Activation of Ras in vitro and in intact fibroblasts by the Vav guanine nucleotide exchange protein.

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Mol Cell Biol. 1994 February; 14(2): 906-913

Activation of Ras in vitro and in intact fibroblasts by the Vav guanine nucleotide exchange protein.

E Gulbins, K M Coggeshall, C Langlet, G Baier, N Bonnefoy-Berard, P Burn, A Wittinghofer, S Katzav and A Altman

Division of Cell Biology, La Jolla Institute for Allergy and Immunology, California 92037.

ABSTRACT

We recently identified Vav, the product of the vav proto-oncogene,as a guanine nucleotide exchange factor (GEF) for Ras. Vav isenzymatically activated by lymphocyte antigen receptor-coupledprotein tyrosine kinases or independently by diglycerides. Tofurther evaluate the physiological role of Vav, we assessedits GDP-GTP exchange activity against several Ras-related proteinsin vitro and determined whether Vav activation in transfectedNIH 3T3 fibroblasts correlates with the activity status of Rasand mitogen-activated protein (MAP) kinases. In vitro translatedpurified Vav activated by phorbol myristate acetate (PMA) orphosphorylation with recombinant p56lck displayed GEF activityagainst Ras but not against recombinant RacI, RacII, Ral, orRhoA proteins. Expression of vav or proto-vav in stably transfectedNIH 3T3 cells led to a approximately 10-fold increase in basalor PMA-stimulated Ras exchange activity, respectively, in total-celllysates and Vav immunoprecipitates. Elevated GEF activity wasparalleled in each case by a significant increase in the proportionof active, GTP-bound Ras. PMA had a minimal effect on the lowRas. GTP level in untransfected control fibroblasts but increasedit from 20 to 37% in proto-vav-transfected cells. vav-transfectedcells displayed a constitutively elevated Ras. GTP level (35%),which was not increased further by PMA treatment. MAP kinases,known downstream intermediates in Ras-dependent signaling pathways,similarly exhibited increased basal or PMA-stimulated activityin Vav-expressing cells by comparison with normal NIH 3T3 cells.These results demonstrate a physiologic interaction betweenVav and its target, Ras, leading to MAP kinase activation.

Mol Cell Biol. 1994 February; 14(2): 906-913

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