BAYESIAN FORECASTING OF GENTAMICIN PHARMACOKINETICS IN PEDIATRIC INTENSIVE-CARE UNIT PATIENTS

被引：15

作者：

KRAUS, DM

DUSIK, CM

RODVOLD, KA

CAMPBELL, MM

KECSKES, SA

机构：

[1] UNIV ILLINOIS,COLL MED,DEPT PEDIAT,CHICAGO,IL 60680

[2] UNIV ILLINOIS,COLL MED,DEPT INFECT DIS,CHICAGO,IL 60680

来源：

PEDIATRIC INFECTIOUS DISEASE JOURNAL | 1993年 / 12卷 / 09期

关键词：

GENTAMICIN; PHARMACOKINETICS; PEDIATRIC INTENSIVE CARE; BAYESIAN FORECASTING; CRITICALLY ILL CHILDREN;

D O I：

10.1097/00006454-199309000-00002

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

The predictive performance of a one compartment Bayesian forecasting program was evaluated in pediatric intensive care unit patients with normal renal function. Gentamicin pharmacokinetic parameters were determined in 44 PICU patients (0.8 month to 14 years old) from all available serum concentrations and doses by nonlinear least squares regression. Population pharmacokinetic parameter estimates were established from 27 of the PICU patients. Mean prediction error (ME) and mean absolute error (MAE) for 2 future sets of peak and trough gentamicin serum concentrations with the use of the population parameter estimates with and without feedback were evaluated in the remaining 17 patients. Mean clearance (+/- SD) and volume of distribution for all 44 patients were 0.123 +/- 0.041 liter/hour/kg and 0.424 +/- 0.116 liter/kg, respectively. Bayesian forecasting of the second set of peak and trough concentrations with feedback from the first set of peak and trough concentrations resulted in smaller bias (peak ME, -0.15 mg/liter; trough ME, 0.13 mg/liter) and better accuracy (peak MAE, 0.91 mg/liter; trough MAE, 0.28 mg/liter) compared with the population parameter estimates alone (peak ME, 0.4 mg/liter; trough ME, 0.28 mg/liter; peak MAE, 1.21 mg/liter; trough MAE, 0.57 mg/liter). This study indicates that gentamicin volume of distribution in PICU patients is larger than non-PICU literature values. The Bayesian program, with specific population parameter estimates for PICU patients, provides accurate initial and subsequent predictions of gentamicin serum concentrations.

引用

页码：713 / 718

页数：6

共 50 条

[1] BAYESIAN FORECASTING OF SERUM GENTAMICIN CONCENTRATIONS IN INTENSIVE-CARE PATIENTS
RODVOLD, KA
PRYKA, RD
KUEHL, PG
BLUM, RA
DONAHUE, P
[J]. CLINICAL PHARMACOKINETICS, 1990, 18 (05) : 409 - 418
[2] GENTAMICIN-(G) PHARMACOKINETICS (PK) IN PEDIATRIC INTENSIVE-CARE UNIT (PICU) PATIENTS
KRAUS, DM
DUSIK, CM
KECSKES, SA
RODVOLD, KA
[J]. CLINICAL PHARMACOLOGY & THERAPEUTICS, 1993, 53 (02) : 144 - 144
[3] THE PHARMACOKINETICS OF DOBUTAMINE IN PEDIATRIC INTENSIVE-CARE UNIT PATIENTS
SCHWARTZ, PH
ELDADAH, MK
NEWTH, CJL
[J]. DRUG METABOLISM AND DISPOSITION, 1991, 19 (03) : 614 - 619
[4] DOBUTAMINE PHARMACOKINETICS IN PEDIATRIC INTENSIVE-CARE PATIENTS
HABIB, DM
PADBURY, JF
PERKIN, RM
ANAS, NG
MARTINEZ, AM
MINAGAR, C
[J]. CLINICAL RESEARCH, 1989, 37 (01): : A176 - A176
[5] TRAUMA PATIENTS IN A PEDIATRIC INTENSIVE-CARE UNIT
HOPKINS, RL
[J]. CLINICAL RESEARCH, 1984, 32 (05): : A888 - A888
[6] DOBUTAMINE PHARMACOKINETICS AND PHARMACODYNAMICS IN PEDIATRIC INTENSIVE-CARE PATIENTS
HABIB, DM
PADBURY, JF
ANAS, NG
PERKIN, RM
MINEGAR, C
[J]. CRITICAL CARE MEDICINE, 1992, 20 (05) : 601 - 608
[7] DOBUTAMINE PHARMACOKINETICS AND PHARMACODYNAMICS IN PEDIATRIC INTENSIVE-CARE PATIENTS
HABIB, DM
PADBURY, JF
ANAS, NG
PERKIN, RM
MINEGAR, C
[J]. PEDIATRIC RESEARCH, 1989, 25 (04) : A67 - A67
[8] PHARMACOKINETICS OF ONCE-DAILY DOSING OF GENTAMICIN IN SURGICAL, INTENSIVE-CARE UNIT PATIENTS WITH OPEN FRACTURES
SANGHA, KS
MIYAGAWA, CI
HEALY, DP
BJORNSON, HS
[J]. ANNALS OF PHARMACOTHERAPY, 1995, 29 (02) : 117 - 119
[9] OUTCOME OF ONCOLOGY PATIENTS IN THE PEDIATRIC INTENSIVE-CARE UNIT
SIVAN, Y
SCHWARTZ, PH
SCHONFELD, T
COHEN, IJ
NEWTH, CJL
[J]. INTENSIVE CARE MEDICINE, 1991, 17 (01) : 11 - 15
[10] PENTOBARBITAL SEDATION FOR PATIENTS IN THE PEDIATRIC INTENSIVE-CARE UNIT
TOBIAS, JD
DESHPANDE, JK
PIETSCH, JB
WHEELER, TJ
GREGORY, DF
[J]. SOUTHERN MEDICAL JOURNAL, 1995, 88 (03) : 290 - 294

← 1 2 3 4 5 →