4.5 Review

CRMP2: Functional Roles in Neural Development and Therapeutic Potential in Neurological Diseases

期刊

NEUROSCIENTIST
卷 20, 期 6, 页码 589-598

出版社

SAGE PUBLICATIONS INC
DOI: 10.1177/1073858413514278

关键词

neuronal polarization; microtubule; neuronal migration; cortex development; neurological disease

资金

  1. Research Grants Council of Hong Kong [HKUST660110, 660610, 660810, 660711, 661111, 661212, T13-607/12R]
  2. National Key Basic Research Program of China [2013CB530900]
  3. Innovation and Technology Fund for State Key Laboratory [ITCPT/17-9]
  4. Shenzhen Peacock Plan
  5. S.H. Ho Foundation

向作者/读者索取更多资源

Cytoskeletal restructuring is essential for nearly all cellular processes in the developing brain. After cell fate determination, newborn cortical neurons must migrate to their final positions while establishing proper axon-dendrite polarity. Significant progress has recently been made towards understanding the cellular and molecular mechanisms underlying neuronal polarization in vivo. Collapsin response mediator protein 2 (CRMP2) has long been identified as a microtubule-binding protein that regulates neuronal polarity in vitro. Recent studies provide new insights into the roles of CRMP2 in neuronal migration and subsequent neuronal differentiation. Both the expression and activity of CRMP2 are tightly regulated during cortex development. CRMP2 is suggested to be important in the multipolar-bipolar transition in radial migration. The increasing number of known interaction partners indicates that CRMP2 has functions beyond cytoskeletal regulation, including axonal transport, vesicle trafficking, and neurotransmitter release. This review discusses the current knowledge about CRMP2 in the context of neuronal development and highlights a recent emerging theme regarding its potential therapeutic applications.

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