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Going Rogue: Mechanisms, Regulation, and Roles of Mutationally Activated Gα in Human Cancer.

Morgan B Dwyer, Jenna L Aumiller, Philip B Wedegaertner

Molecular pharmacology 2024 Oct 17


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    G protein-coupled receptors (GPCRs) couple to heterotrimeric G proteins, comprised of α and βγ subunits, to convert extracellular signals into activation of intracellular signaling pathways. Canonically, GPCR-mediated activation results in the exchange of GDP for GTP on G protein α subunits (Gα) and the dissociation of Gα-GTP and G protein βγ subunits (Gβγ), both of which can regulate a variety of signaling pathways. Hydrolysis of bound GTP by returns the protein to Gα-GDP and allows reassociation with Gβγ to reform the inactive heterotrimer. Naturally occurring mutations in have been found at conserved glutamine and arginine amino acids that disrupt the canonical G protein cycle by inhibiting GTP hydrolysis, rendering these mutants constitutively active. Interestingly, these dysregulated mutants are found in many different cancers due to their ability to sustain aberrant signaling without a need for activation by GPCRs. This review will highlight an increased recognition of the prevalence of such constitutively activating mutations in cancers and the signaling pathways activated. In addition, we will discuss new knowledge regarding how these constitutively active are regulated, how different mutations are biochemically distinct, and how mutationally activated are unique compared with GPCR-activated Lastly, we will discuss recent progress in developing inhibitors directly targeting constitutively active mutants. SIGNIFICANCE STATEMENT: Constitutively activating mutations in G protein α subunits (Gα) widely occur in and contribute to the development of many human cancers. To develop ways to inhibit dysregulated, oncogenic signaling by these mutant , it is crucial to better understand mechanisms that lead to constitutive activation and unique mechanisms that regulate mutationally activated in cells. The prevalence of activating mutations in in various cancers makes proteins compelling targets for the development of therapeutics. Copyright © 2024 by The American Society for Pharmacology and Experimental Therapeutics.

    Citation

    Morgan B Dwyer, Jenna L Aumiller, Philip B Wedegaertner. Going Rogue: Mechanisms, Regulation, and Roles of Mutationally Activated Gα in Human Cancer. Molecular pharmacology. 2024 Oct 17;106(5):198-215

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    PMID: 39187387

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