Gatzemeier U, Rodriguez G, Treat J, Miller V, von Roemeling R, Viallet J, Rey A
Department of Thoracic Oncology, Hospital Grosshansdorf, Hamburg, Germany.
Br J Cancer. 1998 Jun;77 Suppl 4(Suppl 4):15-7. doi: 10.1038/bjc.1998.431.
Tirapazamine is a novel bioreductive agent with selective cytotoxicity against hypoxic tumour cells. Synergy with cisplatin and other chemotherapeutic agents has been shown in preclinical trials. Pharmacokinetic studies of tirapazamine have revealed that exposure increases with dose over the range of 18-450 mg m(-2) for a single dose and of 9-390 mg m(-2) for multiple doses. Plasma clearance is high. Tirapazamine has been clinically tested in combination with cisplatin at escalating doses in a phase I trial and at therapeutic doses in three separate phase II trials in patients with advanced non-small-cell lung cancer (NSCLC) in 11 study centres. Limiting toxicity for tirapazamine at an intravenous dose of 390 mg m(-2) was acute, reversible hearing loss. Other frequently observed side-effects included muscle cramping and gastrointestinal symptoms. Tirapazamine did not cause myelosuppression, and no toxic deaths were reported in these trials. The anti-tumour efficacy against previously untreated, advanced NSCLC was evaluated by cumulative intent-to-treat analysis of 132 patients. The objective response rate (confirmed by two independent measurements) was 25% [confidence interval (CI) 17.8-33.33], with a median survival of 38.9 weeks (CI 29.4-49.9). The efficacy of tirapazamine plus cisplatin shown in these trials was better than that of historical controls with cisplatin monotherapy. Two large-scale international trials have been conducted, involving more than 70 centres, to confirm these results. The CATAPULT I trial compares tirapazamine plus cisplatin with cisplatin and has finished accrual with 446 patients. The CATAPULT II trial, which is comparing tirapazamine plus cisplatin with etoposide plus cisplatin, had enrolled 550 patients by June 1997. Follow-up is ongoing. Tirapazamine is the promising first drug from a new class of cytotoxic agents with a novel mechanism of action. It can be effectively combined with cisplatin, and possibly with other agents, because of its safety profile and lack of overlapping dose-limiting toxicity, such as myelosuppression. The combination of tirapazamine and cisplatin appears to be safe and effective in the treatment of NSCLC.
替拉扎明是一种新型的生物还原药物,对缺氧肿瘤细胞具有选择性细胞毒性。临床前试验已表明其与顺铂及其他化疗药物具有协同作用。替拉扎明的药代动力学研究显示,单次给药剂量在18 - 450 mg m(-2)范围内、多次给药剂量在9 - 390 mg m(-2)范围内时,药物暴露量随剂量增加而升高。血浆清除率较高。在11个研究中心,替拉扎明已在一项I期试验中与顺铂联合进行了剂量递增试验,并在三项针对晚期非小细胞肺癌(NSCLC)患者的单独II期试验中进行了治疗剂量试验。静脉注射剂量为390 mg m(-2)时,替拉扎明的剂量限制性毒性为急性、可逆性听力丧失。其他常见的副作用包括肌肉痉挛和胃肠道症状。替拉扎明未引起骨髓抑制,且这些试验中未报告有因毒性导致的死亡。通过对132例患者的累积意向性治疗分析,评估了替拉扎明对先前未治疗的晚期NSCLC的抗肿瘤疗效。客观缓解率(经两次独立测量确认)为25% [置信区间(CI)17.8 - 33.33],中位生存期为38.9周(CI 29.4 - 49.9)。这些试验中显示的替拉扎明加顺铂的疗效优于顺铂单药治疗的历史对照。已经进行了两项大规模国际试验,涉及70多个中心,以证实这些结果。CATAPULT I试验将替拉扎明加顺铂与顺铂进行比较,已完成446例患者的入组。CATAPULT II试验将替拉扎明加顺铂与依托泊苷加顺铂进行比较,截至1997年6月已招募550例患者。随访正在进行中。替拉扎明是一类具有新作用机制的细胞毒性药物中首个有前景的药物。由于其安全性和缺乏如骨髓抑制等重叠的剂量限制性毒性,它可有效地与顺铂联合,也可能与其他药物联合。替拉扎明与顺铂联合在NSCLC治疗中似乎是安全有效的。