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Hetero-oligomerization of Rho and Ras GTPases Connects GPCR Activation to mTORC2-AKT Signaling

Hiroshi Senoo, May Wai, Hideaki T. Matsubayashi, Hiromi Sesaki, Miho Iijima

2020Cell Reports19 citationsDOIOpen Access PDF

Abstract

The activation of G-protein-coupled receptors (GPCRs) leads to the activation of mTORC2 in cell migration and metabolism. However, the mechanism that links GPCRs to mTORC2 remains unknown. Here, using Dictyostelium cells, we show that GPCR-mediated chemotactic stimulation induces hetero-oligomerization of phosphorylated GDP-bound Rho GTPase and GTP-bound Ras GTPase in directed cell migration. The Rho-Ras hetero-oligomers directly and specifically stimulate mTORC2 activity toward AKT in cells and after biochemical reconstitution using purified proteins in vitro. The Rho-Ras hetero-oligomers do not activate ERK/MAPK, another kinase that functions downstream of GPCRs and Ras. Human KRas4B functionally replace Dictyostelium Ras in mTORC2 activation. In contrast to GDP-Rho, GTP-Rho antagonizes mTORC2-AKT signaling by inhibiting the oligomerization of GDP-Rho with GTP-Ras. These data reveal that GPCR-stimulated hetero-oligomerization of Rho and Ras provides a critical regulatory step that controls mTORC2-AKT signaling.

Topics & Concepts

G protein-coupled receptorCell biologymTORC2GTPaseProtein kinase BSignal transductionPleckstrin homology domainG proteinChemistryPhosphorylationRac GTP-Binding ProteinsMAPK/ERK pathwayBiologymTORC1RAC1Cellular Mechanics and InteractionsProtein Kinase Regulation and GTPase SignalingPI3K/AKT/mTOR signaling in cancer