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. 2014 Jan 15;127(Pt 2):328-40.
doi: 10.1242/jcs.130161. Epub 2013 Nov 8.

Spire-1 contributes to the invadosome and its associated invasive properties

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Spire-1 contributes to the invadosome and its associated invasive properties

Vanessa Lagal et al. J Cell Sci. .

Abstract

Cancer cells have an increased ability to squeeze through extracellular matrix gaps that they create by promoting proteolysis of its components. Major sites of degradation are specialized micro-domains in the plasma membrane collectively named invadosomes where the Arp2/3 complex and formin proteins cooperate to spatio-temporally control actin nucleation and the folding of a dynamic F-actin core. At invadosomes, proper coupling of exo-endocytosis allows polarized delivery of proteases that facilitate degradation of ECM and disruption of the cellular barrier. We investigated the contribution of the actin nucleator Spire-1 to invadosome structure and function, using Src-activated cells and cancer cells. We found that Spire-1 is specifically recruited at invadosomes and is part of a multi-molecular complex containing Src kinase, the formin mDia1 and actin. Spire-1 interacts with the Rab3A GTPase, a key player in the regulation of exocytosis that is present at invadosomes. Finally, over- and under-expression of Spire-1 resulted in cells with an increased or decreased potential for matrix degradation, respectively, therefore suggesting a functional interplay of Spire-1 with both actin nucleation and vesicular trafficking that might impact on cell invasive and metastatic behavior.

Keywords: Actin; Endothelial transmigration; Gelatin invasion; Invadosome; Spire-1; Src-activated 3T3; Vesicular trafficking.

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