Egorin M J, Conley B A, Forrest A, Zuhowski E G, Sinibaldi V, Van Echo D A
Division of Developmental Therapeutics, University of Maryland School of Medicine, Baltimore.
Cancer Res. 1987 Nov 15;47(22):6104-10.
We performed a phase I study of menogaril to determine if dosage reduction was required in patients with hepatic dysfunction and if the relationship between pharmacokinetics and leukopenia, previously defined in patients with normal hepatic and renal function, was altered. Eighteen patients received 27 courses of menogaril, of which 26 were evaluable for toxicity. Patient characteristics were median age, 63 years (range, 28-80 years), 14 male/4 female, and median Karnofsky performance status 80% (range, 60-100%). Prior therapy included none, five; chemotherapy only, seven; radiotherapy only, two; and chemotherapy and radiotherapy, four. Menogaril was administered as a 2-h.i.v. infusion every 28 days at 62.5 (one patient), 125 (eight patients), 187.5 (seven patients), and 250 mg/m2 (six patients), based on pretreatment serum bilirubin, aspartate aminotransferase, alanine aminotransferase, and alkaline phosphatase. Patients also had indocyanine green and antipyrine clearances measured before menogaril treatment. Menogaril and metabolites were assayed by high performance liquid chromatography. Dose-limiting toxicity was leukopenia. WBC nadirs occurred between days 8 and 20 (median, 15). Three patients developed platelet nadirs below 100,000/microliters. Other toxicities included grade I nausea and vomiting in three patients and phlebitis at the site of drug infusion in six patients. Correlations were defined between pretreatment indocyanine green clearance and serum concentrations of alkaline phosphatase and total bilirubin. There were no correlations between pretreatment serum concentrations of bilirubin, aspartate aminotransferase, alanine aminotransferase, alkaline phosphatase, indocyanine green clearance or antipyrine and menogaril clearances. Menogaril pharmacokinetics in patients with elevated liver function tests was indistinguishable from that described in patients with normal liver function tests. There were excellent correlations between plasma area under the curve of menogaril and the percentage decreases in WBC and neutrophils. These were well described by two models previously used to study the same relationships in patients with normal hepatic and renal function. When compared to previous studies, patients with hepatic and renal dysfunction had a greater percentage decrease in WBC for any given area under the curve than did patients with normal hepatic and renal function. On the other hand, there was no difference in the relationship between percentage decrease in neutrophils and menogaril area under the curve in these two groups of patients.(ABSTRACT TRUNCATED AT 400 WORDS)
我们开展了一项美诺加(menogaril)的I期研究,以确定肝功能不全患者是否需要降低剂量,以及之前在肝肾功能正常患者中确定的药代动力学与白细胞减少之间的关系是否发生改变。18例患者接受了27个疗程的美诺加治疗,其中26个疗程可评估毒性。患者特征为年龄中位数63岁(范围28 - 80岁),男性14例/女性4例,卡氏功能状态中位数80%(范围60 - 100%)。既往治疗情况为:未接受过治疗的有5例;仅接受化疗的有7例;仅接受放疗的有2例;接受化疗和放疗的有4例。根据治疗前血清胆红素、天冬氨酸转氨酶、丙氨酸转氨酶和碱性磷酸酶水平,美诺加以每28天一次、持续2小时静脉输注的方式给药,剂量分别为62.5mg/m²(1例患者)、125mg/m²(8例患者)、187.5mg/m²(7例患者)和250mg/m²(6例患者)。患者在接受美诺加治疗前还进行了吲哚菁绿和安替比林清除率测定。美诺加及其代谢产物通过高效液相色谱法进行测定。剂量限制性毒性为白细胞减少。白细胞最低点出现在第8至20天之间(中位数为15天)。3例患者血小板最低点低于100,000/微升。其他毒性包括3例患者出现I级恶心和呕吐,6例患者出现药物输注部位静脉炎。确定了治疗前吲哚菁绿清除率与碱性磷酸酶和总胆红素血清浓度之间的相关性。治疗前血清胆红素、天冬氨酸转氨酶、丙氨酸转氨酶、碱性磷酸酶、吲哚菁绿清除率或安替比林浓度与美诺加清除率之间无相关性。肝功能检查结果升高的患者中美诺加的药代动力学与肝功能检查结果正常的患者中所描述的情况无差异。美诺加血浆曲线下面积与白细胞和中性粒细胞百分比下降之间存在良好的相关性。这可以用之前用于研究肝肾功能正常患者相同关系的两个模型很好地描述。与之前的研究相比,对于任何给定的曲线下面积,肝肾功能不全患者的白细胞百分比下降幅度大于肝肾功能正常的患者。另一方面,在这两组患者中,中性粒细胞百分比下降与美诺加曲线下面积之间的关系没有差异。(摘要截短至400字)
