Coarse-grained/molecular mechanics of the TAS2R38 bitter taste receptor: experimentally-validated detailed structural prediction of agonist binding.

Alessandro Marchiori,Alejandro Giorgetti,Wolfgang Meyerhof,Paolo Carloni,Paolo Gasparini,Maik Behrens,Luciana Capece,Yoshiro Ishimaru

doi:10.1371/journal.pone.0064675

Abstract

Bitter molecules in humans are detected by ∼25 G protein-coupled receptors (GPCRs). The lack of atomic resolution structure for any of them is complicating an in depth understanding of the molecular mechanisms underlying bitter taste perception. Here, we investigate the molecular determinants of the interaction of the TAS2R38 bitter taste receptor with its agonists phenylthiocarbamide (PTC) and propylthiouracil (PROP). We use the recently developed hybrid Molecular Mechanics/Coarse Grained (MM/CG) method tailored specifically for GPCRs. The method, through an extensive exploration of the conformational space in the binding pocket, allows the identification of several residues important for agonist binding that would have been very difficult to capture from the standard bioinformatics/docking approach. Our calculations suggest that both agonists bind to Asn103, Phe197, Phe264 and Trp201, whilst they do not interact with the so-called extra cellular loop 2, involved in cis-retinal binding in the GPCR rhodopsin. These predictions are consistent with data sets based on more than 20 site-directed mutagenesis and functional calcium imaging experiments of TAS2R38. The method could be readily used for other GPCRs for which experimental information is currently lacking.

Highlights

Bitter taste perception prevents humans and other mammals from ingesting toxic substances
We have shown that 0.8 ms Mechanics/Coarse Grained (MM/CG) simulations of a G protein-coupled receptors (GPCRs)/inverseagonist complex for which the 3D X-ray structure is experimentally available -the b2 adrenergic receptor/S-Carazolol (b2 AR/SCar)- could reproduce the results of full atomistic MD [14,18]
We have presented a computational study of the TAS2R38 receptor in complex with its agonists PTC and PROP (Chart S1)

Summary

Introduction

Bitter taste perception prevents humans and other mammals from ingesting toxic substances. TAS2Rs are located in special subsets of taste receptor cells [1,2,3,4]. They are able to detect multiple and diverse natural and synthetic organic molecules [5]. Single nucleotide polymorphisms in the TAS2R38 gene (GenBank: AY258597.1) cause ‘‘blindness’’ to its agonists phenylthiocarbamide (PTC) and propylthiouracil (PROP) (Chart S1) [6]. This constitutes a well-characterized human genetic trait [7].

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Results

Conclusion