大剂量输注疗法后癌症患者甲氨蝶呤和7-羟基甲氨蝶呤清除的决定因素
Determinants of the elimination of methotrexate and 7-hydroxy-methotrexate following high-dose infusional therapy to cancer patients.
作者信息
Joerger M, Huitema A D R, van den Bongard H J G D, Baas P, Schornagel J H, Schellens J H M, Beijnen J H
机构信息
Department of Pharmacy & Pharmacology, Slotervaart Hospital/The Netherlands Cancer Institute, Amsterdam, and Department of Biomedical Analysis, Faculty of Pharmaceutical Sciences, Utrecht University, The Netherlands.
出版信息
Br J Clin Pharmacol. 2006 Jul;62(1):71-80. doi: 10.1111/j.1365-2125.2005.02513.x.
AIMS
To characterize determinants of the elimination of methotrexate (MTX) and 7-hydroxy-methotrexate (7-OH-MTX) in patients receiving high-dose MTX therapy (HDMTX).
METHODS
24 and 48-h blood samples from 76 patients receiving HDMTX (dose range 300 mg m-2 to 12 g m-2) were analysed, and concentration-time data were subjected to population pharmacokinetic and covariate analysis using nonlinear mixed-effect modelling (NONMEM).
RESULTS
Treatment-related mortality was 1.3% (one patient with renal failure). Values for MTX clearance (CLMTX) and 7-OH-MTX clearance (CL7-OH-MTX) were estimated at 8.85 and 2 L-1, respectively. Baseline creatinine clearance correlated with CLMTX and CL7-OH-MTX. Concurrent administration of benzimidazoles led to a 27% decrease in CLMTX and a 39% decrease in CL7-OH-MTX. Prior administration of nonsteroidal anti-inflammatory drugs (NSAIDs) resulted in a 16% decrease in CLMTX and a 38% decrease in CL7-OH-MTX. Plasma MTX concentrations were significantly higher in patients also receiving benzimidazoles at 24 h (2.01 micromol L-1vs. 0.66 micromol L-1, P<10(-4)) and at 48 h (0.25 micromol L-1vs. 0.12 micromol L-1, P<10(-4)). 7-OH-MTX plasma concentrations were also significantly higher in patients with concurrent benzimidazoles as compared with patients without benzimidazoles at 24 h (4.47 micromol L-1vs. 2.52 micromol L-1, P=0.0009) and at 48 h (1.11 micromol L-1vs. 0.72 micromol L-1, P=0.031).
CONCLUSIONS
In patients receiving HDMTX, concurrent administration of benzimidazoles was associated with a significant decrease of CLMTX and CL7-OH-MTX, resulting in significantly higher plasma concentrations of MTX and 7-OH-MTX. The data suggest that benzimidazole treatment should be seen as a relative contraindication for HDMTX.
目的
明确接受大剂量甲氨蝶呤治疗(HDMTX)的患者中甲氨蝶呤(MTX)和7-羟基甲氨蝶呤(7-OH-MTX)清除的决定因素。
方法
分析了76例接受HDMTX治疗(剂量范围为300mg/m²至12g/m²)患者的24小时和48小时血样,并使用非线性混合效应模型(NONMEM)对浓度-时间数据进行群体药代动力学和协变量分析。
结果
治疗相关死亡率为1.3%(1例肾衰竭患者)。MTX清除率(CLMTX)和7-OH-MTX清除率(CL7-OH-MTX)的值分别估计为8.85和2L⁻¹。基线肌酐清除率与CLMTX和CL7-OH-MTX相关。同时给予苯并咪唑导致CLMTX降低27%,CL7-OH-MTX降低39%。先前使用非甾体抗炎药(NSAIDs)导致CLMTX降低16%,CL7-OH-MTX降低38%。在24小时(2.01μmol/L对0.66μmol/L,P<10⁻⁴)和48小时(0.25μmol/L对0.12μmol/L,P<10⁻⁴)时,同时接受苯并咪唑治疗的患者血浆MTX浓度显著更高。与未使用苯并咪唑的患者相比,同时使用苯并咪唑的患者在24小时(4.47μmol/L对2.52μmol/L,P=0.0009)和48小时(1.11μmol/L对0.72μmol/L,P=0.031)时7-OH-MTX血浆浓度也显著更高。
结论
在接受HDMTX治疗的患者中,同时给予苯并咪唑与CLMTX和CL7-OH-MTX显著降低相关,导致MTX和7-OH-MTX的血浆浓度显著升高。数据表明苯并咪唑治疗应被视为HDMTX的相对禁忌证。
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