首页> 美国卫生研究院文献>The Journal of Biological Chemistry >LINGO-1 Interacts with WNK1 to Regulate Nogo-induced Inhibition of Neurite Extension
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LINGO-1 Interacts with WNK1 to Regulate Nogo-induced Inhibition of Neurite Extension

机译:LINGO-1与WNK1相互作用以调节Nogo诱导的神经突延伸抑制。

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摘要

LINGO-1 is a component of the tripartite receptor complexes, which act as a convergent mediator of the intracellular signaling in response to myelin-associated inhibitors and lead to collapse of growth cone and inhibition of neurite extension. Although the function of LINGO-1 has been intensively studied, its downstream signaling remains elusive. In the present study, a novel interaction between LINGO-1 and a serine-threonine kinase WNK1 was identified by yeast two-hybrid screen. The interaction was further validated by fluorescence resonance energy transfer and co-immunoprecipitation, and this interaction was intensified by Nogo66 treatment. Morphological evidences showed that WNK1 and LINGO-1 were co-localized in cortical neurons. Furthermore, either suppressing WNK1 expression by RNA interference or overexpression of WNK1-(123–510) attenuated Nogo66-induced inhibition of neurite extension and inhibited the activation of RhoA. Moreover, WNK1 was identified to interact with Rho-GDI1, and this interaction was attenuated by Nogo66 treatment, further indicating its regulatory effect on RhoA activation. Taken together, our results suggest that WNK1 is a novel signaling molecule involved in regulation of LINGO-1 mediated inhibition of neurite extension.
机译:LINGO-1是三方受体复合物的一个组成部分,可作为细胞内信号传导的聚合介质,响应于髓磷脂相关抑制剂,导致生长锥塌陷并抑制神经突延伸。尽管已对LINGO-1的功能进行了深入研究,但其下游信号传导仍然难以捉摸。在本研究中,通过酵母双杂交筛选鉴定了LINGO-1和丝氨酸-苏氨酸激酶WNK1之间的新型相互作用。通过荧光共振能量转移和免疫共沉淀进一步验证了这种相互作用,并且通过Nogo66处理增强了这种相互作用。形态学证据表明,WNK1和LINGO-1共同位于皮质神经元中。此外,通过RNA干扰抑制WNK1表达或WNK1-(123-510)的过表达减弱了Nogo66诱导的神经突延伸抑制,并抑制了RhoA的激活。此外,已确定WNK1与Rho-GDI1相互作用,并且该相互作用被Nogo66处理减弱,进一步表明其对RhoA激活的调节作用。两者合计,我们的结果表明,WNK1是一种新型信号分子,参与调控LINGO-1介导的神经突扩展抑制。

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