Selectivity and Maximum Response of Vibegron and Mirabegron for β3-Adrenergic Receptors

Benjamin M. Brucker, MD; Jennifer King, PharmD; Paul N. Mudd, Jr, PharmD, MBA; Kimberly McHale, PhD

Current Therapeutic Research (Jan 2022)

Selectivity and Maximum Response of Vibegron and Mirabegron for β3-Adrenergic Receptors

Benjamin M. Brucker, MD,
Jennifer King, PharmD,
Paul N. Mudd, Jr, PharmD, MBA,
Kimberly McHale, PhD

Affiliations

Benjamin M. Brucker, MD: Departments of Urology and Obstetrics and Gynecology, NYU Langone Health, New York, New York
Jennifer King, PharmD: Urovant Sciences, Irvine, California; Currently at: Cyclerion Therapeutics, Boston, Massachusetts
Paul N. Mudd, Jr, PharmD, MBA: Urovant Sciences, Irvine, California; Currently at: Priovant Therapeutics, Durham, North Carolina
Kimberly McHale, PhD: Dermavant Sciences, Morrisville, North Carolina; Address correspondence to: Kimberly McHale, PhD, Dermavant Sciences, 3300 Paramount Pkwy, Ste 150, Morrisville, NC 27560.

Journal volume & issue: Vol. 96
p. 100674

Abstract

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ABSTRACT: Background: The β3-adrenergic agonists vibegron and mirabegron have shown favorable safety profiles and efficacy for the treatment of overactive bladder. However, β-adrenergic receptors are also found outside the bladder, which could lead to off-target activity. Objective: This study assessed the selectivity of vibegron and mirabegron for β-adrenergic receptors and the maximal effect and potency for β3-adrenergic receptors. Methods: Functional cellular assays were performed using Chinese hamster ovary-K1 cells expressing β1-, Chinese hamster ovary cells expressing β2-, and human embryonic kidney 293 cells expressing β3-adrenergic receptors. Cells were incubated with vibegron, mirabegron, or control (β1 and β3, isoproterenol; β2, procaterol). Responses were quantified using homogeneous time-resolved fluorescence of cyclic adenosine monophosphate and were normalized to the respective control. Half-maximal effective concentration and maximum response values were determined by nonlinear least-squares regression analysis. Results: Activation of β3-adrenergic receptors with vibegron or mirabegron resulted in concentration-dependent β3-adrenergic receptor responses. Mean (SEM) half-maximal effective concentration values at β3-adrenergic receptors were 2.13 (0.25) nM for vibegron and 10.0 (0.56) nM for mirabegron. At a concentration of 10 µM, β3-adrenergic activity relative to isoproterenol was 104% for vibegron and 88% for mirabegron. Maximum response at β3-adrenergic receptors was 99.2% for vibegron and 80.4% for mirabegron. β1-adrenergic activity was 0% and 3% for vibegron and mirabegron, respectively; β2-adrenergic activity was 2% and 15%, respectively. Conclusions: Vibegron showed no measurable β1 and low β2 activity compared with mirabegron, which showed low β1 and some β2 activity. Both showed considerable selectivity at β3-adrenergic receptors; however, vibegron demonstrated near-exclusive β3 activity and a higher maximum β3 response.

Published in Current Therapeutic Research

ISSN: 0011-393X (Print); 1879-0313 (Online)
Publisher: Elsevier
Country of publisher: Netherlands
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: http://www.journals.elsevier.com/current-therapeutic-research/

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