Background. The optimal drug dosing in anuric patients undergoing continuous haemofiltration is a difficult task. More pharmacokinetic data is needed to derive practical guidelines for dosage adjustments. Methods. Drug elimination of various antimicrobial agents (amikacin, amoxycillin, ceftazidime, ciprofloxacin flucloxacillin, imipenem, netilmicin, penicillin G, piperacillin, sulphamethoxazole, tobramycin, vancomycin) was studied in 24 patients with acute renal failure treated by pump-assisted continuous venovenous haemofiltration (CVVH). Concentrations of serial blood and ultrafiltrate samples were determined by HPLC or by fluorescence polarization immunoassay. Total body clearance (CL) and haemofilter clearance (CLf) rates were determined by standard model-independent equations. Data from published literature on fractions not bound to proteins (fu), non-renal drug clearance fractions (Qo) and normal clearance values (CLn) were used to derive a pharmacokinetic model, taking into account drug removal by ultrafiltration and by non-renal clearance. Results. A total of 37 treatment periods was studied. Blood flow through the haemofilters was 100 ml/min resulting in an average ultrafiltrate flow rate (UFR) of 13.2±4.6 (range 3.2-22.1) ml/min. Acceptable correlations of calculated and measured haemofilter clearances and total body clearances were obtained. Conclusions. Total body clearance in anuric patients during CVVH is predictable from drug properties, which are generally known. The individual dosage requirements may be calculated by multiplying Qo+fu UFR/CLn with the dose considered appropriate in the absence of renal impairmen

Joos, B.

Keusch, G.

Schmidli, M.

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Nephrol Dial Transplant (1996) 11: 1582-1585Original ArticleIMephrologyDialysisTransplantationPharmacokinetics of antimicrobial agents in anuric patients duringcontinuous venovenous haemofiltrationB. Joos, M. Schmidli and G. KeuschDepartment of Medicine, University Hospital, Zurich, SwitzerlandAbstractBackground. The optimal drug dosing in anuricpatients undergoing continuous haemofiltration is adifficult task. More pharmacokinetic data is needed toderive practical guidelines for dosage adjustments.Methods. Drug elimination of various antimicrobialagents (amikacin, amoxycillin, ceftazidime, ciproflox-acin, flucloxacillin, imipenem, netilmicin, penicillin G,piperacillin, sulphamethoxazole, tobramycin, vanco-mycin) was studied in 24 patients with acute renalfailure treated by pump-assisted continuous venoven-ous haemofiltration (CVVH). Concentrations of serialblood and ultrafiltrate samples were determined byHPLC or by fluorescence polarization immunoassay.Total body clearance (CL) and haemofilter clearance(CLf) rates were determined by standard model-independent equations. Data from published literatureon fractions not bound to proteins (fu), non-renal drugclearance fractions (Qo), and normal clearance values(CLn) were used to derive a pharmacokinetic model,taking into account drug removal by ultrafiltrationand by non-renal clearance.Results. A total of 37 treatment periods was studied.Blood flow through the haemofilters was lOOml/minresulting in an average ultrafiltrate flow rate (UFR)of 13.2 + 4.6 (range 3.2-22.1) ml/min. Acceptable cor-relations of calculated and measured haemofilter clear-ances and total body clearances were obtained.Conclusions. Total body clearance in anuric patientsduring CVVH is predictable from drug properties,which are generally known. The individual dosagerequirements may be calculated by multiplyingQo + fu' UFR/CLn with the dose considered appro-priate in the absence of renal impairment.Key words: acute renal failure; antimicrobial agents;continuous venovenous haemofiltration; drug dosage;pharmacokineticsCorrespondence and offprint requests to: Dr Beda Joos, Division ofInfectious Diseases, Department of Medicine, University HospitalZurich, CH-8091 Zurich, Switzerland.IntroductionContinuous haemofiltration is a well-established toolin the treatment of patients with renal failure. However,despite good control of uraemia, acute renal failureis often associated with a high mortality rate [1].Septicaemia frequently complicates the disease progres-sion, and it has been identified as a major predictor ofa poor outcome. Optimal drug dosing is thus essentialin this situation but pharmacokinetic data during con-tinuous renal replacement therapy are scarce. Complexmathematical models have been proposed [2,3], buttheir application in clinical practice is limited. Thecurrent methods to estimate drug removal through thehaemofilter rely on sieving coefficients, i.e. averagefiltrate to blood concentration ratios [2-5]. Thesevalues, however, must be determined previously foreach drug.The aim of this study is to investigate the pharmaco-kinetics