The Toca-1-N-WASP Complex Links Filopodial Formation to Endocytosis

Artigo Acesso aberto Revisado por pares

The Toca-1-N-WASP Complex Links Filopodial Formation to Endocytosis

2009; Elsevier BV; Volume: 284; Issue: 17 Linguagem: Inglês

10.1074/jbc.m805940200

ISSN

1083-351X

Autores

Wenyu Bu, Amy Chou, Kim Buay Lim, Thankiah Sudhaharan, Sohail Ahmed,

Tópico(s)

Cellular transport and secretion

Resumo

The transducer of Cdc42-dependent actin assembly (Toca-1)-N-WASP complex was isolated as an essential cofactor for Cdc42-driven actin polymerization in vitro. Toca-1 consists of an N-terminal F-BAR domain, followed by a Cdc42 binding site (HR1 domain) and an SH3 domain, (the N-WASP interacting site). N-WASP is an activator of actin nucleation through the Arp2/3 complex. The aim of the present study was to investigate the cellular function of the Toca-1-N-WASP complex. We report that Toca-1 induces filopodia and neurites as does N-WASP in N1E115 neuroblastoma cells. Toca-1 requires the F-BAR domain, Cdc42 binding site, and SH3 domain to induce filopodia. Toca-1 and N-WASP both require each other to induce filopodia. The expression of Toca-1 and N-WASP affects the distribution, size, and number of Rab5 positive membranes. Toca-1 interacts directly with N-WASP in filopodia and Rab5 membrane as seen by Forster resonance energy transfer. Thus the Toca-1-N-WASP complex localizes to and induces the formation of filopodia and endocytic vesicles. Last, three inhibitors of endocytosis, Dynamin-K44A, Eps15Delta95/295, and clathrin heavy chain RNA interference, block Toca-1-induced filopodial formation. Taken together, these data suggest that the Toca-1-N-WASP complex can link filopodial formation to endocytosis.

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The Toca-1-N-WASP Complex Links Filopodial Formation to Endocytosis