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Volume 2, Number 4, December 2001
High serum enalaprilat in chronic renal failure Thomas Elung-Jensen, Jens Heisterberg, Anne-Lise Kamper, Jesper Sonne, Svend Strandgaard, Niels Erik Larsen Background:
Most angiotensin-converting
enzyme (ACE) inhibitors and their metabolites are excreted renally and doses should
hence be reduced in renal insufficiency. We studied whether the dosage of enalapril
in daily clinical practice is associated with drug accumulation of enalaprilat
in chronic renal failure.
Methods:
Fifty nine out-patients with
plasma creatinine >150 μmol/L and chronic antihypertensive treatment with
enalapril were investigated, in a cross-sectional design.
Results:
Median glomerular filtration
rate (GFR) was 23 (range 6–60) ml/minute/1.73 m2. The daily dose
of enalapril was 10 (2.5–20) mg and the trough serum concentration of enalaprilat
was 31.8 (<2.5–584.7) ng/ml. Ninety percent of the patients had higher
serum concentrations of enalaprilat than has been reported in subjects with normal
kidney function, and a marked elevation of serum enalaprilat was observed in patients
with GFR <30 ml/minute. All but three patients had serum ACE activity below the
reference range. The ACE genotype did not influence the results. Additional pharmacokinetic
studies were done in nine patients in whom GFR was 23 (10–42) ml/minute/1.73
m2. The median clearance of enalaprilat was 28 (16–68) ml/minute
and correlated linearly with GFR (r=0.86, p=0.003). Intra-subject day-to-day
variation in trough concentrations was 19.7%.
Conclusion:
Patients with chronic renal
failure given small or moderately high doses of enalapril may thus have markedly
elevated levels of serum enalaprilat. Whether this affords extra renoprotection,
or on the contrary may inappropriately impair renal function, is not known, and
should be investigated in prospective, controlled studies. JRAAS 2001;2:240-245. View full PDF article (open in new window) Email this article Right click on this DOI link and copy link to cite this article (What is a DOI link?)
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