The N-terminal extension of Gα(q) is critical for constraining the selectivity of receptor coupling

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Abstract

Characteristically, an individual member of the superfamily of G protein-coupled receptors can interact only with a limited number of the many structurally closely related G protein heterotrimers that are expressed within a cell. Interestingly, the N termini of two G protein α subunits, Gα(q) and Gα11, differ from those of other α subunits in that they display a unique, highly conserved six-amino acid extension. To test the hypothesis that this sequence element is critical for proper receptor recognition, we prepared a Gα(q) deletion mutant (-6q) lacking these first six amino acids. The -6q construct (or wild type Gα(q) as a control) was coexpressed (in COS-7 cells) with several different G(i/o) or G(s)-coupled receptors, and ligand-induced increases in inositol phosphate production were determined as a measure of G protein activation. Whereas these receptors did not efficiently interact with wild type Gα(q), most of them gained the ability to productively couple to -6q. Additional experiments indicated that the observed functional promiscuity of -6q is not due to overexpression (as compared with wild type Gα(q)) or to a lack of palmitoylation. We conclude that the N-terminal extension characteristic for Gα(q)/11 proteins is critical for constraining the receptor coupling selectivity of these subunits, indicative of a novel mechanism by which the fidelity of receptor- G protein interactions can be regulated.

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Kostenis, E., Degtyarev, M. Y., Conklin, B. R., & Wess, J. (1997). The N-terminal extension of Gα(q) is critical for constraining the selectivity of receptor coupling. Journal of Biological Chemistry, 272(31), 19107–19110. https://doi.org/10.1074/jbc.272.31.19107

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