Ryan D P, Supko J G, Eder J P, Seiden M V, Demetri G, Lynch T J, Fischman A J, Davis J, Jimeno J, Clark J W
Massachusetts General Hospital, Boston, Massachusetts 02114, USA.
Clin Cancer Res. 2001 Feb;7(2):231-42.
Ecteinascidin 743 (ET-743) is a cytotoxic tetrahydroisoquinoline alkaloid that covalently binds to DNA in the minor groove. The in vitro chemosensitivity of cancer cells to ET-743 is markedly enhanced by prolonging the duration of exposure to the drug. A Phase I study of ET-743 given as a 72-h continuous i.v. infusion every 21 days was performed. Characteristics of the 21 adult patients with refractory solid tumors enrolled in the study were as follows: (a) 12 men; (b) 9 women; (c) median age, 59 years; (d) Eastern Cooperative Oncology Group performance status < or = 1, 20 patients; and (e) two prior regimens of chemotherapy, 7 patients. Dose limiting toxicity (DLT) was defined by typical criteria, except that grade 3 transaminitis did not constitute a DLT. There were no DLTs in the six patients evaluated at the first two dose levels of 600 and 900 microg/m2. Reversible grade 4 transaminitis occurred in two of nine patients after treatment with the first cycle of therapy at the third dose level of 1200 microg/m2. Another patient experienced grade 4 rhabdomyolysis, renal failure requiring hemodialysis, grade 4 neutropenia, and grade 3 thrombocytopenia during the second cycle of therapy with this dose. The maximum tolerated dose was 1200 microg/m2, and an additional six patients were enrolled at an intermediate dose level of 1050 microg/m2. This well-tolerated dose was established as the recommended Phase II dose. The disposition of ET-743 was distinctly biexponential, and a departure from linear pharmacokinetic behavior was evident at the 1200-microg/m2 dose level. Pharmacokinetic parameters determined at 1050 microg/m2 were (mean +/- SD): maximum plasma concentration, 318 +/- 147 pg/ml; initial disposition phase half-life, 9.0 +/- 10.3 min; terminal phase half-life, 69.0 +/- 56.7 h; and total plasma clearance, 28.4 +/- 22.5 liters/h/m2. Prolonged systemic exposure to concentrations of the agent that are cytotoxic in vitro were achieved. Toxicity of the drug is clearly schedule-dependent, because increasing the duration of infusion from 3 or 24 h to 72 h results in decreased myelosuppression and comparable hepatotoxicity. Although there were no objective responses to therapy, clear evidence of antitumor activity was observed in a patient with epithelioid mesothelioma, as confirmed by positron emission tomography studies. A Phase II trial to assess the efficacy of ET-743 against this highly refractory neoplasm has been initiated on the basis of this observation. The therapeutically optimal administration schedule remains to be established, inasmuch as there have been indications of activity against a variety of tumors during Phase I studies when the drug was infused over times ranging from 1 to 72 h. Characterizing the pharmacokinetics of ET-743 during the course of Phase II trials and Phase I combination studies is recommended to assure that this promising new anticancer drug can be used with an acceptable margin of safety.
埃博霉素 743(ET - 743)是一种细胞毒性四氢异喹啉生物碱,它能与小沟中的 DNA 共价结合。延长癌细胞对 ET - 743 的暴露时间可显著增强其体外化学敏感性。开展了一项 I 期研究,每 21 天进行一次为期 72 小时的静脉持续输注 ET - 743。参与该研究的 21 例难治性实体瘤成年患者的特征如下:(a)男性 12 例;(b)女性 9 例;(c)中位年龄 59 岁;(d)东部肿瘤协作组体能状态≤1 分,20 例患者;(e)接受过两种化疗方案,7 例患者。剂量限制毒性(DLT)按典型标准定义,但 3 级转氨酶升高不构成 DLT。在最初两个剂量水平 600 和 900 μg/m²评估的 6 例患者中未出现 DLT。在第三个剂量水平 1200 μg/m²进行第一周期治疗后,9 例患者中有 2 例出现可逆性 4 级转氨酶升高。另 1 例患者在此剂量的第二周期治疗期间出现 4 级横纹肌溶解、需要血液透析的肾衰竭、4 级中性粒细胞减少和 3 级血小板减少。最大耐受剂量为 1200 μg/m²,另外 6 例患者在中间剂量水平 1050 μg/m²入组。这一耐受性良好的剂量被确定为推荐的 II 期剂量。ET - 743 的处置明显呈双指数型,在 1200 μg/m²剂量水平时明显偏离线性药代动力学行为。在 1050 μg/m²时测定的药代动力学参数为(均值±标准差):最大血浆浓度,318±147 pg/ml;初始处置相半衰期,9.0±10.3 分钟;终末相半衰期,69.0±56.7 小时;总血浆清除率,28.4±22.5 升/小时/平方米。实现了长时间全身暴露于体外具有细胞毒性浓度的该药物。该药物的毒性明显依赖于给药方案,因为将输注时间从 3 或 24 小时增加到 72 小时会导致骨髓抑制减轻且肝毒性相当。尽管治疗无客观反应,但在 1 例上皮样间皮瘤患者中观察到了明确的抗肿瘤活性证据,正电子发射断层扫描研究证实了这一点。基于这一观察结果,已启动一项 II 期试验以评估 ET - 743 对这种高度难治性肿瘤的疗效。由于在 I 期研究中当药物输注时间从 1 小时至 72 小时不等时已显示出对多种肿瘤的活性迹象,治疗上的最佳给药方案仍有待确定。建议在 II 期试验和 I 期联合研究过程中对 ET - 743 的药代动力学进行表征,以确保这种有前景的新型抗癌药物能够在可接受的安全范围内使用。
