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大剂量异环磷酰胺、卡铂和依托泊苷的药代动力学:血浆药物水平与肾毒性的相关性

High-dose ifosfamide, carboplatin, and etoposide pharmacokinetics: correlation of plasma drug levels with renal toxicity.

作者信息

Wright J E, Elias A, Tretyakov O, Holden S, Andersen J, Wheeler C, Schwartz G, Antman K, Rosowsky A, Frel E

机构信息

Department of Medicine, Dana-Farber Cancer Institute, Boston, MA 02115, USA.

出版信息

Cancer Chemother Pharmacol. 1995;36(4):345-51. doi: 10.1007/BF00689053.

Abstract

An autologous bone marrow transplant regimen of ifosfamide, carboplatin, and etoposide (ICE) has been developed as treatment for certain malignancies. At maximum tolerated doses renal insufficiency precludes dose escalation. The objective was to examine whether measurement of plasma drug levels early during treatment would provide warning of renal failure. Nine patients received a 96-h continuous infusion of ifosfamide 16,000 mg/m2, carboplatin 1600 mg/m2, and etoposide 1200 mg/m2. Pharmacokinetics, including drug levels and plasma concentration-time curves, of ifosfamide, ultrafiltrable platinum (uPt) and etoposide were analyzed and correlated with renal function. One of the nine patients developed anuric renal failure requiring hemodialysis. By 17 h from the start of infusion, this patient showed substantially higher drug levels of ifosfamide (200 vs mean 217 microM) and uPt (19 vs mean 10 microM) than those patients with preserved renal function. The 95% confidence intervals suggested that a 16-22 h ifosfamide level > 153 microM and an uPt level > microM predict the development of significant renal dysfunction. Although drug levels were substantially higher at 56 h, the serum creatinine did not yet reflect kidney injury. This study suggests that high plasma ifosfamide and uPt levels, analyzed early in the course of a 96-h infusion of high-dose ICE, provide warning of severe and potentially fatal renal injury. Since ICE has substantial activity in a number of malignancies, but significant renal morbidity, real-time pharmacokinetic-guided dosing may reduce treatment-related toxicity.

摘要

异环磷酰胺、卡铂和依托泊苷(ICE)的自体骨髓移植方案已被开发用于治疗某些恶性肿瘤。在最大耐受剂量下,肾功能不全限制了剂量的增加。目的是研究在治疗早期测量血浆药物水平是否能为肾衰竭提供预警。9名患者接受了96小时持续输注异环磷酰胺16000mg/m²、卡铂1600mg/m²和依托泊苷1200mg/m²。分析了异环磷酰胺、超滤铂(uPt)和依托泊苷的药代动力学,包括药物水平和血浆浓度-时间曲线,并与肾功能进行了关联。9名患者中有1名发生无尿性肾衰竭,需要进行血液透析。从输注开始17小时起,该患者的异环磷酰胺(200μM对平均217μM)和uPt(19μM对平均10μM)药物水平明显高于肾功能正常的患者。95%置信区间表明,异环磷酰胺水平在16 - 22小时>153μM且uPt水平>μM可预测严重肾功能不全的发生。尽管在56小时时药物水平显著升高,但血清肌酐尚未反映肾脏损伤。这项研究表明,在大剂量ICE 96小时输注过程早期分析的高血浆异环磷酰胺和uPt水平,可为严重且可能致命的肾损伤提供预警。由于ICE在多种恶性肿瘤中具有显著活性,但会导致明显的肾脏发病率,实时药代动力学指导给药可能会降低治疗相关毒性。

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