Allostery of atypical modulators at oligomeric G protein-coupled receptors

Author:

Shivnaraine Rabindra V.,Kelly Brendan,Elmslie Gwendolynne,Huang Xi-Ping,Dong Yue John,Seidenberg Margaret,Wells James W.,Ellis John

Abstract

AbstractMany G protein-coupled receptors (GPCRs) are therapeutic targets, with most drugs acting at the orthosteric site. Some GPCRs also possess allosteric sites, which have become a focus of drug discovery. In the M2 muscarinic receptor, allosteric modulators regulate the binding and functional effects of orthosteric ligands through a mix of conformational changes, steric hindrance and electrostatic repulsion transmitted within and between the constituent protomers of an oligomer. Tacrine has been called an atypical modulator because it exhibits positive cooperativity, as revealed by Hill coefficients greater than 1 in its negative allosteric effect on binding and response. Radioligand binding and molecular dynamics simulations were used to probe the mechanism of that modulation in monomers and oligomers of wild-type and mutant M2 receptors. Tacrine is not atypical at monomers, which indicates that its atypical effects are a property of the receptor in its oligomeric state. These results illustrate that oligomerization of the M2 receptor has functional consequences.

Funder

Canadian Institutes of Health Research

Heart and Stroke Foundation of Canada

National Institutes of Health

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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