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Discovery and characterization of ORM‐11372, a novel inhibitor of the sodium‐calcium exchanger with positive inotropic activity
BACKGROUND AND PURPOSE: The lack of selective sodium–calcium exchanger (NCX) inhibitors has hampered the exploration of physiological and pathophysiological roles of cardiac NCX 1.1. We aimed to discover more potent and selective drug like NCX 1.1 inhibitor. EXPERIMENTAL APPROACH: A flavan series‐ba...
Autores principales: | , , , , , , , , , , , , , , , , , , , , |
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Formato: | Online Artículo Texto |
Lenguaje: | English |
Publicado: |
John Wiley and Sons Inc.
2020
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Materias: | |
Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7707092/ https://www.ncbi.nlm.nih.gov/pubmed/32959887 http://dx.doi.org/10.1111/bph.15257 |
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author | Otsomaa, Leena Levijoki, Jouko Wohlfahrt, Gerd Chapman, Hugh Koivisto, Ari‐Pekka Syrjänen, Kaisa Koskelainen, Tuula Peltokorpi, Saara‐Elisa Finckenberg, Piet Heikkilä, Aira Abi‐Gerges, Najah Ghetti, Andre Miller, Paul E. Page, Guy Mervaala, Eero Nagy, Norbert Kohajda, Zsófia Jost, Norbert Virág, László Varró, András Papp, Julius Gy. |
author_facet | Otsomaa, Leena Levijoki, Jouko Wohlfahrt, Gerd Chapman, Hugh Koivisto, Ari‐Pekka Syrjänen, Kaisa Koskelainen, Tuula Peltokorpi, Saara‐Elisa Finckenberg, Piet Heikkilä, Aira Abi‐Gerges, Najah Ghetti, Andre Miller, Paul E. Page, Guy Mervaala, Eero Nagy, Norbert Kohajda, Zsófia Jost, Norbert Virág, László Varró, András Papp, Julius Gy. |
author_sort | Otsomaa, Leena |
collection | PubMed |
description | BACKGROUND AND PURPOSE: The lack of selective sodium–calcium exchanger (NCX) inhibitors has hampered the exploration of physiological and pathophysiological roles of cardiac NCX 1.1. We aimed to discover more potent and selective drug like NCX 1.1 inhibitor. EXPERIMENTAL APPROACH: A flavan series‐based pharmacophore model was constructed. Virtual screening helped us identify a novel scaffold for NCX inhibition. A distinctively different NCX 1.1 inhibitor, ORM‐11372, was discovered after lead optimization. Its potency against human and rat NCX 1.1 and selectivity against other ion channels was assessed. The cardiovascular effects of ORM‐11372 were studied in normal and infarcted rats and rabbits. Human cardiac safety was studied ex vivo using human ventricular trabeculae. KEY RESULTS: ORM‐11372 inhibited human NCX 1.1 reverse and forward currents; IC(50) values were 5 and 6 nM respectively. ORM‐11372 inhibited human cardiac sodium 1.5 (I (Na)) and hERG K(V)11.1 currents (I (hERG)) in a concentration‐dependent manner; IC(50) values were 23.2 and 10.0 μM. ORM‐11372 caused no changes in action potential duration; short‐term variability and triangulation were observed for concentrations of up to 10 μM. ORM‐11372 induced positive inotropic effects of 18 ± 6% and 35 ± 8% in anaesthetized rats with myocardial infarctions and in healthy rabbits respectively; no other haemodynamic effects were observed, except improved relaxation at the lowest dose. CONCLUSION AND IMPLICATIONS: ORM‐11372, a unique, novel, and potent inhibitor of human and rat NCX 1.1, is a positive inotropic compound. NCX inhibition can induce clinically relevant improvements in left ventricular contractions without affecting relaxation, heart rate, or BP, without pro‐arrhythmic risk. |
format | Online Article Text |
id | pubmed-7707092 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 2020 |
publisher | John Wiley and Sons Inc. |
record_format | MEDLINE/PubMed |
