学术探索
学术期刊
新闻热点
数据分析
智能评审

THE PHARMACOKINETICS OF HIGH-DOSE CARBOPLATIN IN PEDIATRIC-PATIENTS WITH CANCER

被引:53
作者
MADDEN, T
SUNDERLAND, M
SANTANA, VM
RODMAN, JH
机构
[1] ST JUDE CHILDRENS RES HOSP, DIV PHARMACEUT, 332 N LAUDERDALE BLVD, MEMPHIS, TN 38105 USA
[2] ST JUDE CHILDRENS RES HOSP, DEPT HEMATOL ONCOL, MEMPHIS, TN 38101 USA
[3] UNIV TENNESSEE, DEPT CLIN PHARM & PEDIAT, KNOXVILLE, TN 37996 USA
来源
CLINICAL PHARMACOLOGY & THERAPEUTICS | 1992年 / 51卷 / 06期
关键词
D O I
10.1038/clpt.1992.82
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Carboplatin disposition was studied in 18 pediatric patients with cancer over a dosage range of 400 to 700 mg/m2 given on an alternate-day schedule (total doses of 1200 to 2100 mg/m2) with high-dose etoposide. Median age was 7.7 years, hepatic functions were normal, and serum creatinine levels were less-than-or-equal-to 1.0 mg/dl. Carboplatin pharmacokinetics were determined by atomic absorption spectroscopy. Median pharmacokinetic parameters for ultrafilterable platinum were as follows: clearance 45.8 mt/min/m2 (range, 25.5 to 65.3 ml/min/m2) and a terminal half-life of 3.6 hours (range, 2.1 to 14.2 hours). Carboplatin clearance (CL) values and volume of distribution (V(C) were highly correlated to body size (CL = 55 x Body surface area in [BSA, in square meters] - 6.7, r2 = 0.73, V(C) = 5 x BSA [in square meters] + 0.26, r2 = 0.69). However, carboplatin doses normalized to BSA still resulted in twofold to threefold variability in area under the concentration - time curve. Carboplatin CL was significantly lower in those subjects (n = 9) who had previously received cumulative cisplatin doses of greater-than-or-equal-to 960 mg/m2 (p < 0.05) but was not influenced by age, gender, or diagnosis.
引用
收藏
页码:701 / 707
页数:7
相关论文
共 22 条
[1]   EARLY CLINICAL-STUDIES WITH CIS-DIAMMINE-1,1-CYCLOBUTANE DICARBOXYLATE PLATINUM-II [J].
CALVERT, AH ;
HARLAND, SJ ;
NEWELL, DR ;
SIDDIK, ZH ;
JONES, AC ;
MCELWAIN, TJ ;
RAJU, S ;
WILTSHAW, E ;
SMITH, IE ;
BAKER, JM ;
PECKHAM, MJ ;
HARRAP, KR .
CANCER CHEMOTHERAPY AND PHARMACOLOGY, 1982, 9 (03) :140-147
[2]   CARBOPLATIN DOSAGE - PROSPECTIVE EVALUATION OF A SIMPLE FORMULA BASED ON RENAL-FUNCTION [J].
CALVERT, AH ;
NEWELL, DR ;
GUMBRELL, LA ;
OREILLY, S ;
BURNELL, M ;
BOXALL, FE ;
SIDDIK, ZH ;
JUDSON, IR ;
GORE, ME ;
WILTSHAW, E .
JOURNAL OF CLINICAL ONCOLOGY, 1989, 7 (11) :1748-1756
[3]   EVALUATION OF AMINOGLYCOSIDE DISPOSITION IN PATIENTS PREVIOUSLY TREATED WITH CISPLATIN [J].
CHRISTENSEN, ML ;
STEWART, CF ;
CROM, WR .
THERAPEUTIC DRUG MONITORING, 1989, 11 (06) :631-636
[4]   THE EFFECT OF PRIOR CISPLATIN THERAPY ON THE PHARMACOKINETICS OF HIGH-DOSE METHOTREXATE [J].
CROM, WR ;
PRATT, CB ;
GREEN, AA ;
CHAMPION, JE ;
CROM, DB ;
STEWART, CF ;
EVANS, WE .
JOURNAL OF CLINICAL ONCOLOGY, 1984, 2 (06) :655-661
[5]   CLINICAL-TRIAL AND PHARMACOKINETICS OF CARBOPLATIN 560 MG/M2 IN CHILDREN [J].
DOZ, F ;
BRUGIERES, L ;
BASTIAN, G ;
QUINTANA, E ;
LEMERLE, J ;
ZUCKER, JM .
MEDICAL AND PEDIATRIC ONCOLOGY, 1990, 18 (06) :459-465
[6]  
EGORIN MJ, 1984, CANCER RES, V44, P5432
[7]  
ELFERINK F, 1987, CANCER TREAT REP, V71, P1231
[8]   A PHASE-I STUDY OF HIGH-DOSE IFOSFAMIDE AND ESCALATING DOSES OF CARBOPLATIN WITH AUTOLOGOUS BONE-MARROW SUPPORT [J].
ELIAS, AD ;
AYASH, LJ ;
EDER, JP ;
WHEELER, C ;
DEARY, J ;
WEISSMAN, L ;
SCHRYBER, S ;
HUNT, M ;
CRITCHLOW, J ;
SCHNIPPER, L ;
FREI, E ;
ANTMAN, KH .
JOURNAL OF CLINICAL ONCOLOGY, 1991, 9 (02) :320-327
[9]   CONCEPT OF MAXIMUM TOLERATED SYSTEMIC EXPOSURE AND ITS APPLICATION TO PHASE-I-II STUDIES OF ANTICANCER DRUGS [J].
EVANS, WE ;
RODMAN, JH ;
RELLING, MV ;
CROM, WR ;
RIVERA, GK ;
PRATT, CB ;
CRIST, WM .
MEDICAL AND PEDIATRIC ONCOLOGY, 1991, 19 (03) :153-159
[10]   THE DISPOSITION OF CARBOPLATIN IN OVARIAN-CANCER PATIENTS [J].
GAVER, RC ;
COLOMBO, N ;
GREEN, MD ;
GEORGE, AM ;
DEEB, G ;
MORRIS, AD ;
CANETTA, RM ;
SPEYER, JL ;
FARMEN, RH ;
MUGGIA, FM .
CANCER CHEMOTHERAPY AND PHARMACOLOGY, 1988, 22 (03) :263-270
123