of various antimicrobial agents in patientswith acute renal failure undergoing pump-assisted con-tinuous venovenous haemofiltration (CVVH) and toderive practical guidelines for dosage adjustments.Subjects and methodsSelection of patientsAnuric patients undergoing continuous renal replacementtherapy and receiving antimicrobial chemotherapy were con-sidered eligible for inclusion in the study. Drug clearancerates were measured during the CWH in a total of 24patients with acute renal failure due to various causes.HaemofiltrationPump-assisted CWH was performed by a double-lumensubclavian catheter [1]. Blood flow through the polyamidehollow-fibre membrane filters (Gambro FH66) was set at100 ml/min. The replacement fluid (Ringer's lactate) wasadministered in pre-dilution or post-dilution mode. Theultrafiltrate flow rate (UFR) was continuously monitoredthroughout treatment.© 1996 European Dialysis and Transplant Association-European Renal AssociationPharmacokinetics during C W HTable 1. Dosage and median pharmacokinetic parameters observed in 24 patients during continuous venovenous haemofUtration1583DrugAmikacinAmoxycillinCeftazidimeCiprofloxacinFlucloxacillinImipenemNetilmicinPenicillin-GPiperacillinSulphamethoxazoleTobramycinVancomycinTotal, rangeNumber ofpatients236231618V1337bNumber ofintervals23133621021612464Dose(mg)600-800600-1200500-10002001000-200050040-20011981000-400040040500-100040-4000Interval(h)246-126-136-124-391224-7244-12122424-434-72Half-life(h)15.65.813.27.59.93.013.912.610.69.99.223.12.3-139CL-total(ml/min)263820231271392051566513349-286CL-filter(ml/min)161051424121110109171-27a Trimethoprim concentrations in haemofiltrate were below the limit of detection (<0.2 mg/1) in this patient.bTherapy consisted of 1—3 different drugs in individual patients, resulting in a total of 37 treatment periods.Dosage and administrationAntibiotics were administered intravenously either alone or incombination (Table 1). The choice of antimicrobial therapyfor each patient was based on clinical judgement only. Thedosing interval was chosen according to the presumed half-life of the respective drug.Up to three different drugs were administered to eachpatient during the study, resulting in a total of 37 evaluabletreatment periods. In many cases, several subsequent dosingintervals per drug and patient were studied (64 totally) inorder to obtain more reliable data and to ensure that asteady state was reached.Specimen collectionSerial blood samples and pooled ultrafiltrate were obtainedat various time points during the steady state. On the average,11 + 7 specimens were collected during each of the 37 treat-ment periods. The optimal timing of sample collection wasdetermined individually depending on the drug to be stud-ied and on the actual length of the dosing interval.Concentrations of imipenem were determined immediatelydue to its limited stability, while aminoglycoside and vanco-mycin levels were assayed within 24 h. All other serum andhaemofiltrate samples were stored together with appropriatecontrol standards at — 70°C for up to 3 months before beingmeasured in batch.Assay methodsConcentrations of beta-lactam antibiotics, ciprofloxacin, andsulphamethoxazole were determined by HPLC whereasthe aminoglycosides and vancomycin were measured by afluorescence polarization immunoassay (Abbott TDX).Pharmacokinetic analysisThe timing of the doses, dosing intervals, duration of infu-sion, and the volume of the ultrafiltrate produced per timeunit were recorded for each patient. A serum concentrationversus time profile was plotted for each dosing interval andthe area under the curve (AUC) was calculated by the log-trapezoidal method. The amount of drug excreted throughthe haemofilter during one dosing interval was calculatedfrom the volume of collected ultrafiltrate and the drugconcentration in the ultrafiltrate. Standard model-inde-pendent equations were applied to calculatetotal body clearance (CL = Dose/AUC) andfilter clearance (excreted amount/AUC).Selected drug properties such as protein binding (unboundfraction fu), non-renal drug clearance fraction (Qo), andnormal clearance values (CLn) were derived from publishedliterature [6-8] (Table 2).Statistical methodsThe correlations of calculated and measured clearances weredetermined by standardized principal component analysis[9], and by distribution independent regression analysisaccording to Passing and Bablok [10,11]. The latter modelestimates confidence intervals for slope and intercept andtests for linearity by cusum statistics and by the run test.The performance of the prediction method was determinedTable 2. Selected drug properties used to predict total body clearanceand haemofilter clearance [6—8]DrugAmikacinAmoxycillinCeftazidimeCiprofloxacinFlucloxacillinImipenemNetilmicinPenicillin-GPiperacillinSulphamethoxazoleTobramycinVancomycinRange0.960.870.850.70.20.750.960.60.840.61.00.90.2-1.0Qo80.020.060.050.50.30.30.010.080.250.80.020.050.01-0.8(ml/min)92372132500832339250018226777726-500afu, unbound fraction; Qo, non-renal drug clearance fraction; CLnnormal clearance.1584 B. Joos et al.by calculating bias and precision (root of mean squareddifferences) according to Sheiner and Beal [12].ResultsTwenty-four patients were included in the study.Approximately 50% of the patients experienced anacute renal failure due to various internal medicalcauses, e.g. septic shock, pneumonia, ARDS, pancreat-itis, hepatorenal syndrome. One-third of the patientssuffered from postoperative acute renal failure follow-ing either renal transplantation, combined renal andpancreas transplantation, or cardiac surgery. Theremaining patients had multiple traumatic lesions ortraumatic brain injury. Half of the patients were onthe internal and half on the surgical intensive careunit. All patients were attended by a nephrologist.The antimicrobial therapy used consisted of 12different antimicrobial agents given in a wide varietyof dosages either alone or in combination (Table 1).Serum and nitrate kinetics were studied during atotal of 37 treatments (64 dosing intervals). The aver-age ultrafiltrate flow rate was 13.2 ±4.6 ml/min(mean + SD, range 3.2-22.1).Using the fundamental pharmacokinetic drug para-meters observed in individuals without renal failure(Table 2), a theoretical model was derived which couldbe used to predict the clearance values. The measuredhaemofilter clearances and total body clearanceswere in good agreement with fu-UFR and withfu • UFR + Qo • Cln respectively. Figures 1 and 2 illus-trate the distribution of the observed values. Thequantity fu • UFR was a good predictor of filter clear-ance (Table 3). The majority of the measurementsdeviated by less than 15%. Total body clearance wasunderestimated by fu • UFR + Qo • Cln by an average of7.6 ml/min. Deviations were <33%, however, in themajority of the 37 treatment periods.1001000E11O10-100measured (ml/min)10 100measured (ml/min)1000Fig. 2. Measured and calculated total body clearance rates of 12different drugs during continuous venovenous haemofiltration (calcu-lated values were obtained from fu-UFR + Q0-CLn).Table 3. Comparison of measured and calculated haemofilter clear-ance and total body clearance values during 37 treatment periodsMethod Filter clearance"Predictive performance [12]:bias (ml/min)precision (rmseb)0.6 (-0.2, 1.4)2.4(1.7, 3.0)Standardized principal component analysis [9]:slopey-intercept (ml/min)0.941.3Distribution-independent regression analysis [10,slope0y-interceptc (ml/min)1.04(0.87, 1.24)0.56 (-1.3, 2.0)Total clearance8-7.6 (-16.4, 1.1)27.0(14.0, 35.6)1.03-8.91 ]:0.81 (0.57, 1.05)-2.0 (-9.9, 5.7)Fig. 1. Measured and calculated haemofilter clearance rates of 12different drugs during continuous venovenous haemofiltration (calcu-lated values were obtained from fu-UFR).* 95% confidence intervals are indicated in parentheses.b Root of mean squared prediction error.cNo statistically significant differences of slopes from 1 or ofintercepts from 0 (P<0.05) and no significant deviation fromlinearity as determined by the cusum and run tests (P>0.1).Comparison of the measured and calculated valuesfor both haemofilter and total body clearance bydistribution-independent linear regression analysisyielded slopes of approximately 1 and y-intercepts near0 ml/min (Table 3). No significant deviation from lin-earity was found by the cusum and run tests (P>0.\).DiscussionThe existing mathematical models used to estimatedrug elimination during continuous renal replacementtherapy have recently been reviewed by Reetze-Bonorden et al. [5]. Sieving coefficients are frequentlyused to characterize the ability of a drug to passthrough the haemofilter membrane. These values, how-Pharmacokinetics during CVVHever, have not been measured for all drugs used inpatients with acute renal failure.The approach presented in this study has the advant-age that all parameters needed to estimate drug clear-ance are readily available. The convective transportfrom blood to ultrafiltrate was calculated from ultrafil-trate flow rate and unbound fraction alone, and thenon-renal clearance was assumed to be the same as inpatients without renal impairment. This simple modelis far from being perfect. It is evident that proteinbinding may be altered in anuric patients and non-renal elimination may be impaired in these severely illpatients. Moreover, possible interactions due to mul-tiple drug therapy may be responsible for pharmaco-kinetic alterations. It is conceivable also that a reducedhepatic clearance may be in part compensated by lowerprotein binding and consequently increased haemofilterclearance and vice versa.Various statistical methods were used to comparepredicted with