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

Jingyi ZhaoVincent DiGiacomoMariola Ferreras-GutierrezShiva DastjerdiAlain Ibáñez de OpakuaJong-Chan ParkAlex LuebbersQingyan ChenAaron BeelerFrancisco J BlancoMikel Garcia-Marcos
Published in: Proceedings of the National Academy of Sciences of the United States of America (2023)
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.
Keyphrases
  • small molecule
  • squamous cell carcinoma
  • papillary thyroid
  • gene expression
  • small cell lung cancer
  • stem cells
  • signaling pathway
  • immune response
  • nuclear factor
  • bone marrow
  • drug discovery