Renin‐angiotensin aldosterone profile before and after angiotensin‐converting enzyme‐inhibitor administration in dogs with angiotensin‐converting enzyme gene polymorphism

Darcy Adin; Clarke Atkins; Oliver Domenig; Teresa DeFrancesco; Bruce Keene; Sandra Tou; Joshua A. Stern; Kathryn M. Meurs

doi:10.1111/jvim.15746

Journal of Veterinary Internal Medicine (Mar 2020)

Renin‐angiotensin aldosterone profile before and after angiotensin‐converting enzyme‐inhibitor administration in dogs with angiotensin‐converting enzyme gene polymorphism

Darcy Adin,
Clarke Atkins,
Oliver Domenig,
Teresa DeFrancesco,
Bruce Keene,
Sandra Tou,
Joshua A. Stern,
Kathryn M. Meurs

Affiliations

Darcy Adin: College of Veterinary Medicine University of Florida Gainesville Florida
Clarke Atkins: College of Veterinary Medicine, North Carolina State University Raleigh North Carolina
Oliver Domenig: Attoquant Diagnostics Vienna Austria
Teresa DeFrancesco: College of Veterinary Medicine, North Carolina State University Raleigh North Carolina
Bruce Keene: College of Veterinary Medicine, North Carolina State University Raleigh North Carolina
Sandra Tou: College of Veterinary Medicine, North Carolina State University Raleigh North Carolina
Joshua A. Stern: Department of Medicine and Epidemiology School of Veterinary Medicine, University of California Davis California
Kathryn M. Meurs: College of Veterinary Medicine, North Carolina State University Raleigh North Carolina

DOI: https://doi.org/10.1111/jvim.15746
Journal volume & issue: Vol. 34, no. 2
pp. 600 – 606

Abstract

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Abstract Background An angiotensin‐converting enzyme (ACE) gene polymorphism occurs in dogs; however, functional importance is not well studied. Hypothesis We hypothesized that dogs with the polymorphism would show alternative renin‐angiotensin aldosterone system (RAAS) pathway activation and classical RAAS pathway suppression before and after ACE‐inhibitor administration, as compared to dogs without the polymorphism that would show this pattern only after ACE‐inhibitor administration. Animals Twenty‐one dogs with mitral valve disease that were genotyped for the ACE gene polymorphism. Methods This retrospective study utilized stored samples from 8 ACE gene polymorphism‐negative (PN) dogs and 13 ACE gene polymorphism‐positive (PP) dogs before and after enalapril administration. Equilibrium analysis was performed to evaluate serum RAAS metabolites and enzyme activities. Results were compared before and after enalapril, and between groups. Results The classical RAAS pathway was suppressed and the alternative RAAS pathway was enhanced for both genotypes after administration of enalapril, with no differences before enalapril administration. Aldosterone breakthrough occurred in both PN (38%) and PP (54%) dogs despite angiotensin II suppression. Aldosterone was significantly higher (P = .02) in ACE gene PP dogs (median, 92.17 pM; IQR, 21.85‐184.70) compared to ACE gene PN dogs (median, 15.91 pM; IQR, <15.00‐33.92) after enalapril. Conclusions and Clinical Importance The ACE gene polymorphism did not alter baseline RAAS activity. Aldosterone breatkthrough in some dogs suggests nonangiotensin mediated aldosterone production that might be negatively influenced by genotype. These results support the use of aldosterone receptor antagonists with ACE‐inhibitors when RAAS inhibition is indicated for dogs, especially those positive for the ACE gene polymorphism.

Published in Journal of Veterinary Internal Medicine

ISSN: 0891-6640 (Print); 1939-1676 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Agriculture: Animal culture: Veterinary medicine
Website: https://onlinelibrary.wiley.com/journal/19391676

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