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GAP-43 in the axons of mammalian CNS neurons regenerating into peripheral nerve grafts.

作者信息

Campbell G, Anderson P N, Turmaine M, Lieberman A R

机构信息

Department of Anatomy and Developmental Biology, University College London, UK.

出版信息

Exp Brain Res. 1991;87(1):67-74. doi: 10.1007/BF00228507.

DOI:10.1007/BF00228507
PMID:1836765
Abstract

Although mature mammalian CNS neurons do not normally regenerate axons after injury, it is well established that they will regrow axons over long distances into peripheral nerve implants. We have autografted segments of sciatic nerve into the brains of adult albino rats and have used light and electron microscopic immunocytochemistry to examine the distribution of the growth associated protein GAP-43 in and around the graft in the first two weeks following implantation. GAP-43 was present, 3-14 days after grafting, in small non-myelinated axonal sprouts in the brain parenchyma around the proximal tip of the graft. At 11-14 days after implantation similar sprouts within the graft itself were GAP-43 immunoreactive. The sprouts were either naked or associated with other cell processes (chiefly of Schwann cells; to a lesser extent of astrocytes). We also show that small numbers of neuronal perikarya around the tip of the graft become GAP-43 immunoreactive 11-14 days after implantation. Thus mature mammalian CNS neurons regenerating axons into a PNS graft display a marked increase in their content of GAP-43. In addition, we report that small plaques of GAP-43 reaction product are sometimes present on the plasma membranes of Schwann cells or astrocytes adjacent to immunoreactive axons, and that narrow sheet-like or filopodial processes of astrocytes, Schwann cells and possibly other non-neuronal cell types, may contain small amounts of GAP-43.

摘要

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本文引用的文献

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Reinnervation of peripheral nerve segments implanted into the rat central nervous system.植入大鼠中枢神经系统的周围神经节段的再支配
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Targeted overexpression of the neurite growth-associated protein B-50/GAP-43 in cerebellar Purkinje cells induces sprouting after axotomy but not axon regeneration into growth-permissive transplants.在小脑浦肯野细胞中靶向过表达神经突生长相关蛋白B-50/GAP-43可在轴突切断后诱导出芽,但不能诱导轴突再生进入允许生长的移植组织。
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