4.6 Article

Gβ5γ2 is a highly selective activator of phospholipid-dependent enzymes

Journal

JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 275, Issue 18, Pages 13746-13754

Publisher

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.275.18.13746

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In this study, G beta specificity in the regulation of G beta gamma-sensitive phosphoinositide 3-kinases (PI3Ks) and phospholipase C beta (PLC beta) isozymes was examined. Recombinant mammalian G beta(1-3)gamma(2) complexes purified from Sf9 membranes stimulated PI3K gamma lipid kinase activity with similar potency (10-30 nM) and efficacy, whereas transducin G beta gamma was less potent. Functionally active G beta(5)gamma(2) dimers were purified from Sf9 cell membranes following coexpression of G beta(5) and G gamma(2-His). This preparation as well as G beta(1)gamma(2-His) supported pertussis toxin-mediated ADP-ribosylation of G alpha(i1) G beta(1)gamma(2-His) Stimulated PI3K gamma lipid and protein kinase activities at nanomolar concentrations, whereas G beta(5)gamma(2-His) had no effect. Accordingly, G beta(1)gamma(2-His), but not G beta(5)gamma(2-His), significantly stimulated the lipid kinase activity of PI3K beta in the presence or absence of tyrosine-phosphorylated peptides derived from the p85-binding domain of the platelet derived-growth factor receptor. Conversely, both preparations were able to stimulate PLC beta(2) and PLC beta(1). However, G beta(1)gamma(2-His) but not G beta(5)gamma(2-His), activated PLC beta(3). Experimental evidence suggests that the mechanism of G beta(5)-dependent effector selectivity may differ between PI3K and PLC beta. In conclusion, these data indicate that G beta subunits are able to discriminate among effecters independently of G alpha due to selective protein-protein interaction.

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