| Literature DB >> 25358863 |
Fumio Nakamura1, Kosuke Kumeta1, Tomonobu Hida1, Toshinari Isono2, Yuichi Nakayama1, Emiko Kuramata-Matsuoka1, Naoya Yamashita1, Yutaka Uchida1, Ken-ichi Ogura1, Keiko Gengyo-Ando3, Shohei Mitani3, Toshio Ogino4, Yoshio Goshima1.
Abstract
Reorganization of the actin cytoskeleton is an early cellular response to various extracellular signals. Sema3A, a repulsive axon guidance molecule, induces the reorganization of actin cytoskeleton in the growth cones. Collapsin response mediator protein 1 (CRMP1) mediates the intracellular Sema3A signalling through its Ser522 phosphorylation. Here we show that UNC-33, CRMP1 C. elegans homologue, interacts with FLN-1, an actin-binding Filamin-A orthologue. In nematodes, this interaction participates in the projection of DD/VD motor neurons. CRMP1 binds both the actin-binding domain and the last immunoglobulin-like repeat of Filamin-A. The alanine mutants of Filamin-A or CRMP1 in their interacting residues suppress the Sema3A repulsion in neurons. Conversely, a phosphor-mimicking mutant CRMP1(Ser522Asp) enhances the Sema3A response. Atomic-force microscopy analysis reveals that the V-shaped Filamin-A changes to a condensed form with CRMP1(Ser522Asp). CRMP1(Ser522Asp) weakens the F-actin gelation crosslinked by Filamin-A. Thus, phosphorylated CRMP1 may remove Filamin-A from the actin cytoskeleton to facilitate its remodelling.Entities:
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Year: 2014 PMID: 25358863 DOI: 10.1038/ncomms6325
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919