吸入性阿霉素联合铂类疗法治疗晚期非小细胞肺癌的I/II期研究
Phase I/II study of inhaled doxorubicin combined with platinum-based therapy for advanced non-small cell lung cancer.
作者信息
Otterson Gregory A, Villalona-Calero Miguel A, Hicks William, Pan Xueliang, Ellerton John A, Gettinger Scott N, Murren John R
机构信息
Comprehensive Cancer Center and Center for Biostatistics, The Ohio State University, Columbus, Ohio, USA.
出版信息
Clin Cancer Res. 2010 Apr 15;16(8):2466-73. doi: 10.1158/1078-0432.CCR-09-3015. Epub 2010 Apr 6.
PURPOSE
We have shown the feasibility of administering inhaled doxorubicin to patients with cancer. This study evaluated inhaled doxorubicin combined with cisplatin and docetaxel in patients with non-small cell lung cancer. The principal objective was to determine safety and, secondarily, efficacy.
EXPERIMENTAL DESIGN
Patients who had chemo-naïve advanced non-small cell lung cancer were enrolled in the study. Adequate organ and pulmonary function was required: diffusing capacity for carbon monoxide/forced expiratory volume in 1 second/forced vital capacity > or =50%, resting/exercise O(2) saturation > or =90%/85%. In phase I, doxorubicin was escalated: dose level 1 (6 mg/m(2)) and level 2 (7.5 mg/m(2)). Escalation was permitted if < or =2 of 6 patients experienced pulmonary dose-limiting toxicity (grade 2 Radiation Therapy Oncology Group lung morbidity; resting O(2) saturation of <85%; decrease in diffusing capacity for carbon monoxide, forced vital capacity, or forced expiratory volume in 1 second of > or =20% from baseline or < or =30% of predicted; or grade 3 Common Terminology Criteria for Adverse Events version 3.0 pulmonary toxicity). Doses of cisplatin and docetaxel were 75 mg/m(2). Treatments and pulmonary function tests were repeated every 21 days, with up to eight cycles for responding patients.
RESULTS
Twenty-eight patients were treated at level 1 and eight patients at level 2. Doxorubicin was escalated to 7.5 mg/m(2), however, after two patients developed pulmonary dose-limiting toxicity; the remainder were treated at 6.0 mg/m(2). Twenty-four evaluable patients received at least two courses or had progressive disease following the first course at the phase II dose. Toxicity was associated with i.v. chemotherapy although one patient had delayed pulmonary toxicity responding to corticosteroids and oxygen. Seven (29%) evaluable patients responded (six partial responses and one complete response) and 13 (54%) patients had stable disease for up to eight cycles.
CONCLUSION
Although this combination was safe, the primary objective was not met and will not be pursued further.
目的
我们已证明对癌症患者给予吸入性阿霉素的可行性。本研究评估了吸入性阿霉素联合顺铂和多西他赛用于非小细胞肺癌患者的情况。主要目的是确定安全性,其次是疗效。
实验设计
初治的晚期非小细胞肺癌患者纳入本研究。要求器官和肺功能良好:一氧化碳弥散量/第1秒用力呼气量/用力肺活量≥50%,静息/运动时氧饱和度≥90%/85%。在I期,阿霉素剂量逐步增加:剂量水平1(6mg/m²)和水平2(7.5mg/m²)。如果6名患者中≤2名出现肺部剂量限制性毒性(2级放射治疗肿瘤学组肺部发病率;静息氧饱和度<85%;一氧化碳弥散量、用力肺活量或第1秒用力呼气量较基线下降≥20%或<预测值的30%;或3级不良事件通用术语标准第3.0版肺部毒性),则允许剂量增加。顺铂和多西他赛的剂量为75mg/m²。每21天重复进行治疗和肺功能测试,反应良好的患者最多进行8个周期。
结果
28名患者接受1级剂量治疗,8名患者接受2级剂量治疗。然而,有2名患者出现肺部剂量限制性毒性后,阿霉素剂量增加至7.5mg/m²;其余患者接受6.0mg/m²治疗。24名可评估患者在II期剂量下接受了至少两个疗程或在第一个疗程后出现疾病进展。毒性与静脉化疗有关,尽管有1名患者出现了对皮质类固醇和氧气有反应的延迟性肺部毒性。7名(29%)可评估患者有反应(6名部分缓解和1名完全缓解),13名(54%)患者疾病稳定长达8个周期。
结论
虽然这种联合治疗是安全的,但未达到主要目标,不会进一步进行研究。
Zotero 插件