Litcius/Paper detail

Enhancing the Signaling of GPCRs via Orthosteric Ions

H. C. Stephen Chan, Yueming Xu, Liang Tan, Horst Vogel, Jianjun Cheng, Dong Wu, Shuguang Yuan

2020ACS Central Science38 citationsDOIOpen Access PDF

Abstract

has been proposed to stabilize the inactive receptor state by mediating interactions between transmembrane helices. Here, we probed the existence of internal and functionally important sodium ions in the dopamine D2 receptor, using molecular dynamics simulations. Besides a new sodium ion at the allosteric ligand binding site, we discovered an additional sodium ion, located close to the orthosteric ligand binding site. Through cell-based activation assays, the signaling of D2 receptor with site-specific mutations was tested against a series of chemically modified agonists. We concluded an important structural role of this newly discovered orthosteric sodium ion in modulating the receptor signaling: It enables the coordination of a polar residue in the ligand binding site with an appropriately designed agonist molecule. An identical interaction was also observed in a recently released high-resolution crystal structure of mu-opioid receptor, which was reresolved in this work. Probably because of similar interactions, various metal ions have been found to increase the signaling of many other GPCRs. This unique principle and strategy could be used to optimize the drug activity of GPCR. Our findings open a new mechanistic opportunity of GPCR signaling and help design the next generation of drugs targeting GPCRs.

Topics & Concepts

G protein-coupled receptorAllosteric regulationChemistryReceptorIon channelAllosteric modulatorSignal transductionLigand (biochemistry)Binding siteAgonistFunctional selectivityDrug discoveryBiophysicsBiochemistryBiologyReceptor Mechanisms and SignalingNeuropeptides and Animal PhysiologyChemical Synthesis and Analysis