DAY-TO-DAY VARIABILITY IN AZATHIOPRINE PHARMACOKINETICS IN RENAL-TRANSPLANT RECIPIENTS

被引：0

作者：

OHLMAN, S

ALBERTIONI, F

PETERSON, C

机构：

来源：

CLINICAL TRANSPLANTATION | 1994年 / 8卷 / 03期

关键词：

AZATHIOPRINE; 6-MERCAPTOPURINE; PHARMACOKINETICS; INTRAINDIVIDUAL VARIABILITY; INTERINDIVIDUAL VARIABILITY; RENAL TRANSPLANTATION;

D O I：

暂无

中图分类号：

R61 [外科手术学];

学科分类号：

摘要：

The intraindividual and the interindividual variability in the pharmacokinetics of azathioprine (Aza) and its main metabolite 6-mercaptopurine (6-MP) were investigated in 10 renal transplant patients on 2 consecutive days, after repeated oral doses of Aza. On the 1st study, the dose-adjusted Aza AUC (0-6 h) ranged from 8.4 to 129.1 ngh*ml-1/mg* kg-1, mean 41.4 (+/- 37.6) ngh*ml-1/mg*kg-1. The corresponding values for the dose-adjusted 6-MP AUC (0-6 h) ranged from 37.9 to 172.0 ngh*ml-1/mg*kg-1, mean 91.7 (+/- 50.7) ngh*ml-1/mg*kg-1. The absolute percentage intraindividual difference in Aza AUC (0-6 h) between the two days ranged from 1.2% to 256.6% (mean 64.7%), and for 6-MP AUC (0-6 h) from 5.9% to 98.5% (mean 49.8%). However, no statistically significant difference was found when comparing the pharmacokinetics on the 2 study days. The mean half-life of Aza was 1.7 h and of 6-MP 1.2 h. Impaired renal function did not seem to affect the pharmacokinetics. No correlation was found between the given dose of Aza and AUC (0-6 h) for Aza or 6-MP. A strong correlation was found between the concentrations of Aza and 6-MP obtained at 2 h after the oral dose and the corresponding AUCs (0-6 h) (Aza: r = 0.85, p < 0.001, n = 20; 6-MP: r = 0.9, p < 0.00 1, n = 20). We conclude that the intraindividual variability in Aza pharmacokinetics is marked. but it is less pronounced than the even larger interpatient variability found in this study and previously described.

引用

页码：217 / 223

页数：7

共 50 条

[31] GAMMA/DELTA LYMPHOCYTE-T IN RENAL-TRANSPLANT RECIPIENTS
RAASVELD, MHM
BLOEMENA, E
SURACHNO, S
TENBERGE, RJM
NEPHROLOGY DIALYSIS TRANSPLANTATION, 1992, 7 (06) : 530 - 533
[32] GINGIVAL OVERGROWTH AMONG RENAL-TRANSPLANT RECIPIENTS AND UREMIC PATIENTS
PERNU, HE
PERNU, LMH
KNUUTTILA, MLE
HUTTUNEN, KRH
NEPHROLOGY DIALYSIS TRANSPLANTATION, 1993, 8 (11) : 1254 - 1258
[33] HYPERPARATHYROIDISM, HYPERTENSION AND LOOP DIURETIC MEDICATION IN RENAL-TRANSPLANT RECIPIENTS
BITTAR, AE
RATCLIFFE, PJ
RICHARDSON, AJ
BROWN, RC
WOODHEAD, JS
MORRIS, PJ
NEPHROLOGY DIALYSIS TRANSPLANTATION, 1989, 4 (08) : 740 - 744
[34] SERUM PROPEPTIDES OF TYPE-I AND TYPE-III PROCOLLAGENS IN RENAL-TRANSPLANT RECIPIENTS - A COMPARISON OF CYCLOSPORINE AND AZATHIOPRINE TREATMENT
HEICKENDORFF, L
FROST, L
MADSEN, JK
PEDERSEN, EB
NEPHRON, 1994, 67 (02): : 203 - 208
[35] PHARMACOKINETICS OF CYCLOSPORINE-A IN RENAL-TRANSPLANT PATIENTS AFTER INFUSION
GU, CN
DENG, YL
ZHU, YH
ZHU, CJ
GU, QP
ACTA PHARMACOLOGICA SINICA, 1991, 12 (06): : 528 - 530
[36] TPMT but not ITPA gene polymorphism influences the risk of azathioprine intolerance in renal transplant recipients
Mateusz Kurzawski
Krzysztof Dziewanowski
Agnieszka Lener
Marek Drozdzik
European Journal of Clinical Pharmacology, 2009, 65
[37] RENIN SECRETION AND CAPTOPRIL STIMULATION IN HYPERTENSIVE RENAL-TRANSPLANT RECIPIENTS
KUTKUHN, B
HOLLENBECK, M
WESTHOFF, A
IVENS, K
HEERING, P
GRABENSEE, B
UROLOGIA INTERNATIONALIS, 1994, 52 (02) : 82 - 86
[38] LIPID-LOWERING TREATMENT WITH PANTETHINE IN RENAL-TRANSPLANT RECIPIENTS
CORONEL, F
TORNERO, F
MACIA, M
HERRERO, JA
SANCHEZ, A
BARRIENTOS, A
NEFROLOGIA, 1995, 15 (01): : 68 - 73
[39] DIAGNOSIS AND TREATMENT OF CYTOMEGALOVIRUS DISEASE IN PEDIATRIC RENAL-TRANSPLANT RECIPIENTS
BURD, RS
GILLINGHAM, KJ
FARBER, MS
STATZ, CL
KRAMER, MS
NAJARIAN, JS
DUNN, DL
JOURNAL OF PEDIATRIC SURGERY, 1994, 29 (08) : 1049 - 1054
[40] TRIAL OF INTRAVESICAL VERSUS EXTRAVESICAL URETERONEOCYSTOSTOMY IN RENAL-TRANSPLANT RECIPIENTS
JINDAL, RM
CARPINITO, G
BERNARD, D
SCHMITT, G
IDELSON, B
JOSHI, P
HAKAIM, A
CHO, SI
CLINICAL TRANSPLANTATION, 1994, 8 (04) : 396 - 398

← 1 2 3 4 5 →