorphic neurons of the hilar region. Identical morphologies were observed in both adult and neonatal hosts, although a greater percentage of beta-galactosidase immunoreactive cells had differentiated in the neonatal brains. These results suggest that RN33B cells have the developmental plasticity to respond to local microenvironmental signals and that the adult brain retains the capacity to direct the differentiation of neuronal precursor cells in a direction that is consistent with that of endogenous neurons.
机译:移植到成年和新生大鼠海马和大脑皮层后,检查了条件永生化的神经元细胞系RN33B的长期存活和分化。在克隆培养中,分化的RN33B细胞表达p75NTR和trkB mRNA和蛋白,并通过诱导c-fos mRNA响应脑源性神经营养因子治疗。在大多数动物中,直到移植后24周(最近检查的时间点),都可以看到使用免疫组织化学方法检测到的β-半乳糖苷酶表达所识别的移植细胞。观察到稳定整合的细胞,其形态与移植部位一致。在大脑皮层中,许多RN33B细胞的分化形态类似于锥体神经元和星状细胞。在海马结构中,许多RN33B细胞的形态类似于CA1和CA3区的锥体神经元,齿状回的颗粒细胞层神经元和肺门区的多态神经元。在成年和新生儿宿主中均观察到相同的形态,尽管在新生大脑中分化出更大比例的β-半乳糖苷酶免疫反应性细胞。这些结果表明,RN33B细胞具有对局部微环境信号作出反应的发育可塑性,并且成年大脑保留了在与内源性神经元一致的方向上指导神经元前体细胞分化的能力。

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