Effect of nesiritide on renal function in patients admitted for decompensated heart failure

doi:10.1093/qjmed/hcm089

QJM 2007 100(11):699-706; doi:10.1093/qjmed/hcm089

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Effect of nesiritide on renal function in patients admitted for decompensated heart failure

S. Arora¹, K. Clarke², V. Srinivasan¹ and A. Gradman¹

From the Departments of ¹Cardiovascular Disease and ²Internal Medicine, Western Pennsylvania Hospital/Temple University, Pittsburgh, USA

Address correspondence to Dr S. Arora, Department of Cardiovascular Disease, Suite 3411 North Western Pennsylvania Hospital/Temple University Program, 4800 Friendship Avenue, Pittsburgh, PA 15224, USA. email: sandeeparora24{at}hotmail.com

Received 13 May 2007 Accepted for publication 11 July 2007.

Abstract

Background: Studies addressing the effect of nesiritide on renalfunction in patients hospitalized for decompensated heart failure(HF) are limited, with conflicting results.

Aim: To study the effect of nesiritide on renal function inpatients admitted for acute decompensated HF.

Methods: We retrospectively reviewed charts of patients admittedwith decompensated HF, comparing those who received nesiritidealong with conventional therapy vs. those who received conventionaltherapy alone. Serum creatinine levels and body weight weremeasured on admission, and were compared with levels at day3 to estimate deterioration in renal function. Worsening renalfunction (WRF) was defined as a rise in serum creatinine of $>=$ 0.3 mg/dl from baseline, with final creatinine level >1.5mg/dl.

Results: We reviewed 206 charts (116 controls, 90 nesiritidegroup). WRF developed in 28/90 (31.1%) in the nesiritide groupand 37/116 (31.9%) controls (p = 1.0). Mean change in creatininein the nesiritide group was 0.15 ± 0.37 mg/dl, comparedto 0.17 ± 0.25 mg/dl in controls (p = 0.75). Using analternative cut-off increase in serum creatinine of $>=$ 0.5 mg/dl,16/90 (17.7%) patients in the nesiritide group developed WRFcompared to 18/116 (15.5%) controls (p = 0.80). If WRF was definedas elevation in serum creatinine levels by $>=$ 0.3 mg/dl anytimeduring hospitalization, the incidence of WRF in the nesiritidegroup remained similar to that of controls (42.2% vs. 41.3%,p = 0.90). On multivariate analysis, nesiritide therapy wasnot associated with WRF (OR 0.8, 95% CI 0.4–1.6, p = 0.48).

Discussion: We failed to detect any significant risk of WRFin patients treated with nesiritide compared to conventionaltherapy in patients with decompensated HF during index hospitalization.Larger randomized, placebo-controlled trials are required tofurther elucidate the effect of nesiritide on renal functionin these patients.

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