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切断轴突的周围神经的施万细胞中神经生长因子受体的表达:超微结构定位、轴突接触的抑制作用及结合特性

Expression of nerve growth factor receptors by Schwann cells of axotomized peripheral nerves: ultrastructural location, suppression by axonal contact, and binding properties.

作者信息

Taniuchi M, Clark H B, Schweitzer J B, Johnson E M

机构信息

Department of Pharmacology, Washington University School of Medicine, St. Louis, Missouri 63110.

出版信息

J Neurosci. 1988 Feb;8(2):664-81. doi: 10.1523/JNEUROSCI.08-02-00664.1988.

Abstract

Axotomy of sciatic nerve fibers in adult rats induces expression of NGF receptor in the entire population of Schwann cells located distal to the injury (Taniuchi et al., 1986b). In the present study we have used immunocytochemistry, with a monoclonal antibody directed against the rat NGF receptor, to examine axotomized peripheral nerves by light and electron microscopy. We have found that (1) the NGF receptor molecules were localized to the cell surface of Schwann cells forming bands of Bungner; (2) axonal regeneration into the distal portion of sciatic nerve coincided temporally and spatially with a decrease in Schwann cell expression of NGF receptor; (3) Schwann cell NGF receptor could be induced by axotomy of NGF-independent neurons, such as motoneurons and parasympathetic neurons; and (4) the presence of axon-Schwann cell contact was inversely related to expression of Schwann cell NGF receptor. Using biochemical assays we have found that, in striking contrast to peripheral nerves, there was no detectable induction of NGF receptor in the spinal cord and brain after axotomy of NGF receptor-bearing fibers. Filtration assays of 125I-NGF binding to the induced NGF receptors of Schwann cells measured a Kd of 1.5 nM and a fast dissociation rate, both characteristics of class II receptor sites. We conclude that Wallerian degeneration induces Schwann cells, but not central neuroglia, to produce and position upon their plasmalemmal surface the class II NGF receptor molecules. The induction is ubiquitous among Schwann cells, irrespective of the type of axon they originally ensheathed. Expression of Schwann cell NGF receptor is negatively regulated by axonal contact, being induced when axons degenerate and suppressed when regenerating axons grow out along the Schwann cell surface. We propose that the induced NGF receptors function to bind NGF molecules upon the Schwann cell surface and thereby provide a substratum laden with trophic support and chemotactic guidance for regenerating sensory and sympathetic neurons.

摘要

成年大鼠坐骨神经纤维切断术可诱导损伤部位远端所有雪旺细胞表达神经生长因子(NGF)受体(谷内等人,1986b)。在本研究中,我们使用免疫细胞化学方法,用一种针对大鼠NGF受体的单克隆抗体,通过光学显微镜和电子显微镜检查切断轴突的周围神经。我们发现:(1)NGF受体分子定位于形成郎飞结带的雪旺细胞的细胞表面;(2)坐骨神经远端部分的轴突再生在时间和空间上与雪旺细胞NGF受体表达的减少相吻合;(3)雪旺细胞NGF受体可由与NGF无关的神经元(如运动神经元和副交感神经元)的轴突切断术诱导产生;(4)轴突与雪旺细胞的接触与雪旺细胞NGF受体的表达呈负相关。通过生化分析我们发现,与周围神经形成鲜明对比的是,切断携带NGF受体的纤维后,脊髓和脑中未检测到NGF受体的诱导。对结合到雪旺细胞诱导的NGF受体上的125I-NGF进行过滤分析,测得解离常数(Kd)为1.5 nM,解离速率快,这是II类受体位点的两个特征。我们得出结论,沃勒变性诱导雪旺细胞而非中枢神经胶质细胞在其质膜表面产生并定位II类NGF受体分子。这种诱导在所有雪旺细胞中普遍存在,无论它们最初包裹的轴突类型如何。雪旺细胞NGF受体的表达受轴突接触的负调节,当轴突退化时被诱导,而当再生轴突沿着雪旺细胞表面生长时被抑制。我们认为,诱导产生的NGF受体的功能是在雪旺细胞表面结合NGF分子,从而为再生的感觉神经元和交感神经元提供富含营养支持和趋化引导的基质。

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