spelling | pubmed-77070922020-12-09 Discovery and characterization of ORM‐11372, a novel inhibitor of the sodium‐calcium exchanger with positive inotropic activity Otsomaa, Leena Levijoki, Jouko Wohlfahrt, Gerd Chapman, Hugh Koivisto, Ari‐Pekka Syrjänen, Kaisa Koskelainen, Tuula Peltokorpi, Saara‐Elisa Finckenberg, Piet Heikkilä, Aira Abi‐Gerges, Najah Ghetti, Andre Miller, Paul E. Page, Guy Mervaala, Eero Nagy, Norbert Kohajda, Zsófia Jost, Norbert Virág, László Varró, András Papp, Julius Gy. Br J Pharmacol Research Papers BACKGROUND AND PURPOSE: The lack of selective sodium–calcium exchanger (NCX) inhibitors has hampered the exploration of physiological and pathophysiological roles of cardiac NCX 1.1. We aimed to discover more potent and selective drug like NCX 1.1 inhibitor. EXPERIMENTAL APPROACH: A flavan series‐based pharmacophore model was constructed. Virtual screening helped us identify a novel scaffold for NCX inhibition. A distinctively different NCX 1.1 inhibitor, ORM‐11372, was discovered after lead optimization. Its potency against human and rat NCX 1.1 and selectivity against other ion channels was assessed. The cardiovascular effects of ORM‐11372 were studied in normal and infarcted rats and rabbits. Human cardiac safety was studied ex vivo using human ventricular trabeculae. KEY RESULTS: ORM‐11372 inhibited human NCX 1.1 reverse and forward currents; IC(50) values were 5 and 6 nM respectively. ORM‐11372 inhibited human cardiac sodium 1.5 (I (Na)) and hERG K(V)11.1 currents (I (hERG)) in a concentration‐dependent manner; IC(50) values were 23.2 and 10.0 μM. ORM‐11372 caused no changes in action potential duration; short‐term variability and triangulation were observed for concentrations of up to 10 μM. ORM‐11372 induced positive inotropic effects of 18 ± 6% and 35 ± 8% in anaesthetized rats with myocardial infarctions and in healthy rabbits respectively; no other haemodynamic effects were observed, except improved relaxation at the lowest dose. CONCLUSION AND IMPLICATIONS: ORM‐11372, a unique, novel, and potent inhibitor of human and rat NCX 1.1, is a positive inotropic compound. NCX inhibition can induce clinically relevant improvements in left ventricular contractions without affecting relaxation, heart rate, or BP, without pro‐arrhythmic risk. John Wiley and Sons Inc. 2020-11-10 2020-12 /pmc/articles/PMC7707092/ /pubmed/32959887 http://dx.doi.org/10.1111/bph.15257 Text en © 2020 The Authors. British Journal of Clinical Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited. |
spellingShingle | Research Papers Otsomaa, Leena Levijoki, Jouko Wohlfahrt, Gerd Chapman, Hugh Koivisto, Ari‐Pekka Syrjänen, Kaisa Koskelainen, Tuula Peltokorpi, Saara‐Elisa Finckenberg, Piet Heikkilä, Aira Abi‐Gerges, Najah Ghetti, Andre Miller, Paul E. Page, Guy Mervaala, Eero Nagy, Norbert Kohajda, Zsófia Jost, Norbert Virág, László Varró, András Papp, Julius Gy. Discovery and characterization of ORM‐11372, a novel inhibitor of the sodium‐calcium exchanger with positive inotropic activity |
title | Discovery and characterization of ORM‐11372, a novel inhibitor of the sodium‐calcium exchanger with positive inotropic activity |
title_full | Discovery and characterization of ORM‐11372, a novel inhibitor of the sodium‐calcium exchanger with positive inotropic activity |
title_fullStr | Discovery and characterization of ORM‐11372, a novel inhibitor of the sodium‐calcium exchanger with positive inotropic activity |
title_full_unstemmed | Discovery and characterization of ORM‐11372, a novel inhibitor of the sodium‐calcium exchanger with positive inotropic activity |
title_short | Discovery and characterization of ORM‐11372, a novel inhibitor of the sodium‐calcium exchanger with positive inotropic activity |
title_sort | discovery and characterization of orm‐11372, a novel inhibitor of the sodium‐calcium exchanger with positive inotropic activity |
topic | Research Papers |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7707092/ https://www.ncbi.nlm.nih.gov/pubmed/32959887 http://dx.doi.org/10.1111/bph.15257 |
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