The Self-Association of the KRAS4b Protein is Altered by Lipid-Bilayer Composition and Electrostatics |
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| Authors: | Prof Ki-Young Lee Prof Mitsuhiko Ikura Dr Christopher B Marshall |
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| Institution: | 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 |
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| Abstract: | KRAS 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. |
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| Keywords: | KRAS Dimers Lipids NMR Spectroscopy Nanodiscs Plastic Interactions |
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