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大鼠和人类表皮生长因子反应性前体细胞移植到成年中枢神经系统损伤部位后的存活与分化

Survival and differentiation of rat and human epidermal growth factor-responsive precursor cells following grafting into the lesioned adult central nervous system.

作者信息

Svendsen C N, Clarke D J, Rosser A E, Dunnett S B

机构信息

MRC Cambridge Centre for Brain Repair, University of Cambridge, United Kingdom.

出版信息

Exp Neurol. 1996 Feb;137(2):376-88. doi: 10.1006/exnr.1996.0039.

Abstract

Epidermal Growth Factor (EGF)-responsive stem cells isolated from the developing central nervous system (CNS) can be expanded exponentially in culture while retaining the ability to differentiate into neurons and glia. As such, they represent a possible source of tissue for neural transplantation, providing they can survive and mature following grafting into the adult brain. In this study we have shown that purified rat stem cells generated from either the embryonic mesencephalon or the striatum can survive grafting into the striatum of rats with either ibotenic acid or nigrostriatal dopamine lesions. However, transplanted stem cells do not survive as a large mass typical of primary embryonic CNS tissue grafts, but in contrast form thin grafts containing only a small number of surviving cells. There was no extensive migration of transplanted stem cells labeled with either the lac-z gene or bromodeoxyuridine into the host region surrounding the graft, although a small number of labeled cells were seen in the ventral striatum some distance from the site of implantation. Some of these appeared to differentiate into dopamine neurons, particularly when the developing mesencephalon was used as the starting material for generating the stem cells. EGF-responsive stem cells could also be isolated from the mesencephalon of developing human embryos and expanded in culture, but only grew in large numbers when the gestational age of the embryo was greater than 11 weeks. Purified human CNS stem cells were also transplanted into immunosuppressed rats with nigrostriatal lesions and formed thin grafts similar to those seen when using rat stem cells. However, when primary cultures of human mesencephalon were grown with EGF for only 10 days and this mixture of stem cells and primary neural tissue was transplanted into the dopamine-depleted striatum, large well-formed grafts developed. These contained mostly small undifferentiated cells intermixed with a number of well-differentiated TH-positive neurons. These results show that purified populations of rat or human EGF-responsive CNS stem cells do not form large graft masses or migrate extensively into the surrounding host tissues when transplanted into the adult striatum. However, modifications of the growth conditions in vitro may lead to an improvement of their survival in vivo.

摘要

从发育中的中枢神经系统(CNS)分离出的表皮生长因子(EGF)反应性干细胞,在培养中可呈指数级扩增,同时保留分化为神经元和神经胶质细胞的能力。因此,倘若它们在移植到成年大脑后能够存活并成熟,那么它们就代表了一种神经移植的潜在组织来源。在本研究中,我们已经表明,从胚胎中脑或纹状体产生的纯化大鼠干细胞,在移植到用鹅膏蕈氨酸或黑质纹状体多巴胺损伤的大鼠纹状体后能够存活。然而,移植的干细胞并不像典型的原发性胚胎中枢神经系统组织移植那样形成大量的团块,而是形成仅含有少量存活细胞的薄移植体。用lac - z基因或溴脱氧尿苷标记的移植干细胞,并没有广泛迁移到移植体周围的宿主区域,尽管在距植入部位一定距离的腹侧纹状体中可见少量标记细胞。其中一些细胞似乎分化为多巴胺神经元,特别是当发育中的中脑用作产生干细胞的起始材料时。EGF反应性干细胞也可以从发育中的人类胚胎中脑分离出来并在培养中扩增,但只有当胚胎的孕周大于11周时才能大量生长。纯化的人类中枢神经系统干细胞也被移植到患有黑质纹状体损伤的免疫抑制大鼠中,并形成了类似于使用大鼠干细胞时所见的薄移植体。然而,当人类中脑的原代培养物仅用EGF培养10天,并且这种干细胞和原代神经组织的混合物被移植到多巴胺缺乏的纹状体中时,就会形成发育良好的大移植体。这些移植体主要包含小的未分化细胞,并与一些分化良好的TH阳性神经元混合在一起。这些结果表明,纯化的大鼠或人类EGF反应性中枢神经系统干细胞群体在移植到成年纹状体后,不会形成大的移植团块,也不会广泛迁移到周围的宿主组织中。然而,体外生长条件的改变可能会提高它们在体内的存活率。

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