Effect of Allopurinol on Mortality and Hospitalisations in Chronic Heart Failure: a Retrospective Cohort Study

Overview

Journal Heart

Date 2002 Feb 16

PMID 11847159

Citations 38

Authors

A D Struthers

P T Donnan

P Lindsay

D McNaughton

J Broomhall

T M MacDonald

Affiliations

Soon will be listed here.

Abstract

Objective: To examine whether allopurinol is associated with any alteration in mortality and hospitalisations in patients with chronic heart failure (CHF). This hypothesis is based on previous data that a high urate concentration is independently associated with mortality with a risk ratio of 4.23 in CHF.

Design: Retrospective cohort study.

Setting: Medicines Monitoring Unit, Ninewells Hospital, Dundee, UK.

Patients: 1760 CHF patients divided into four groups: those on no allopurinol, those on long term low dose allopurinol, those on short term low dose allopurinol, and those on long term high dose allopurinol.

Main Outcome Measures: Total mortality, cardiovascular mortality, cardiovascular hospitalisations, cardiovascular mortality or hospitalisations.

Results: Long term low dose allopurinol was associated with a significant worsening in mortality over those who never received allopurinol (relative risk 2.04, 95% confidence interval (CI) 1.48 to 2.81). This may be because low dose allopurinol is insufficient to negate the adverse effect of a high urate concentration. However, long term high dose (> or = 300 mg/day) allopurinol was associated with a significantly better mortality than longstanding low dose allopurinol (relative risk 0.59, 95% CI 0.37 to 0.95). This may mean that high dose allopurinol can fully negate the adverse effect of urate and return the mortality to normal.

Conclusions: Long term high dose allopurinol may be associated with a better mortality than long term low dose allopurinol in patients with CHF because of a dose related beneficial effect of allopurinol against the well described adverse effect of urate. Further work is required to substantiate or refute this finding.

Citing Articles

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Yokota T, Kinugawa S, Fukushima A, Okumura T, Murohara T, Tsutsui H Heart Vessels. 2024; 40(2):111-122.

PMID: 39158751 DOI: 10.1007/s00380-024-02448-9.

Uric acid is a biomarker for heart failure, but not therapeutic target: result from a comprehensive meta-analysis.

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Nishino M, Egami Y, Nakamura H, Ukita K, Kawamura A, Matsuhiro Y Health Sci Rep. 2022; 5(2):e563.

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Wu J, Dong E, Zhang Y, Xiao H Front Physiol. 2021; 12:709703.

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