Covariate determinants of effective dosing regimens for time-dependent beta-lactam antibiotics for critically ill patients.

BIOMEDICAL PAPERS-OLOMOUC(2018)

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Abstract
Aims. Critically ill patients undergoing aggressive fluid resuscitation and treated empirically with hydrosoluble time-dependent beta-lactam antibiotics are at risk for sub-therapeutic plasma concentrations. The aim of this study was to assess the impact of two covariates - creatinine clearance (Cl-cr) and cumulative fluid balance (CFB) on pharmacokinetics/pharmacodynamics (PK/PD) target attainment within a week of treatment with meropenem (ME) or piperacillin/tazobactam (PIP/TZB). Methods. In this prospective observational pharmacokinetic (PK) study, 18 critically ill patients admitted to a surgical Intensive Care Unit (ICU) were enrolled. The primary PK/PD target was free antibiotic concentrations above MIC at 100% of the dosing interval (100% fT > MIC) to obtain maximum bactericidal activity. Drug concentration was measured using liquid chromatography-tandem mass spectrometry. Results. The treatment of both 8 septic patients with IV extended ME dosing 2 g/3 h q8 h and 10 polytraumatized patients with IV intermittent PIP/TZB dosing 4.0/0.5 g q8 h was monitored. 8/18 patients (44%) manifested augmented renal clearence (ARC) where Cl-cr >= 130 mL/min/1.73 m(2). Maximum changes were reported on days 2-3: the median positive CFB followed by the large median volume of distribution: Vd(me) = 70.3 L (41.9-101.5), Vd(pip) = 46.8 L (39.7-60.0). 100%fT(me) > MIC was achieved in all patients on ME (aged >= 60 years), and only in two patients (non-ARC, aged >= 65 years) out of 10 on PIP/TZB. A mixed model analysis revealed positive relationship of CFBpip with Vd(pip) (P = 0.021). Conclusion. Assuming that the positive correlation between CFB and Vd exists for piperacillin in the setting of the pathological state, then CFB should predict Vd(pip) across subjects at each and every time point.
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Key words
beta-lactam antibiotics,meropenem,piperacillin,pharmacokinetics/pharmacodynamics target,critically ill patient
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