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胚胎干细胞来源的神经祖细胞在蜗神经干中的植入与分化:突起向柯蒂氏器的生长。

Engraftment and differentiation of embryonic stem cell-derived neural progenitor cells in the cochlear nerve trunk: growth of processes into the organ of Corti.

作者信息

Corrales C Eduardo, Pan Luying, Li Huawei, Liberman M Charles, Heller Stefan, Edge Albert S B

机构信息

Department of Otology and Laryngology, Harvard Medical School, Boston, MA 02115, USA.

出版信息

J Neurobiol. 2006 Nov;66(13):1489-500. doi: 10.1002/neu.20310.

Abstract

Hearing loss in mammals is irreversible because cochlear neurons and hair cells do not regenerate. To determine whether we could replace neurons lost to primary neuronal degeneration, we injected EYFP-expressing embryonic stem cell-derived mouse neural progenitor cells into the cochlear nerve trunk in immunosuppressed animals 1 week after destroying the cochlear nerve (spiral ganglion) cells while leaving hair cells intact by ouabain application to the round window at the base of the cochlea in gerbils. At 3 days post transplantation, small grafts were seen that expressed endogenous EYFP and could be immunolabeled for neuron-specific markers. Twelve days after transplantation, the grafts had neurons that extended processes from the nerve core toward the denervated organ of Corti. By 64-98 days, the grafts had sent out abundant processes that occupied a significant portion of the space formerly occupied by the cochlear nerve. The neurites grew in fasciculating bundles projecting through Rosenthal's canal, the former site of spiral ganglion cells, into the osseous spiral lamina and ultimately into the organ of Corti, where they contacted hair cells. Neuronal counts showed a significant increase in neuronal processes near the sensory epithelium, compared to animals that were denervated without subsequent stem cell transplantation. The regeneration of these neurons shows that neurons differentiated from stem cells have the capacity to grow to a specific target in an animal model of neuronal degeneration.

摘要

哺乳动物的听力损失是不可逆的,因为耳蜗神经元和毛细胞不会再生。为了确定我们是否能够替代因原发性神经元变性而丧失的神经元,我们在沙土鼠耳蜗神经(螺旋神经节)细胞被破坏1周后,将表达增强型黄色荧光蛋白(EYFP)的胚胎干细胞衍生的小鼠神经祖细胞注射到免疫抑制动物的耳蜗神经干中,同时通过向耳蜗底部圆窗应用哇巴因来保持毛细胞完整。移植后3天,可见小的移植物表达内源性EYFP,并且可以用神经元特异性标记物进行免疫标记。移植后12天,移植物中有神经元从神经核心向失神经支配的柯蒂氏器伸出突起。到64 - 98天时,移植物发出大量突起,占据了以前由耳蜗神经占据的很大一部分空间。神经突成束生长,穿过螺旋神经节细胞以前所在的罗森塔尔管,进入骨螺旋板,最终进入柯蒂氏器,在那里它们与毛细胞接触。神经元计数显示,与未进行后续干细胞移植而失神经支配的动物相比,感觉上皮附近的神经元突起显著增加。这些神经元的再生表明,从干细胞分化而来的神经元在神经元变性的动物模型中具有向特定靶点生长的能力。

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