Vinflunine is a novel tubulin-targeted agent that is currently indicated as a monotherapy in bladder cancer patients. The recommended dose of 320 mg/m(2) is given as an intravenous infusion once every 3 weeks. Vinflunine is metabolized through CYP3A4 and mainly eliminated via the feces. A phase I trial was designed to explore the tolerability and pharmacokinetics of vinflunine in cancer patients with ranging degrees of liver dysfunction (LD). A sequential design was used for patient accrual, with the objective of determining the maximum tolerated dose (MTD) and the recommended dose (RD) of vinflunine in 3 groups of increasing LD levels. Vinflunine and its only active metabolite 4-O-deacetylvinflunine were quantified in serial whole blood samples. PK parameters were derived and compared between LD groups and with a reference PK database. Vinflunine and 4-O-deacetylvinflunine PK parameters were not affected in any of the explored LD levels. Geometric mean values for vinflunine total clearance were 47.8, 37.5 and 45.4 L/h in the 3 groups of increasing degrees of LD, as compared to 42.5 L/h in reference patients with no LD. No relationship was found between vinflunine clearance and the presence or absence of cirrhosis, nor was it found with the presence or absence of liver metastasis or with liver-related biochemical parameters. Based on the observed tolerability profile, the recommended doses of i.v. vinflunine are 320 mg/m(2), 250 mg/m(2) or 200 mg/m(2) for patients with increasing degrees of liver dysfunction.

译文

:长春氟宁是一种新型的微管蛋白靶向药物,目前被认为是膀胱癌患者的一种单一疗法。每3周一次静脉滴注,建议剂量为320 mg / m(2)。长春氟宁通过CYP3A4代谢,主要通过粪便消除。设计了一项I期试验,以研究长春氟宁在具有一定程度的肝功能不全(LD)的癌症患者中的耐受性和药代动力学。为了确定患者的累积量,采用了顺序设计,目的是确定3组LD水平升高的患者中长春氟宁的最大耐受剂量(MTD)和推荐剂量(RD)。在连续全血样品中对长春氟宁及其唯一的活性代谢物4-O-去乙酰长春氟宁进行了定量。得出PK参数,并在LD组之间与参考PK数据库进行比较。在任何探索的LD水平中,长春氟宁和4-O-去乙酰长春氟宁PK参数均不受影响。在3组LD升高程度较高的组中,长春氟宁总清除率的几何平均值为47.8、37.5和45.4 L / h,而没有LD的参考患者为42.5 L / h。在长春氟宁清除率与是否存在肝硬化之间未发现相关性,也未发现其与是否存在肝转移或与肝脏相关的生化参数有关。根据观察到的耐受性,推荐静脉注射剂量。对于肝功能异常程度增加的患者,长春氟宁为320 mg / m(2),250 mg / m(2)或200 mg / m(2)。

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