A cross-sectional study of the effects of β-blocker therapy on the interpretation of the aldosterone/renin ratio: can dosing regimen predict effect? : Journal of Hypertension

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ORIGINAL PAPERS: Aldosteronism

A cross-sectional study of the effects of β-blocker therapy on the interpretation of the aldosterone/renin ratio

can dosing regimen predict effect?

Griffin, Tomás P.a,b; Browne, Gerard A.a; Wall, Deirdrec; Dennedy, Michael C.a,b; O'Shea, Paula M.d

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Journal of Hypertension 34(2):p 307-315, February 2016. | DOI: 10.1097/HJH.0000000000000775

Abstract

Context and aim: 

Aldosterone/renin ratio (ARR) is used as the primary screening tool for primary aldosteronism. Its interpretation is often challenging because of the interference of antihypertensive medication. β-blocker therapy suppresses renin production by inhibiting β-adrenergic receptors in the juxtaglomerular apparatus of the kidney and consequently aldosterone secretion (to a lesser extent). Therefore, β-blocker therapy has the potential to elevate the ARR. The aim of this study was to investigate whether or not the effect of β-blocker therapy on the ARR could be predicted from the dosing regimen.

Methods: 

A prospective cross-sectional study was conducted. Participants were stratified into one of four groups (control/low/medium/high) based on the quantity of β-blocker prescribed. ARR was calculated from renin/aldosterone, measured using two assay systems.

Results: 

Eighty-nine volunteers were recruited to our study. In the control group, zero patients had a positive ARR using plasma renin activity (PRA)/direct renin concentration (DRC). In the low, medium, and high-dose β-blocker groups between 8–25% of patients demonstrated screen positive ARR results for primary aldosteronism using DRC and PRA. DRC was significantly lower in patients in the medium/high-dose groups and PRA significantly lower in the low/medium/high-dose groups compared with controls. ARR using DRC was significantly higher in the medium/high-dose groups and ARR using PRA was significantly higher in the low/medium/high-dose groups compared with controls.

Conclusion: 

Our study suggests that β-blocker therapy is associated with an increased risk of positive ARR screens for primary aldosteronism irrespective of the dose of β-blocker prescribed, in patients in whom it is clinically reasonable to expect that primary aldosteronism may be present.

Copyright © 2016 Wolters Kluwer Health, Inc. All rights reserved.

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