甲氨蝶呤治疗骨肉瘤的药代动力学及不良反应。

H. Ikeda, T. Sugita, K. Miyake, E. Sato, Y. Kimura, T. Kitaura, H. Fukuchi, Y. Ikuta, K. Kihira
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引用次数: 2

摘要

研究了甲氨蝶呤(MTX)剂量对大鼠肾、肝及血液功能药动学参数的影响。20例骨肉瘤患者(年龄13 ~ 53岁)接受MTX输注,剂量3.3 ~ 11.2g/m2,持续6小时。血清MTX浓度在6h、12h和24h几乎与注射剂量成正比增加。血清总MTX清除率和半衰期在所有剂量范围内几乎不变。为评价剂量与实验室检测值的关系,根据甲氨蝶呤剂量将患者分为低剂量组(3.3 ~ 5.2g/m2)、中剂量组(5.4 ~ 8.3g/m2)、高剂量组(9.0 ~ 11.2g/m2)。注射甲氨蝶呤前两组患者的肾功能和血液学功能无明显差异。高剂量组在第2天、第7天血清GOT、GPT值显著升高,提示肝功能下降。尽管MIX的药代动力学是线性的,但与中、低剂量相比,高剂量可能导致GOT和GPT值的显著非线性增加。为避免MTX治疗在高剂量组出现严重不良反应,输注后仔细监测MTX的血药浓度和肝功能是重要的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Pharmacokinetics and Adverse Reaction in Methotrexate Therapy of Osteosarcoma.
The effect of the dosage of methotrexate (MTX) on pharmacokinetic parameters in renal, hepatic and hematological functions were investigated. Twenty osteosarcoma patients (age: 13-53 years) received MTX infusions (dosage: 3.3-11.2g/m2) for 6 hrs. The serum MTX concentrations at 6h, 12h and 24h increased almost proportionally with the infused dose. The total serum MTX clearance and half-lives were almost constant in all the dosing ranges examined.To evaluate the relationship between the dosage and laboratory values, the patients were divided into three groups based on the MTX dosage and consisting of: low-dose (dosage: 3.3-5.2g/m2), middle-dose (dosage: 5.4-8.3g/m2), and high-dose (dosage: 9.0-11.2g/m2) groups. There was no significant difference between the renal and hematological functions before MTX infusion. In the high-dose group, significantly increased GOT and GPT values were observed on days 2 and 7, which indicate a decreased in hepatic function.In spite of the linear pharmacokinetics of MIX, a high-dose may cause remarkably nonlinear increased GOT and GPT values compared to those with low-and middle-doses.To avoid a severe adverse reaction of MTX therapy in the high-dosage group, careful monitoring of both the serum concentration of MTX and the liver functions is considered to be important after infusion.
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