Clinical efficacy of a benazepril and spironolactone combination in dogs with congestive heart failure due to myxomatous mitral valve disease: The BEnazepril Spironolactone STudy (BESST)

Melissa Coffman; Emilie Guillot; Thomas Blondel; Catherine Garelli-Paar; Shuo Feng; Susanne Heartsill; Clarke E Atkins

doi:10.1111/jvim.16155

Clinical efficacy of a benazepril and spironolactone combination in dogs with congestive heart failure due to myxomatous mitral valve disease: The BEnazepril Spironolactone STudy (BESST)

J Vet Intern Med. 2021 Jul;35(4):1673-1687. doi: 10.1111/jvim.16155. Epub 2021 May 24.

Authors

Melissa Coffman¹, Emilie Guillot², Thomas Blondel³, Catherine Garelli-Paar², Shuo Feng⁴, Susanne Heartsill⁵, Clarke E Atkins⁶

Affiliations

¹ Pharmaceutical Innovation & Development, Ceva Animal Health, Lenexa, Kansas, USA.
² Companion Animal Franchise, Ceva Santé Animale, Libourne, France.
³ Innovation & Development, Ceva Santé Animale, Libourne, France.
⁴ Innovation & Development, Ceva Biomune, Lenexa, Kansas, USA.
⁵ Veterinary Services, Ceva Animal Health, Lenexa, Kansas, USA.
⁶ Department of Clinical Sciences, College of Veterinary Medicine, North Carolina State University, Raleigh, North Carolina, USA.

Abstract

Background: The renin-angiotensin-aldosterone system (RAAS), when chronically activated, is harmful and RAAS-suppressive drugs are beneficial in the treatment of congestive heart failure (CHF). Mineralocorticoid receptor antagonists are widely used in the treatment of CHF in people.

Hypothesis/objectives: To determine if a mineralocorticoid receptor antagonist (spironolactone) is beneficial and safe in CHF due to myxomatous mitral valve disease (MMVD) of varying severity, we hypothesized that, when combined with furosemide, a combination product (S+BNZ) containing the ACE inhibitor (ACE-I), benazepril, and spironolactone, would be superior to benazepril alone.

Animals: Five hundred and sixty-nine client-owned dogs, with MMVD and CHF (ACVIM Stage C) of ≤10-days' duration.

Methods: After initial stabilization, dogs were randomized into a positive-controlled, double-blind, multicenter trial, to receive furosemide plus S+BNZ or furosemide plus benazepril. The primary outcome variable was the percentage of dogs reaching cardiac endpoint before Day 360. Cardiac endpoint was defined as cardiac death or euthanasia, recurrence of pulmonary edema, necessity for nonauthorized cardiac drug(s) or a furosemide dosage >8 mg/kg/d.

Results: A significantly lower percentage of dogs treated with S+BNZ reached the primary outcome variable by Day 360 (OR = 0.56; 95% CI, 0.32-0.98; P = .04) and risk of dying or worsening from cardiac causes, was significantly reduced (HR = 0.73; 95% CI = 0.59-0.89, P = .002) vs benazepril alone. Adverse events, potentially associated with treatment, were rare and equal between groups.

Conclusion and clinical importance: The combination of S+BNZ is effective, safe, and superior to benazepril alone, when used with furosemide for the management of mild, moderate or severe CHF caused by MMVD in dogs.

Keywords: ACE inhibitor; MRA; RAAS; aldosterone breakthrough; mitral regurgitation.

Publication types

Multicenter Study
Randomized Controlled Trial, Veterinary

MeSH terms

Animals
Benzazepines
Dog Diseases* / drug therapy
Dogs
Heart Failure* / drug therapy
Heart Failure* / veterinary
Mitral Valve
Spironolactone / therapeutic use
Treatment Outcome

Substances

Benzazepines
Spironolactone
benazepril

Grants and funding

Ceva Santé Animale