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施万细胞与哺乳动物中枢神经系统轴突的再生:大鼠视觉系统移植研究综述

Schwann cells and the regrowth of axons in the mammalian CNS: a review of transplantation studies in the rat visual system.

作者信息

Harvey A R, Plant G W, Tan M M

机构信息

Department of Anatomy and Human Biology, The University of Western Australia, Nedlands, Perth, Australia.

出版信息

Clin Exp Pharmacol Physiol. 1995 Aug;22(8):569-79. doi: 10.1111/j.1440-1681.1995.tb02068.x.

Abstract
  1. We have used peripheral nerve transplants or cultured Schwann cells grafted in association with different types of polymer to study axonal regrowth in the rat visual system. In some instances the glia were co-grafted with fetal tectal tissue. 2. The studies have two main aims: (i) to determine whether retinal axons can be induced to regrow at a site distant from their cell soma, that is, after damage to the brachial region of the optic tract; (ii) to determine whether retinal axons exposed to Schwann cells retain the ability to recognize their appropriate target neurons in CNS tissue. 3. In brachial lesion studies, Schwann cells were placed in the lesion site in association with nitrocellulose papers, within polycarbonate tubes in the presence or absence of a supporting extracellular matrix (ECM), or within polymer hydrogel scaffolds. Autologous sciatic nerve grafts were also used. Immunohistochemical studies revealed the presence of regenerating axons within all polymer bridges. Regrowth of retinal axons was also seen, however, growth was not extensive and was limited to the proximal 1-1.5 mm of the implants. 4. In target innervation experiments, two surgical paradigms were developed. In one experiment, a segment of sciatic nerve was autografted onto the transected optic nerve in adult rats and the distal end of each graft was placed adjacent to fetal tectal (target) tissue implanted into the frontal cortex. To date, we have not been able to demonstrate selective recognition of target regions within tectal transplants by retinal axons exiting the sciatic nerve implants. 5. In the second experiment, Schwann cells were mixed with fetal tectal cells and co-grafted to the midbrain of newborn host rats. Schwann cells altered the characteristic pattern of host retinal growth into tectal grafts; in some cases axons were induced to grow away from appropriate target areas by nearby co-grafted Schwann cells. 6. In summary, Schwann cell/polymer scaffolds may provide a useful way of promoting the regrowth of damaged axons in the CNS, however: (i) in adults, at least, their effectiveness is reduced if they are located at a distance from the cell bodies giving rise to regenerating axons; (ii) in some circumstances exposure to a peripheral glial environment may affect the capacity of regenerating axons to recognize appropriate target cells in the CNS neuropil.
摘要
  1. 我们已使用周围神经移植或与不同类型聚合物联合移植的培养雪旺细胞,来研究大鼠视觉系统中的轴突再生。在某些情况下,神经胶质细胞与胎儿顶盖组织共同移植。2. 这些研究有两个主要目的:(i)确定视网膜轴突在远离其细胞体的部位,即在视神经臂部区域受损后,是否能被诱导再生;(ii)确定接触雪旺细胞的视网膜轴突是否保留识别中枢神经系统组织中合适靶神经元的能力。3. 在臂部损伤研究中,将雪旺细胞与硝酸纤维素纸一起置于损伤部位,或置于有或无支持性细胞外基质(ECM)的聚碳酸酯管内,或置于聚合物水凝胶支架内。也使用了自体坐骨神经移植。免疫组织化学研究显示所有聚合物桥内均有再生轴突。也观察到了视网膜轴突的再生,然而,生长并不广泛,仅限于植入物近端1 - 1.5毫米处。4. 在靶神经支配实验中,开发了两种手术范式。在一个实验中,将一段坐骨神经自体移植到成年大鼠横断的视神经上,并将每个移植体的远端置于植入额叶皮质的胎儿顶盖(靶)组织附近。迄今为止,我们尚未能够证明离开坐骨神经移植体的视网膜轴突能选择性识别顶盖移植体内的靶区域。5. 在第二个实验中,将雪旺细胞与胎儿顶盖细胞混合,共同移植到新生宿主大鼠的中脑。雪旺细胞改变了宿主视网膜向顶盖移植体生长的特征模式;在某些情况下,附近共同移植的雪旺细胞会诱导轴突从合适的靶区域生长离开。6. 总之,雪旺细胞/聚合物支架可能为促进中枢神经系统中受损轴突的再生提供一种有用的方法,然而:(i)至少在成体中,如果它们距离产生再生轴突的细胞体较远,其有效性会降低;(ii)在某些情况下,暴露于外周神经胶质环境可能会影响再生轴突识别中枢神经系统神经毡中合适靶细胞的能力。

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