The Self‐Association of the KRAS4b Protein is Altered by Lipid‐Bilayer Composition and Electrostatics

Author:

Lee Ki‐Young1ORCID,Ikura Mitsuhiko2,Marshall Christopher B.2

Affiliation:

1. Department of Pharmacy College of Pharmacy and Institute of Pharmaceutical Sciences CHA University Gyeonggi-Do South Korea

2. Princess Margaret Cancer Centre University Health Network Toronto Ontario M5G 1L7 Canada

Abstract

AbstractKRAS is a peripheral membrane protein that regulates multiple signaling pathways, and is mutated in ≈30 % of cancers. Transient self‐association of KRAS is essential for activation of the downstream effector RAF and oncogenicity. The presence of anionic phosphatidylserine (PS) lipids in the membrane was shown to promote KRAS self‐assembly, however, the structural mechanisms remain elusive. Here, we employed nanodisc bilayers of defined lipid compositions, and probed the impact of PS concentration on KRAS self‐association. Paramagnetic NMR experiments demonstrated the existence of two transient dimer conformations involving alternate electrostatic contacts between R135 and either D153 or E168 on the “α4/5‐α4/5” interface, and revealed that lipid composition and salt modulate their dynamic equilibrium. These dimer interfaces were validated by charge‐reversal mutants. This plasticity demonstrates how the dynamic KRAS dimerization interface responds to the environment, and likely extends to the assembly of other signaling complexes on the membrane.

Funder

Canadian Cancer Society Research Institute

Canadian Institutes of Health Research

Princess Margaret Cancer Foundation

Gyeonggi-do Regional Research Center

Canada Foundation for Innovation

Publisher

Wiley

Subject

General Chemistry,Catalysis

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