In Vitro Pharmacological Profile of a New Small Molecule Bradykinin B(2) Receptor Antagonist

We here report the discovery and early characterization of Compound 3, a representative of a novel class of small molecule bradykinin (BK) B(2) receptor antagonists, and its superior profile to the prior art B(2) receptor antagonists Compound 1 and Compound 2. Compound 3, Compound 2, and Compound 1...

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Autores principales: Lesage, Anne, Gibson, Christoph, Marceau, François, Ambrosi, Horst-Dieter, Saupe, Jörn, Katzer, Werner, Loenders, Brigitte, Charest-Morin, Xavier, Knolle, Jochen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7316994/
https://www.ncbi.nlm.nih.gov/pubmed/32636746
http://dx.doi.org/10.3389/fphar.2020.00916
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author Lesage, Anne
Gibson, Christoph
Marceau, François
Ambrosi, Horst-Dieter
Saupe, Jörn
Katzer, Werner
Loenders, Brigitte
Charest-Morin, Xavier
Knolle, Jochen
author_facet Lesage, Anne
Gibson, Christoph
Marceau, François
Ambrosi, Horst-Dieter
Saupe, Jörn
Katzer, Werner
Loenders, Brigitte
Charest-Morin, Xavier
Knolle, Jochen
author_sort Lesage, Anne
collection PubMed
description We here report the discovery and early characterization of Compound 3, a representative of a novel class of small molecule bradykinin (BK) B(2) receptor antagonists, and its superior profile to the prior art B(2) receptor antagonists Compound 1 and Compound 2. Compound 3, Compound 2, and Compound 1 are highly potent antagonists of the human recombinant B(2) receptor (K(b) values 0.24, 0.95, and 1.24 nM, respectively, calcium mobilization assay). Compound 3 is more potent than the prior art compounds and icatibant in this assay (K(b) icatibant 2.81 nM). The compounds also potently inhibit BK-induced contraction of endogenous B(2) receptors in a human isolated umbilical vein bioassay. The potencies of Compound 3, Compound 2, Compound 1, and icatibant are (pA(2) values) 9.67, 9.02, 8.58, and 8.06 (i.e. 0.21, 0.95, 2.63, and 8.71 nM), respectively. Compound 3 and Compound 2 were further characterized. They inhibit BK-induced c-Fos signaling and internalization of recombinant human B(2) receptors in HEK293 cells, and do not antagonize the venous effects mediated by other G protein-coupled receptors in the umbilical vein model, including the bradykinin B(1) receptor. Antagonist potency of Compound 3 at cloned cynomolgus monkey, dog, rat, and mouse B(2) receptors revealed species selectivity, with a high antagonist potency for human and monkey B(2) receptors, but several hundred-fold lower potency for the other B(2) receptors. The in vitro off-target profile of Compound 3 demonstrates a high degree of selectivity over a wide range of molecular targets, including the bradykinin B(1) receptor. Compound 3 showed a lower intrinsic clearance in the microsomal stability assay than the prior art compounds. With an efflux ratio of 1.0 in the Caco-2 permeability assay Compound 3 is predicted to be not a substrate of efflux pumps. In conclusion, we discovered a novel chemical class of highly selective and very potent B(2) receptor antagonists, as exemplified by Compound 3. The compound showed excellent absorption in the Caco-2 assay, predictive of good oral bioavailability, and favourable metabolic stability in liver microsomes. Compound 3 has provided a significant stepping stone towards the discovery of the orally bioavailable B(2) antagonist PHA-022121, currently in phase 1 clinical development.
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spelling pubmed-73169942020-07-06 In Vitro Pharmacological Profile of a New Small Molecule Bradykinin B(2) Receptor Antagonist Lesage, Anne Gibson, Christoph Marceau, François Ambrosi, Horst-Dieter Saupe, Jörn Katzer, Werner Loenders, Brigitte Charest-Morin, Xavier Knolle, Jochen Front Pharmacol Pharmacology We here report the discovery and early characterization of Compound 3, a representative of a novel class of small molecule bradykinin (BK) B(2) receptor antagonists, and its superior profile to the prior art B(2) receptor antagonists Compound 1 and Compound 2. Compound 3, Compound 2, and Compound 1 are highly potent antagonists of the human recombinant B(2) receptor (K(b) values 0.24, 0.95, and 1.24 nM, respectively, calcium mobilization assay). Compound 3 is more potent than the prior art compounds and icatibant in this assay (K(b) icatibant 2.81 nM). The compounds also potently inhibit BK-induced contraction of endogenous B(2) receptors in a human isolated umbilical vein bioassay. The potencies of Compound 3, Compound 2, Compound 1, and icatibant are (pA(2) values) 9.67, 9.02, 8.58, and 8.06 (i.e. 0.21, 0.95, 2.63, and 8.71 nM), respectively. Compound 3 and Compound 2 were further characterized. They inhibit BK-induced c-Fos signaling and internalization of recombinant human B(2) receptors in HEK293 cells, and do not antagonize the venous effects mediated by other G protein-coupled receptors in the umbilical vein model, including the bradykinin B(1) receptor. Antagonist potency of Compound 3 at cloned cynomolgus monkey, dog, rat, and mouse B(2) receptors revealed species selectivity, with a high antagonist potency for human and monkey B(2) receptors, but several hundred-fold lower potency for the other B(2) receptors. The in vitro off-target profile of Compound 3 demonstrates a high degree of selectivity over a wide range of molecular targets, including the bradykinin B(1) receptor. Compound 3 showed a lower intrinsic clearance in the microsomal stability assay than the prior art compounds. With an efflux ratio of 1.0 in the Caco-2 permeability assay Compound 3 is predicted to be not a substrate of efflux pumps. In conclusion, we discovered a novel chemical class of highly selective and very potent B(2) receptor antagonists, as exemplified by Compound 3. The compound showed excellent absorption in the Caco-2 assay, predictive of good oral bioavailability, and favourable metabolic stability in liver microsomes. Compound 3 has provided a significant stepping stone towards the discovery of the orally bioavailable B(2) antagonist PHA-022121, currently in phase 1 clinical development. Frontiers Media S.A. 2020-06-19 /pmc/articles/PMC7316994/ /pubmed/32636746 http://dx.doi.org/10.3389/fphar.2020.00916 Text en Copyright © 2020 Lesage, Gibson, Marceau, Ambrosi, Saupe, Katzer, Loenders, Charest-Morin and Knolle http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Lesage, Anne
Gibson, Christoph
Marceau, François
Ambrosi, Horst-Dieter
Saupe, Jörn
Katzer, Werner
Loenders, Brigitte
Charest-Morin, Xavier
Knolle, Jochen
In Vitro Pharmacological Profile of a New Small Molecule Bradykinin B(2) Receptor Antagonist
title In Vitro Pharmacological Profile of a New Small Molecule Bradykinin B(2) Receptor Antagonist
title_full In Vitro Pharmacological Profile of a New Small Molecule Bradykinin B(2) Receptor Antagonist
title_fullStr In Vitro Pharmacological Profile of a New Small Molecule Bradykinin B(2) Receptor Antagonist
title_full_unstemmed In Vitro Pharmacological Profile of a New Small Molecule Bradykinin B(2) Receptor Antagonist
title_short In Vitro Pharmacological Profile of a New Small Molecule Bradykinin B(2) Receptor Antagonist
title_sort in vitro pharmacological profile of a new small molecule bradykinin b(2) receptor antagonist
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7316994/
https://www.ncbi.nlm.nih.gov/pubmed/32636746
http://dx.doi.org/10.3389/fphar.2020.00916
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