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神经元神经调节蛋白 1 型 III 指导施万细胞迁移。

Neuronal Neuregulin 1 type III directs Schwann cell migration.

机构信息

Department of Developmental Biology, 279 Campus Dr., Beckman Center B300, Stanford University, Stanford, CA 94305, USA.

出版信息

Development. 2011 Nov;138(21):4639-48. doi: 10.1242/dev.068072. Epub 2011 Sep 28.

Abstract

During peripheral nerve development, each segment of a myelinated axon is matched with a single Schwann cell. Tight regulation of Schwann cell movement, proliferation and differentiation is essential to ensure that these glial cells properly associate with axons. ErbB receptors are required for Schwann cell migration, but the operative ligand and its mechanism of action have remained unknown. We demonstrate that zebrafish Neuregulin 1 (Nrg1) type III, which signals through ErbB receptors, controls Schwann cell migration in addition to its previously known roles in proliferation and myelination. Chimera analyses indicate that ErbB receptors are required in all migrating Schwann cells, and that Nrg1 type III is required in neurons for migration. Surprisingly, expression of the ligand in a few axons is sufficient to induce migration along a chimeric nerve constituted largely of nrg1 type III mutant axons. These studies also reveal a mechanism that allows Schwann cells to fasciculate axons regardless of nrg1 type III expression. Time-lapse imaging of transgenic embryos demonstrated that misexpression of human NRG1 type III results in ectopic Schwann cell migration, allowing them to aberrantly enter the central nervous system. These results demonstrate that Nrg1 type III is an essential signal that controls Schwann cell migration to ensure that these glia are present in the correct numbers and positions in developing nerves.

摘要

在周围神经发育过程中,每个有髓轴突的节段都与单个施万细胞匹配。施万细胞的运动、增殖和分化受到严格调控,以确保这些神经胶质细胞与轴突正确结合。ErbB 受体是施万细胞迁移所必需的,但操作配体及其作用机制仍不清楚。我们证明,斑马鱼神经调节蛋白 1(Nrg1)III 型通过 ErbB 受体信号转导,除了其先前在增殖和髓鞘形成中的已知作用外,还控制施万细胞的迁移。嵌合体分析表明,ErbB 受体在所有迁移的施万细胞中都需要,并且 Nrg1 型 III 在神经元中迁移是必需的。令人惊讶的是,在几条轴突中表达配体足以诱导沿着主要由 nrg1 型 III 突变轴突组成的嵌合神经的迁移。这些研究还揭示了一种机制,允许施万细胞无论 Nrg1 型 III 的表达如何,都能聚集轴突。转染胚胎的延时成像显示,人 NRG1 型 III 的异位表达导致施万细胞的异位迁移,使它们能够异常进入中枢神经系统。这些结果表明,Nrg1 型 III 是一种必不可少的信号,它控制施万细胞的迁移,以确保这些神经胶质细胞在发育中的神经中以正确的数量和位置存在。

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