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Small-molecule targeting of GPCR-independent noncanonical G-protein signaling in cancer

Jingyi Zhao, Vincent DiGiacomo, Mariola Ferreras-Gutiérrez, Shiva Dastjerdi, Alain Ibáñez de Opakua, Jong‐Chan Park, Alex Luebbers, Qingyan Chen, Aaron B. Beeler, Francisco J. Blanco, Mikel Garcia‐Marcos

2023Proceedings of the National Academy of Sciences17 citationsDOIOpen Access PDF

Abstract

Activation of heterotrimeric G-proteins (Gαβγ) by G-protein-coupled receptors (GPCRs) is a quintessential mechanism of cell signaling widely targeted by clinically approved drugs. However, it has become evident that heterotrimeric G-proteins can also be activated via GPCR-independent mechanisms that remain untapped as pharmacological targets. GIV/Girdin has emerged as a prototypical non-GPCR activator of G proteins that promotes cancer metastasis. Here, we introduce IGGi-11, a first-in-class small-molecule inhibitor of noncanonical activation of heterotrimeric G-protein signaling. IGGi-11 binding to G-protein α-subunits (Gαi) specifically disrupted their engagement with GIV/Girdin, thereby blocking noncanonical G-protein signaling in tumor cells and inhibiting proinvasive traits of metastatic cancer cells. In contrast, IGGi-11 did not interfere with canonical G-protein signaling mechanisms triggered by GPCRs. By revealing that small molecules can selectively disable noncanonical mechanisms of G-protein activation dysregulated in disease, these findings warrant the exploration of therapeutic modalities in G-protein signaling that go beyond targeting GPCRs.

Topics & Concepts

Heterotrimeric G proteinG protein-coupled receptorG proteinCell biologySignal transductionBiologyCell signalingRegulator of G protein signalingGTPase-activating proteinProtein Kinase Regulation and GTPase SignalingReceptor Mechanisms and SignalingPI3K/AKT/mTOR signaling in cancer
Small-molecule targeting of GPCR-independent noncanonical G-protein signaling in cancer | Litcius