Literature DB >> 32753482

Delineation of molecular determinants for FR900359 inhibition of Gq/11 unlocks inhibition of Gαs.

Michael W Boesgaard1, Kasper Harpsøe1, Michelle Malmberg1, Christina R Underwood1, Asuka Inoue2, Jesper M Mathiesen1, Gabriele M König3, Evi Kostenis4, David E Gloriam5, Hans Bräuner-Osborne6.   

Abstract

Heterotrimeric G proteins are essential mediators of intracellular signaling of G protein-coupled receptors. The Gq/11 subfamily consists of Gq, G11, G14, and G16 proteins, of which all but G16 are inhibited by the structurally related natural products YM-254890 and FR900359. These inhibitors act by preventing the GDP/GTP exchange, which is necessary for activation of all G proteins. A homologous putative binding site for YM-254890/FR900359 can also be found in members of the other three G protein families, Gs, Gi/o, and G12/13, but none of the published analogs of YM-254890/FR900359 have shown any inhibitory activity for any of these. To explain why the YM-254890/FR900359 scaffold only inhibits Gq/11/14, the present study delineated the molecular selectivity determinants by exchanging amino acid residues in the YM-254890/FR900359-binding site in Gq and Gs We found that the activity of a Gs mutant with a Gq-like binding site for YM-254890/FR900359 can be inhibited by FR900359, and a minimum of three mutations are necessary to introduce inhibition in Gs In all, this suggests that although the YM-254890/FR900359 scaffold has proven unsuccessful to derive Gs, Gi/o, and G12/13 inhibitors, the mechanism of inhibition between families of G proteins is conserved, opening up the possibility of targeting by other, novel inhibitor scaffolds. In lack of a selective Gαs inhibitor, FR900359-sensitive Gαs mutants may prove useful in studies where delicate control over Gαs signaling would be of the essence.
© 2020 Boesgaard et al.

Entities:  

Keywords:  FR900359; G protein; G protein inhibitor; G protein-coupled receptor (GPCR); Gq; Gs; YM-254890; inhibitor; molecular pharmacology; site-directed mutagenesis

Mesh:

Substances:

Year:  2020        PMID: 32753482      PMCID: PMC7535923          DOI: 10.1074/jbc.RA120.013002

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  51 in total

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