RhoB and Actin Polymerization Coordinate Src Activation with Endosome-Mediated Delivery to the Membrane

We have used a c-Src-GFP fusion protein to address the spatial control of Src activation and the nature of Src-associated intracellular structures during stimulus-induced transit to the membrane. Src is activated during transit, particularly in RhoB-containing cytoplasmic endosomes associated with t...

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Veröffentlicht in:Developmental cell 2004-12, Vol.7 (6), p.855-869
Hauptverfasser: Sandilands, Emma, Cans, Christophe, Fincham, Valerie J., Brunton, Valerie G., Mellor, Harry, Prendergast, George C., Norman, Jim C., Superti-Furga, Giulio, Frame, Margaret C.
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Sprache:eng
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Zusammenfassung:We have used a c-Src-GFP fusion protein to address the spatial control of Src activation and the nature of Src-associated intracellular structures during stimulus-induced transit to the membrane. Src is activated during transit, particularly in RhoB-containing cytoplasmic endosomes associated with the perinuclear recycling compartment. Knocking out RhoB or expressing a dominant-interfering Rab11 mutant suppresses both catalytic activation of Src and translocation of active kinase to peripheral membrane structures. In addition, the Src- and RhoB-containing endosomes harbor proteins involved in actin polymerization and filament assembly, for example Scar1, and newly polymerized actin can associate with these endosomes in a Src-dependent manner. This implies that Src may regulate an endosome-associated actin nucleation activity. In keeping with this, Src controls the actin dependence of RhoB endosome movement toward the plasma membrane. This work identifies RhoB as a component of “outside-in” signaling pathways that coordinate Src activation with translocation to transmembrane receptors.
ISSN:1534-5807
1878-1551
DOI:10.1016/j.devcel.2004.09.019