Literature DB >> 31160049

Illuminating G-Protein-Coupling Selectivity of GPCRs.

Asuka Inoue1, Francesco Raimondi2, Francois Marie Ngako Kadji3, Gurdeep Singh4, Takayuki Kishi3, Akiharu Uwamizu3, Yuki Ono3, Yuji Shinjo3, Satoru Ishida3, Nadia Arang5, Kouki Kawakami3, J Silvio Gutkind5, Junken Aoki6, Robert B Russell7.   

Abstract

Heterotrimetic G proteins consist of four subfamilies (Gs, Gi/o, Gq/11, and G12/13) that mediate signaling via G-protein-coupled receptors (GPCRs), principally by receptors binding Gα C termini. G-protein-coupling profiles govern GPCR-induced cellular responses, yet receptor sequence selectivity determinants remain elusive. Here, we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique Gα subunit C termini. For each receptor, we probed chimeric Gα subunit activation via a transforming growth factor-α (TGF-α) shedding response in HEK293 cells lacking endogenous Gq/11 and G12/13 proteins, and complemented G-protein-coupling profiles through a NanoBiT-G-protein dissociation assay. Interrogation of the dataset identified sequence-based coupling specificity features, inside and outside the transmembrane domain, which we used to develop a coupling predictor that outperforms previous methods. We used the predictor to engineer designer GPCRs selectively coupled to G12. This dataset of fine-tuned signaling mechanisms for diverse GPCRs is a valuable resource for research in GPCR signaling.
Copyright © 2019 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  DREADD; G-protein-coupled receptors; HEK293 cells; NanoBiT; TGF-α shedding assay; bioinformatics; chimeric G protein; prediction; protein design; signaling

Year:  2019        PMID: 31160049      PMCID: PMC6773469          DOI: 10.1016/j.cell.2019.04.044

Source DB:  PubMed          Journal:  Cell        ISSN: 0092-8674            Impact factor:   41.582


  68 in total

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