DE-310在晚期实体瘤患者中的I期和药代动力学研究。

Phase I and pharmacokinetic study of DE-310 in patients with advanced solid tumors.

作者信息

Soepenberg Otto, de Jonge Maja J A, Sparreboom Alex, de Bruin Peter, Eskens Ferry A L M, de Heus Gerda, Wanders Jantien, Cheverton Peter, Ducharme Murray P, Verweij Jaap

机构信息

Department of Medical Oncology, Erasmus University Medical Center, Daniel den Hoed Cancer Center, Groene Hilledijk 301, 3075 EA Rotterdam, the Netherlands.

出版信息

Clin Cancer Res. 2005 Jan 15;11(2 Pt 1):703-11.

PMID:15701859

Abstract

PURPOSE

To assess the maximum-tolerated dose, toxicity, and pharmacokinetics of DE-310, a macromolecular prodrug of the topoisomerase I inhibitor exatecan (DX-8951f). in patients with advanced solid tumors.

EXPERIMENTAL DESIGN

Patients received DE-310 as a 3-hour infusion once every 2 weeks (dose, 1.0-2.0 mg/m(2)) or once every 6 weeks (dose, 6.0-9.0 mg/m(2)). Because pharmacokinetics revealed a drug terminal half-life exceeding the 2 weeks administration interval, the protocol was amended to a 6-week interval between administrations also based on available information from a parallel trial using an every 4 weeks schedule. Conjugated DX-8951 (the carrier-linked molecule), and the metabolites DX-8951 and glycyl-DX-8951 were assayed in various matrices up to 35 days post first and second dose.

RESULTS

Twenty-seven patients were enrolled into the study and received a total of 86 administrations. Neutropenia and grade 3 thrombocytopenia, and grade 3 hepatotoxicity with veno-occlusive disease, were dose-limiting toxicities. Other hematologic and nonhematologic toxicities were mild to moderate and reversible. The apparent half-life of conjugated DX-8951, glycyl-DX-8951, and DX-8951 was 13 days. The area under the curve ratio for conjugated DX-8951 to DX-8951 was 600. No drug concentration was detectable in erythrocytes, skin, and saliva, although low levels of glycyl-DX-8951 and DX-8951 were detectable in tumor biopsies. One patient with metastatic adenocarcinoma of unknown primary achieved a histologically proven complete remission. One confirmed partial remission was observed in a patient with metastatic pancreatic cancer and disease stabilization was noted in 14 additional patients.

CONCLUSIONS

The recommended phase II dose of DE-310 is 7.5 mg/m(2) given once every 6 weeks. The active moiety DX-8951 is released slowly from DE-310 and over an extended period, achieving the desired prolonged exposure to this topoisomerase I inhibitor.

摘要

目的

评估拓扑异构酶I抑制剂依喜替康（DX - 8951f）的大分子前药DE - 310在晚期实体瘤患者中的最大耐受剂量、毒性和药代动力学。

实验设计

患者每2周接受一次3小时静脉输注DE - 310（剂量为1.0 - 2.0mg/m²）或每6周接受一次（剂量为6.0 - 9.0mg/m²）。由于药代动力学显示药物终末半衰期超过2周的给药间隔，基于一项采用每4周给药方案的平行试验的现有信息，方案修改为给药间隔为6周。在首次和第二次给药后长达35天的各种基质中检测结合型DX - 8951（载体连接分子）以及代谢产物DX - 8951和甘氨酰 - DX - 8951。

结果

27例患者入组本研究，共接受86次给药。中性粒细胞减少、3级血小板减少以及伴有静脉闭塞性疾病的3级肝毒性为剂量限制性毒性。其他血液学和非血液学毒性为轻度至中度且可逆。结合型DX - 8951、甘氨酰 - DX - 8951和DX - 8951的表观半衰期为13天。结合型DX - 8951与DX - 8951的曲线下面积比为600。在红细胞、皮肤和唾液中未检测到药物浓度，尽管在肿瘤活检中可检测到低水平的甘氨酰 - DX - 8951和DX - 8951。1例原发灶不明的转移性腺癌患者实现了组织学证实的完全缓解。1例转移性胰腺癌患者观察到1次确认的部分缓解，另有14例患者病情稳定。