Assessment of Biased Agonism at the A Adenosine Receptor Using β-arrestin and MiniGα Recruitment Assays

Overview

Journal Biochem Pharmacol

Specialties Biochemistry
Pharmacology

Date 2020 Apr 1

PMID 32224136

Citations 19

Authors

Eline Pottie

Dilip K Tosh

Zhan-Guo Gao

Kenneth A Jacobson

Christophe P Stove

Affiliations

Soon will be listed here.

Abstract

The A adenosine receptor (AAR) is a G protein-coupled receptor that is involved in a wide variety of physiological and pathological processes, such as cancer. However, the use of compounds pharmacologically targeting this receptor remains limited in clinical practice, despite extensive efforts for compound synthesis. Moreover, the possible occurrence of biased agonism further complicates the interpretation of the functional characteristics of compounds. Hence the need for simple assays, which are comparable in terms of the used cell lines and read-out technique. We previously established a stable β-arrestin 2 (βarr2) bioassay, employing a simple, luminescent read-out via functional complementation of a split nanoluciferase enzyme. Here, we developed a complementary, new bioassay in which coupling of an engineered miniGα protein to activated AAR is monitored using a similar approach. Application of both bioassays for the concurrent determination of the potencies and efficacies of a set of 19 N-substituted adenosine analogues not only allowed for the characterization of structure-activity relationships, but also for the quantification of biased agonism. Although a broad distribution in potency and efficacy values was obtained within the test panel, no significant bias was observed toward either the βarr2 or miniGα pathway.

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