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神经细胞黏附分子刺激的神经突生长依赖于蛋白激酶C和Ras-丝裂原活化蛋白激酶途径的激活。

Neural cell adhesion molecule-stimulated neurite outgrowth depends on activation of protein kinase C and the Ras-mitogen-activated protein kinase pathway.

作者信息

Kolkova K, Novitskaya V, Pedersen N, Berezin V, Bock E

机构信息

Protein Laboratory, Institute of Molecular Pathology, University of Copenhagen, DK-2200, Copenhagen N, Denmark.

出版信息

J Neurosci. 2000 Mar 15;20(6):2238-46. doi: 10.1523/JNEUROSCI.20-06-02238.2000.

DOI:10.1523/JNEUROSCI.20-06-02238.2000

PMID:10704499

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6772508/

Abstract

The signal transduction pathways associated with neural cell adhesion molecule (NCAM)-induced neuritogenesis are only partially characterized. We here demonstrate that NCAM-induced neurite outgrowth depends on activation of p59(fyn), focal adhesion kinase (FAK), phospholipase Cgamma (PLCgamma), protein kinase C (PKC), and the Ras-mitogen-activated protein (MAP) kinase pathway. This was done using a coculture system consisting of PC12-E2 cells grown on fibroblasts, with or without NCAM expression, allowing NCAM-NCAM interactions resulting in neurite outgrowth. PC12-E2 cells were transiently transfected with expression plasmids encoding constitutively active forms of Ras, Raf, MAP kinase kinases MEK1 and 2, dominant negative forms of Ras and Raf, and the FAK-related nonkinase. Alternatively, PC12-E2 cells were submitted to treatment with antibodies to the fibroblast growth factor (FGF) receptor, inhibitors of the nonreceptor tyrosine kinase p59(fyn), PLC, PKC and MEK and an activator of PKC, phorbol-12-myristate-13-acetate (PMA). MEK2 transfection rescued cells treated with all inhibitors. The same was found for PMA treatment, except when cells concomitantly were treated with the MEK inhibitor. Arachidonic acid rescued cells treated with antibodies to the FGF receptor or the PLC inhibitor, but not cells in which the activity of PKC, p59(fyn), FAK, Ras, or MEK was inhibited. Interaction of NCAM with a synthetic NCAM peptide ligand, known to induce neurite outgrowth, was shown to stimulate phosphorylation of the MAP kinases extracellular signal-regulated kinases ERK1 and ERK2. The MAP kinase activation was sustained, because ERK1 and ERK2 were phosphorylated in PC12-E2 cells and primary hippocampal neurons even after 24 hr of cultivation on NCAM-expressing fibroblasts. Based on these results, we propose a model of NCAM signaling involving two pathways: NCAM-Ras-MAP kinase and NCAM-FGF receptor-PLCgamma-PKC, and we propose that PKC serves as the link between the two pathways activating Raf and thereby creating the sustained activity of the MAP kinases necessary for neuronal differentiation.

摘要

与神经细胞黏附分子（NCAM）诱导的神经突生长相关的信号转导通路仅得到部分表征。我们在此证明，NCAM诱导的神经突生长依赖于p59（fyn）、黏着斑激酶（FAK）、磷脂酶Cγ（PLCγ）、蛋白激酶C（PKC）以及Ras-丝裂原活化蛋白（MAP）激酶通路的激活。这是通过一种共培养系统完成的，该系统由在成纤维细胞上生长的PC12-E2细胞组成，有或没有NCAM表达，允许NCAM-NCAM相互作用导致神经突生长。PC12-E2细胞用编码Ras、Raf、MAP激酶激酶MEK1和MEK2的组成型活性形式、Ras和Raf的显性负性形式以及FAK相关非激酶的表达质粒进行瞬时转染。或者，PC12-E2细胞用针对成纤维细胞生长因子（FGF）受体的抗体、非受体酪氨酸激酶p59（fyn）、PLC、PKC和MEK的抑制剂以及PKC激活剂佛波醇-12-肉豆蔻酸酯-13-乙酸酯（PMA）进行处理。MEK2转染挽救了用所有抑制剂处理的细胞。PMA处理也得到了相同的结果，除非细胞同时用MEK抑制剂处理。花生四烯酸挽救了用针对FGF受体的抗体或PLC抑制剂处理的细胞，但不能挽救PKC、p59（fyn）、FAK、Ras或MEK活性被抑制的细胞。已知能诱导神经突生长的NCAM与合成NCAM肽配体的相互作用被证明能刺激MAP激酶细胞外信号调节激酶ERK1和ERK2的磷酸化。MAP激酶的激活是持续的，因为即使在表达NCAM的成纤维细胞上培养24小时后，PC12-E2细胞和原代海马神经元中的ERK1和ERK2仍被磷酸化。基于这些结果，我们提出了一个NCAM信号传导模型，涉及两条通路：NCAM-Ras-MAP激酶和NCAM-FGF受体-PLCγ-PKC，并且我们提出PKC作为两条通路之间的连接，激活Raf，从而产生神经元分化所需的MAP激酶的持续活性。

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神经细胞黏附分子刺激的神经突生长依赖于蛋白激酶C和Ras-丝裂原活化蛋白激酶途径的激活。

Neural cell adhesion molecule-stimulated neurite outgrowth depends on activation of protein kinase C and the Ras-mitogen-activated protein kinase pathway.

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