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移植到正常和经X射线照射的成年白质中的施万细胞不会广泛迁移,并且长期存活率较低。

Schwann cells transplanted into normal and X-irradiated adult white matter do not migrate extensively and show poor long-term survival.

作者信息

Iwashita Y, Fawcett J W, Crang A J, Franklin R J, Blakemore W F

机构信息

Department of Clinical Veterinary Medicine, University of Cambridge, Madingley Road, Cambridge, CB3 0ES, United Kingdom.

出版信息

Exp Neurol. 2000 Aug;164(2):292-302. doi: 10.1006/exnr.2000.7440.

Abstract

Although Schwann cells are able to enter the central nervous system (CNS) when the integrity of the glia limitans is disrupted, their ability to migrate through intact CNS remains unclear. We have addressed this issue by transplanting lacZ-labeled Schwann cells into normal adult spinal cord white matter, and into X-irradiated spinal cord (an environment that, unlike normal spinal cord, permits the migration of transplanted oligodendrocyte progenitors). Schwann cell cultures, obtained from neonatal rat sciatic nerve and expanded using bovine pituitary extract and forskolin, were transfected by repeated exposure to retroviral vectors encoding the Escherichia coli lacZ gene. The normal behavior of the transduced cells was confirmed by transplantation into a nonrepairing area of demyelination in the spinal cord, where they formed myelin sheaths around demyelinated axons. A single microliter containing 4 x 10(4) cells was then transplanted into unlesioned normal and X-irradiated white matter of the spinal cord of adult syngeneic rats. One hour after injection, blue cells were observed as a discrete mass within the dorsal funiculus with a longitudinal distribution of 2-3 mm, indicating the extent of passive spread of the injected cells. At subsequent survival times (1, 2, and 4 weeks posttransplantation) blue cells had a distribution that was no more extensive than that seen 1 h after transplantation. However, the number of Schwann cells declined with time following transplantation such that at 4 weeks there were few surviving Schwann cells in both X-irradiated and nonirradiated spinal cord. These results indicate that transplanted Schwann cells do not migrate extensively and show poor long-term survival when introduced into a normal CNS environment.

摘要

尽管当神经胶质界膜完整性被破坏时施万细胞能够进入中枢神经系统(CNS),但其在完整的中枢神经系统中迁移的能力仍不清楚。我们通过将用β-半乳糖苷酶(lacZ)标记的施万细胞移植到正常成年脊髓白质以及经X射线照射的脊髓(与正常脊髓不同,该环境允许移植的少突胶质前体细胞迁移)中来解决这个问题。从新生大鼠坐骨神经获得并使用牛垂体提取物和福司可林进行扩增的施万细胞培养物,通过反复暴露于编码大肠杆菌lacZ基因的逆转录病毒载体进行转染。将转导细胞移植到脊髓脱髓鞘的非修复区域,在那里它们围绕脱髓鞘轴突形成髓鞘,从而证实了转导细胞的正常行为。然后将含有4×10⁴个细胞的1微升细胞悬液移植到同基因成年大鼠脊髓未受损的正常和经X射线照射的白质中。注射后1小时,在背侧索内观察到蓝色细胞形成一个离散的团块,纵向分布为2 - 3毫米,表明注射细胞的被动扩散范围。在随后的存活时间(移植后1、2和4周),蓝色细胞的分布范围并不比移植后1小时观察到的更广泛。然而,移植后施万细胞的数量随时间减少,以至于在4周时,经X射线照射和未照射的脊髓中存活的施万细胞都很少。这些结果表明,当引入正常中枢神经系统环境时,移植的施万细胞不会广泛迁移,并且长期存活率很低。

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