SAR340835, a Novel Selective Na+/Ca2+ Exchanger Inhibitor, Improves Cardiac Function and Restores Sympathovagal Balance in Heart Failure

Michel Pelat; Fabrice Barbe; Cyril Daveu; Laetitia Ly-Nguyen; Thomas Lartigue; Suzanne Marque; Georges Tavares; Véronique Ballet; Jean-Michel Guillon; Klaus Steinmeyer; Klaus Wirth; Heinz Gögelein; Petra Arndt; Nils Rackelmann; John Weston; Patrice Bellevergue; Gary McCort; Marc Trellu; Laurence Lucats; Philippe Beauverger; Marie-Pierre Pruniaux-Harnist; Philip Janiak; Frédérique Chézalviel-Guilbert

doi:10.1124/jpet.120.000238

SAR340835, a Novel Selective Na⁺/Ca²⁺ Exchanger Inhibitor, Improves Cardiac Function and Restores Sympathovagal Balance in Heart Failure

J Pharmacol Exp Ther. 2021 May;377(2):293-304. doi: 10.1124/jpet.120.000238. Epub 2021 Feb 18.

Authors

Michel Pelat¹, Fabrice Barbe¹, Cyril Daveu¹, Laetitia Ly-Nguyen¹, Thomas Lartigue¹, Suzanne Marque¹, Georges Tavares¹, Véronique Ballet¹, Jean-Michel Guillon¹, Klaus Steinmeyer¹, Klaus Wirth¹, Heinz Gögelein¹, Petra Arndt¹, Nils Rackelmann¹, John Weston¹, Patrice Bellevergue¹, Gary McCort¹, Marc Trellu¹, Laurence Lucats¹, Philippe Beauverger¹, Marie-Pierre Pruniaux-Harnist¹, Philip Janiak¹, Frédérique Chézalviel-Guilbert²

Affiliations

¹ Cardiovascular and Metabolism TSU (M.P., F.B., C.D., T.L., S.M., G.T., L.L., Ph.B., M.-P.P.-H., P.J., F.C.-G.) and Integrated Drug Discovery (Pa.B.), Sanofi R&D, Chilly Mazarin, France; Preclinical Safety, Sanofi R&D, Alfortville, France (L.L.-N., V.B., J.-M.G., M.T.); Sanofi R&D, Industriepark Höchst, Frankfurt, Germany (K.S., K.W., H.G., P.A., N.R., J.W.); and Integrated Drug Discovery, Sanofi R&D, Vitry sur Seine, France (G.M.).
² Cardiovascular and Metabolism TSU (M.P., F.B., C.D., T.L., S.M., G.T., L.L., Ph.B., M.-P.P.-H., P.J., F.C.-G.) and Integrated Drug Discovery (Pa.B.), Sanofi R&D, Chilly Mazarin, France; Preclinical Safety, Sanofi R&D, Alfortville, France (L.L.-N., V.B., J.-M.G., M.T.); Sanofi R&D, Industriepark Höchst, Frankfurt, Germany (K.S., K.W., H.G., P.A., N.R., J.W.); and Integrated Drug Discovery, Sanofi R&D, Vitry sur Seine, France (G.M.) frederique.guilbert@sanofi.com.

PMID: 33602875
DOI: 10.1124/jpet.120.000238

Abstract

In failing hearts, Na⁺/Ca²⁺ exchanger (NCX) overactivity contributes to Ca²⁺ depletion, leading to contractile dysfunction. Inhibition of NCX is expected to normalize Ca²⁺ mishandling, to limit afterdepolarization-related arrhythmias, and to improve cardiac function in heart failure (HF). SAR340835/SAR296968 is a selective NCX inhibitor for all NCX isoforms across species, including human, with no effect on the native voltage-dependent calcium and sodium currents in vitro. Additionally, it showed in vitro and in vivo antiarrhythmic properties in several models of early and delayed afterdepolarization-related arrhythmias. Its effect on cardiac function was studied under intravenous infusion at 250,750 or 1500 µg/kg per hour in dogs, which were either normal or submitted to chronic ventricular pacing at 240 bpm (HF dogs). HF dogs were infused with the reference inotrope dobutamine (10 µg/kg per minute, i.v.). In normal dogs, NCX inhibitor increased cardiac contractility (dP/dt_max) and stroke volume (SV) and tended to reduce heart rate (HR). In HF dogs, NCX inhibitor significantly and dose-dependently increased SV from the first dose (+28.5%, +48.8%, and +62% at 250, 750, and 1500 µg/kg per hour, respectively) while significantly increasing dP/dt_max only at 1500 (+33%). Furthermore, NCX inhibitor significantly restored sympathovagal balance and spontaneous baroreflex sensitivity (BRS) from the first dose and reduced HR at the highest dose. In HF dogs, dobutamine significantly increased dP/dt_max and SV (+68.8%) but did not change HR, sympathovagal balance, or BRS. Overall, SAR340835, a selective potent NCX inhibitor, displayed a unique therapeutic profile, combining antiarrhythmic properties, capacity to restore systolic function, sympathovagal balance, and BRS in HF dogs. NCX inhibitors may offer new therapeutic options for acute HF treatment. SIGNIFICANCE STATEMENT: HF is facing growing health and economic burden. Moreover, patients hospitalized for acute heart failure are at high risk of decompensation recurrence, and no current acute decompensated HF therapy definitively improved outcomes. A new potent, Na⁺/Ca²⁺ exchanger inhibitor SAR340835 with antiarrhythmic properties improved systolic function of failing hearts without creating hypotension, while reducing heart rate and restoring sympathovagal balance. SAR340835 may offer a unique and attractive pharmacological profile for patients with acute heart failure as compared with current inotrope, such as dobutamine.

MeSH terms

Animals
Baroreflex
Dogs
Heart / drug effects
Heart Failure / drug therapy*
Heart Rate
Membrane Transport Modulators / administration & dosage
Membrane Transport Modulators / pharmacology
Membrane Transport Modulators / therapeutic use*
Myocardial Contraction
Myocardium / metabolism
Sodium-Calcium Exchanger / antagonists & inhibitors*
Swine
Vagus Nerve / drug effects*

Substances

Membrane Transport Modulators
Sodium-Calcium Exchanger