法尼基蛋白转移酶抑制剂R115777在晚期癌症中的I期及药代动力学研究。

Phase I and pharmacokinetic study of farnesyl protein transferase inhibitor R115777 in advanced cancer.

作者信息

Zujewski J, Horak I D, Bol C J, Woestenborghs R, Bowden C, End D W, Piotrovsky V K, Chiao J, Belly R T, Todd A, Kopp W C, Kohler D R, Chow C, Noone M, Hakim F T, Larkin G, Gress R E, Nussenblatt R B, Kremer A B, Cowan K H

机构信息

Medicine Branch, Division of Clinical Sciences, National Cancer Institute, Bethesda, MD, USA.

出版信息

J Clin Oncol. 2000 Feb;18(4):927-41. doi: 10.1200/JCO.2000.18.4.927.

DOI:10.1200/JCO.2000.18.4.927

PMID:10673536

Abstract

PURPOSE

To determine the maximum-tolerated dose, toxicities, and pharmacokinetic profile of the farnesyl protein transferase inhibitor R115777 when administered orally bid for 5 days every 2 weeks.

PATIENTS AND METHODS

Twenty-seven patients with a median age of 58 years received 85 cycles of R115777 using an intrapatient and interpatient dose escalation schema. Drug was administered orally at escalating doses as a solution (25 to 850 mg bid) or as pellet capsules (500 to 1300 mg bid). Pharmacokinetics were assessed after the first dose and the last dose administered during cycle 1.

RESULTS

Dose-limiting toxicity of grade 3 neuropathy was observed in one patient and grade 2 fatigue (decrease in two performance status levels) was seen in four of six patients treated with 1,300 mg bid. The most frequent clinical grade 2 or 3 adverse events in any cycle included nausea, vomiting, headache, fatigue, anemia, and hypotension. Myelosuppression was mild and infrequent. Peak plasma concentrations of R115777 were achieved within 0.5 to 4 hours after oral drug administration. The elimination of R115777 from plasma was biphasic, with sequential half-lives of about 5 hours and 16 hours. There was little drug accumulation after bid dosing, and steady-state concentrations were achieved within 2 to 3 days. The pharmacokinetics were dose proportional in the 25 to 325 mg/dose range for the oral solution. Urinary excretion of unchanged R115777 was less than 0.1% of the oral dose. One patient with metastatic colon cancer treated at the 500-mg bid dose had a 46% decrease in carcinoembryonic antigen levels, improvement in cough, and radiographically stable disease for 5 months.

CONCLUSION

R115777 is bioavailable after oral administration and has an acceptable toxicity profile. Based upon pharmacokinetic data, the recommended dose for phase II trials is 500 mg orally bid (total daily dose, 1, 000 mg) for 5 consecutive days followed by 9 days of rest. Studies of continuous dosing and studies of R115777 in combination with chemotherapy are ongoing.

摘要

目的

确定法尼基蛋白转移酶抑制剂R115777每2周口服给药bid，持续5天的最大耐受剂量、毒性及药代动力学特征。

患者与方法

27例中位年龄58岁的患者采用患者内和患者间剂量递增方案接受了85个周期的R115777治疗。药物以递增剂量口服给药，溶液剂型（25至850 mg bid）或微丸胶囊剂型（500至1300 mg bid）。在第1周期的第1剂和最后1剂给药后评估药代动力学。

结果

1例患者出现3级神经病变的剂量限制性毒性，6例接受1300 mg bid治疗的患者中有4例出现2级疲劳（两个体能状态水平下降）。任何周期中最常见的2级或3级临床不良事件包括恶心、呕吐、头痛、疲劳、贫血和低血压。骨髓抑制轻微且不常见。口服给药后0.5至4小时内达到R115777的血浆峰浓度。R115777从血浆中的消除呈双相性，相继的半衰期约为5小时和16小时。bid给药后几乎没有药物蓄积，2至3天内达到稳态浓度。口服溶液在25至325 mg/剂量范围内药代动力学呈剂量比例关系。未改变的R115777的尿排泄量少于口服剂量的0.1%。1例接受500 mg bid剂量治疗的转移性结肠癌患者癌胚抗原水平下降46%，咳嗽改善，影像学检查疾病稳定5个月。