measured haemofilter and total bodyclearances. Evaluation of predictive performance [12]has become usual practice; however, this methoddemands an independent variable presumed to be freeof experimental error. Standardized principal compon-ent analysis [9] is a multivariate procedure, but normaldistribution of the values is required. Regression ana-lysis, according to Passing and Bablok [10,11], mayovercome these drawbacks since it does not depend onan error-free variable or on rigid distributional require-ments. In addition, this procedure tests for a linearrelationship between the two variables, confidencelimits are given for the slope and the intercept, andthe influence of outliers is minimized.The 12 drugs studied exhibited marked differencesin their protein binding as well as in their non-renalcontribution to total clearance. In addition wide rangesof dose, dosing intervals, and ultrafiltration rates werecovered. Nevertheless in most patients the proposedformula fu • UFR + Qo • CLn provided a reliable estimateof the total drug clearance. The individual dosagerequirements may be calculated in proportion to theratio of total body clearance observed during CVVHand the normal clearance rate found in patients withoutrenal impairment. Consequently the following formulamay be used to predict the maintenance dose duringrenal replacement therapy.Dose = Dn-(Q0 + fu-UFR/CLn)where Dn denotes normal dose, CLn normal clearance,Qo non-renal clearance fraction, fu unbound fraction,and UFR ultrafiltrate flow rate.In conclusion, the results of the present study allowpractical dosage recommendations to be made for1585anuric patients undergoing CWH. Most drugs usedin clinical practice have relatively low molecularweights, so that similar mechanisms of clearance duringCWH would be expected. It is therefore anticipatedthat the same dosage calculations will also be appro-priate for the majority of other therapeutic agents.Monitoring serum concentrations, however, remainsmandatory when using drugs which possess a narrowtherapeutic range. Prospective studies are needed toevaluate the efficiency of these dosage guidelines andto study specifically whether the desired drug concen-trations are achieved.Acknowledgements. The authors thank the nursing staff of themedical intensive care unit of the University Hospital Zurich fortheir invaluable assistance, and Peter Gowland for his helpful reviewof this manuscript.References1. Keusch G, Schreier P, Binswanger U. Outcome in critically illpatients with acute renal failure treated by continuous hemo-filtration. Contrib Nephrol 1991; 93: 57-602. Vincent HH, van Ittersum FJ, Akcahuseyin E, Vos MC, vanDuyl WA, Schalekamp MA. Solute transport in continuousarteriovenous hemodiafiltration: a new mathematical modelapplied to clinical data. Blood Purif 1990; 8: 149-1593. Kroh UF, Dehne M, El Abed K, Feussner KD, Hofmann W,Lennartz H. Drug dosage during continuous hemofiltration:pharmacokinetics and practical implications. Contrib Nephrol1991; 93: 127-1304. Golper TA, Wedel SK, Kaplan AA, Saad AM, Donta ST,Paganini EP. Drug removal during continuous arteriovenoushemofiltration: theory and clinical observations. Int J ArtifOrgans 1985; 8: 307-3125. Reetze-Bonorden P, Bohler J, Keller E. Drug dosage in patientsduring continuous renal replacement therapy. Pharmacokineticand therapeutic considerations. Clin Pharmacokinet 1993; 24:362-3796. Vozeh S, Schmidlin O, Taeschner W. Pharmacokinetic drugdata. Clin Pharmacokinet 1988; 15: 254-2827. Dettli L. Pharmakokinetische Daten filr die Dosisanpassung.In: Arzneimittel - Kompendium der Schweiz, Registerband.Documed, Basel, 1990: 331-3408. Walther H, Meyer FP. Klinische Pharmakologie anlibakteriellerArzneimittel. Urban & Schwarzenberg, Munchen, 19879. Feldmann U, Schneider B, Klinkers H, Haeckel R. A multivari-ate approach for the biometric comparison of analytical methodsin clinical chemistry. J Clin Chem Clm Biochem 1981; 19: 121 -13710. Passing H, Bablok W. A new biometrical procedure for testingthe equality of measurements from two different analyticalmethods. Application of linear regression procedures for methodcomparison studies in clinical chemistry, Part I. J Clin ChemClin Biochem 1983; 21: 709-72011. Passing H, Bablok W. Comparison of several regression proced-ures for method comparison studies and determination of samplesizes. Application of linear regression procedures for methodcomparison studies in clinical chemistry, Part II. J Clin ChemClin Biochem 1984; 22: 431-44512. Sheiner LB, Beal SL. Some suggestions for measuring predictiveperformance. J Pharmacokinet Biopharm 1981; 9: 503-512Received for publication: 22.1.96Accepted in revised form: 2.4.96

Pharmacokinetics of antimicrobial agents in anuric patients during continuous venovenous haemofiltration

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