Database of articles cited by EMDB/PDB/SASBDB data

Keywords
Structure methods	All X-ray diffraction NMR electron microscopy small angle scattering neutron diffraction fiber diffraction powder diffraction infrared spectroscopy EPR fluorescence transfer theoretical model Hybrid
Author
Journal
IF	>30 >20 >10 >5 all

Title	Structures of the PI3Kα/KRas complex on lipid bilayers reveal the molecular mechanism of PI3Kα activation.
Journal, issue, pages	bioRxiv, Year 2025
Publish date	Mar 25, 2025
Authors	Hayarpi Torosyan / Michael D Paul / Allison Maker / Brigitte G Meyer / Natalia Jura / Kliment A Verba
PubMed Abstract	PI3Kα is a potent oncogene that converts PIP2 to PIP3 at the plasma membrane upon activation by receptor tyrosine kinases and Ras GTPases. In the absence of any structures of activated PI3Kα, the ...PI3Kα is a potent oncogene that converts PIP2 to PIP3 at the plasma membrane upon activation by receptor tyrosine kinases and Ras GTPases. In the absence of any structures of activated PI3Kα, the molecular details of its activation remain unknown. Here, we present cryo-EM structures of the PI3Kα/KRas complex embedded in lipid nanodiscs, revealing a rich ensemble of PI3Kα states adopted at the membrane surface. The sequential addition of a lipid bilayer, PIP2 and an activating phosphopeptide leads to the progressive release of key inhibitory domains from the PI3Kα catalytic core, which directly correlates with the reorganization of its active site. While association with POPC/POPS nanodiscs partially relieves PI3Kα autoinhibition, incorporation of PIP2 triggers near-complete displacement of PI3Kα inhibitory domains and significant restructuring of active site regulatory motifs. The addition of the activating phosphopeptide induces dimerization of the PI3Kα/KRas complex through a p110α catalytic subunit-mediated interface that is sterically occluded in autoinhibited PI3Kα. In cells, this dimeric PI3Kα complex amplifies Akt signaling in response to growth factor stimulation. Collectively, our structures map the conformational landscape of PI3Kα activation and reveal previously unexplored interfaces for potential therapeutic targeting.
External links	bioRxiv / PubMed:40196507 / PubMed Central
Methods	EM (single particle)
Resolution	2.61 - 10.0 Å
Structure data	49452 9ni4 EMDB-49452, PDB-9ni4: Cryo-EM structure of the PI3K alpha/KRas/HER3 phosphopeptide complex dimer on POPC/POPS/PIP2 nanodiscs Method: EM (single particle) / Resolution: 2.61 Å 49453 9ni5 EMDB-49453, PDB-9ni5: Cryo-EM structure of the PI3K alpha/KRas/HER3 phosphopeptide complex on POPC/POPS/PIP2 nanodiscs Method: EM (single particle) / Resolution: 2.89 Å 49454 9ni6 EMDB-49454, PDB-9ni6: Cryo-EM structure of the Class 1 PI3K alpha/KRas complex on POPC/POPS nanodiscs Method: EM (single particle) / Resolution: 3.01 Å 49458 9nid EMDB-49458, PDB-9nid: Cryo-EM structure of the PI3K alpha/KRas/HER3 phosphopeptide complex dimer on POPC/POPS/PIP2 nanodiscs low-pass filtered to 5 angstroms Method: EM (single particle) / Resolution: 5.0 Å 49459 9nie EMDB-49459, PDB-9nie: Cryo-EM structure of the PI3K alpha/KRas/HER3 phosphopeptide complex on POPC/POPS/PIP2 nanodiscs low-pass filtered to 5 angstroms Method: EM (single particle) / Resolution: 5.0 Å 49519 9nlc EMDB-49519, PDB-9nlc: Cryo-EM structure of the Class 1 PI3K alpha/KRas complex on POPC/POPS nanodiscs low-pass filtered to 10 angstroms Method: EM (single particle) / Resolution: 10.0 Å
Chemicals	PDB-1azd: CONCANAVALIN FROM CANAVALIA BRASILIENSIS ChemComp-MG: Unknown entry ChemComp-GNP: PHOSPHOAMINOPHOSPHONIC ACID-GUANYLATE ESTER / GppNHp, GMPPNP, energy-carrying molecule analogue*YM
Source	homo sapiens (human)
Keywords	Transferase/Hydrolase / lipid kinase / GTPase / ONCOPROTEIN / Transferase-Hydrolase complex