Background Although measurement of drug serum levels is an objective direct method for testing compliance, it can be distorted by "white-coat compliance" or by variations in drug elimination. Objective The aim of this prospective study was to evaluate the prevalence of noncompliance with perindopril therapy in adult out-patients using pharmacokinetic simulations. The additional aim was to compare the predictive performance of two glomerular filtration rate markers-creatinine and cystatin C. Setting Department of Cardiology, Tomas Bata Regional Hospital in Zlín, Czech Republic. Method Perindoprilat pharmacokinetic models individualized according to patient characteristics were compared with measured perindoprilat serum concentrations to document compliance. Linear regression was used to evaluate the relations between perindoprilat clearance and glomerular filtration rate estimated using creatinine and cystatin C. Main outcome measure Assessment of non-compliance with medication using drug concentration measurements reinforced with therapeutic drug monitoring. Results Non-detectable perindoprilat levels were observed in 26.1% of patients. Another 21.7% were classified as non-compliant based on therapeutic drug monitoring pharmacokinetic simulations. Volume of distribution, clearance and half-life median value (interquarti°range) for perindoprilat were 408.3 (360.4-456.8) L, 10.1 (4.9-17.0) L h-1 and 24.7 (19.4-62.7) h, respectively. Linear regression models showed tight relationship between cystatin C and perindoprilat clearance. Conclusions Assessment of adherence with medication reinforced with therapeutic drug monitoring and pharmacokinetic simulations is proposed as an optimal method reducing disadvantages of simple drug concentration measurements. Cystatin C proves to be better surrogate marker for perindoprilat elimination than creatinine.

Department of Clinical Biochemistry and Pharmacology Tomas Bata Regional Hospital Zlín Czech Republic

Department of Pharmacology 1st Faculty of Medicine Charles University and General University Hospital Prague Prague Czech Republic

Department of Pharmacy Tomas Bata Regional Hospital Zlín Czech Republic

Institute of Forensic Medicine and Toxicology 1st Faculty of Medicine Charles University and General University Hospital Prague Prague Czech Republic

Zobrazit více v PubMed

Clin Chem. 2015 Oct;61(10):1265-72 PubMed

Clin Chem. 2002 May;48(5):699-707 PubMed

Hypertens Res. 2011 Jan;34(1):87-90 PubMed

Br J Clin Pharmacol. 2015 Jul;80(1):20-7 PubMed

N Engl J Med. 2012 Jul 5;367(1):20-9 PubMed

Br J Clin Pharmacol. 1998 Aug;46(2):95-9 PubMed

N Engl J Med. 2005 Aug 4;353(5):487-97 PubMed

Medicine (Baltimore). 2017 Jan;96(4):e5641 PubMed

Ther Adv Chronic Dis. 2012 Sep;3(5):231-6 PubMed

J Hypertens. 2013 Dec;31(12):2455-61 PubMed

Nephrol Dial Transplant. 2003 Oct;18(10):2024-31 PubMed

Br J Clin Pharmacol. 1991 Aug;32(2):187-92 PubMed

Intern Med J. 2016 Mar;46(3):364-72 PubMed

Vancomycin population pharmacokinetics and dosing proposal for the initial treatment in obese adult patients