Molecular dynamics simulations of GPCR–cholesterol interaction: An emerging paradigm

doi:10.1016/j.bbamem.2015.03.018

Biochimica et Biophysica Acta (BBA) - Biomembranes

Volume 1848, Issue 9, September 2015, Pages 1775-1782

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Highlights

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GPCRs represent important cholesterol-modulated drug targets.
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Multiple cholesterol hot-spots identified in GPCRs.
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High occupancy sites correspond to microsecond time scale association.
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Free energy of cholesterol-GPCR association is of the order of kT.
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Cholesterol modulates GPCR oligomerization.

Abstract

G protein-coupled receptors (GPCRs) are the largest class of molecules involved in signal transduction across cell membranes and represent major targets in the development of novel drug candidates. Membrane cholesterol plays an important role in GPCR structure and function. Molecular dynamics simulations have been successful in exploring the effect of cholesterol on the receptor and a general consensus molecular view is emerging. We review here recent molecular dynamics studies at multiple resolutions highlighting the main features of cholesterol-GPCR interaction. Several cholesterol interaction sites have been identified on the receptor that are reminiscent of nonannular sites. These cholesterol hot-spots are highly dynamic and have a microsecond time scale of exchange with the bulk lipids. A few consensus sites (such as the CRAC site) have been identified that correspond to higher cholesterol interaction. Interestingly, high plasticity is observed in the modes of cholesterol interaction and several sites have been suggested to have high cholesterol occupancy. We therefore believe that these cholesterol hot-spots are indicative of ‘high occupancy sites’ rather than ‘binding sites’. The results suggest that the energy landscape of cholesterol association with GPCRs corresponds to a series of shallow minima interconnected by low barriers. These specific interactions, along with general membrane effects, have been observed to modulate GPCR organization. Membrane cholesterol effects on receptor structure and organization, that in turn influences receptor cross-talk and drug efficacy, represent a new frontier in GPCR research. This article is part of a Special Issue entitled: Lipid-protein interactions. Guest Editors: Amitabha Chattopadhyay and Jean-Marie Ruysschaert.

Graphical abstract

Abbreviations

CCM

cholesterol consensus motif

CRAC

cholesterol recognition amino acid consensus

GPCR

G protein-coupled receptor

POPC

1-palmitoyl-2-oleoyl-sn-glycero-3-phosphocholine

Keywords

GPCR

Coarse-grain simulation

Membrane cholesterol

CRAC

Receptor dimerization

Lipid-receptor interaction

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^☆: This article is part of a Special Issue entitled: Lipid-protein interactions. Guest Editors: Amitabha Chattopadhyay and Jean-Marie Ruysschaert.