| Literature DB >> 29590626 |
Jian-Hua Zhang1, Yi-Fei Zhao1, Xiao-Xiao He1, Yang Zhao1, Zi-Xuan He1, Lei Zhang2, Ying Huang2, Yu-Bing Wang2, Ling Hu2, Lin Liu1, Hua-Li Yu1, Jia-Hui Xu1, Ming-Ming Lai1, Dong-Dong Zhao1, Lei Cui1, Wei-Xiang Guo3, Wen-Cheng Xiong4, Yu-Qiang Ding5, Xiao-Juan Zhu6.
Abstract
Newborn neurons undergo inside-out migration to their final destinations during neocortical development. Reelin-induced tyrosine phosphorylation of disabled 1 (Dab1) is a critical mechanism controlling cortical neuron migration. However, the roles of Reelin-independent phosphorylation of Dab1 remain unclear. Here, we report that deleted in colorectal carcinoma (DCC) interacts with Dab1 via its P3 domain. Netrin 1, a DCC ligand, induces Dab1 phosphorylation at Y220 and Y232. Interestingly, knockdown of DCC or truncation of its P3 domain dramatically delays neuronal migration and impairs the multipolar-to-bipolar transition of migrating neurons. Notably, the migration delay and morphological transition defects are rescued by the expression of a phospho-mimetic Dab1 or a constitutively active form of Fyn proto-oncogene (Fyn), a member of the Src-family tyrosine kinases that effectively induces Dab1 phosphorylation. Collectively, these findings illustrate a DCC-Dab1 interaction that ensures proper neuronal migration during neocortical development.Entities:
Keywords: DCC; Dab1; Fyn; Reelin; morphological transition; neocortex development; netrin 1; neuronal migration; tyrosine phosphorylation
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Year: 2018 PMID: 29590626 DOI: 10.1016/j.celrep.2018.03.005
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423