Furuse K, Fukuoka M, Kato H, Horai T, Kubota K, Kodama N, Kusunoki Y, Takifuji N, Okunaka T, Konaka C
Department of Internal Medicine, National Kinki Central Hospital for Chest Diseases, Osaka, Japan.
J Clin Oncol. 1993 Oct;11(10):1852-7. doi: 10.1200/JCO.1993.11.10.1852.
A phase II study was conducted between June 1989 and February 1992 to evaluate the activity and toxicity of photodynamic therapy (PDT) with photofrin II in centrally located early-stage lung cancer and to determine the complete response (CR) rate as the primary end point.
Patients had histologically proven lung cancer and endoscopically superficial thickening or small protrusions. All lesions were located in subsegmental or larger bronchi. All patients had a performance status (PS) of 0 to 2 and arterial oxygen pressure tension (PaO2) > or = 60 mm Hg. No lymph node or distant metastases were present. All patients received photofrin II (2 mg/kg) intravenously 48 hours before PDT. Tumor lesions were superficially photoradiated by an argon dye laser or an excimer dye laser.
Of 54 patients with 64 carcinomas, 51 with 61 carcinomas were eligible for toxicity evaluation and 49 with 59 carcinomas were assessable for response. Of the 59 assessable carcinomas, 50 (84.8%; 95% confidence interval, 73.0% to 92.8%) showed a CR after initial PDT. The median duration of CR was 14.0+ months (range, 2.0+ to 32.4+). The multiple regression model indicates that estimated length of longitudinal tumor extent was the only independent prognostic factor for CR (P = .002). Five carcinomas that had a CR had a local recurrence at 6, 10, 12, 16, and 18 months after initial PDT, respectively. Toxicity assessment (World Health Organization [WHO] grade 2) showed transient elevation of ALT (1.9%), pulmonary toxicity (7.7%), and allergic reaction (7.7%), as well as sunburn (1.9%).
PDT with photofrin II has an excellent effect on patients with centrally located early-stage lung cancer who have limited tumor invasion extending over a small area (< or = 1 cm).
1989年6月至1992年2月开展了一项II期研究,以评估用卟吩姆钠(光卟啉II)进行光动力疗法(PDT)对中心型早期肺癌的有效性及毒性,并将完全缓解(CR)率确定为主要终点。
患者经组织学确诊为肺癌,且在内镜检查下可见表面增厚或小的隆起。所有病变均位于亚段或更大的支气管。所有患者的体能状态(PS)为0至2,动脉血氧分压(PaO2)≥60 mmHg。无淋巴结或远处转移。所有患者在PDT前48小时静脉注射卟吩姆钠(2 mg/kg)。肿瘤病变用氩染料激光或准分子染料激光进行表面光辐射。
54例患者共64处癌灶,51例患者的61处癌灶符合毒性评估标准,49例患者的59处癌灶可评估疗效。在59处可评估疗效的癌灶中,50处(84.8%;95%置信区间,73.0%至92.8%)在初次PDT后显示CR。CR的中位持续时间为14.0 +个月(范围,2.0 +至32.4 +)。多元回归模型表明,纵向肿瘤范围的估计长度是CR的唯一独立预后因素(P = .002)。5处达到CR的癌灶分别在初次PDT后6、10、12、16和18个月出现局部复发。毒性评估(世界卫生组织[WHO] 2级)显示谷丙转氨酶短暂升高(1.9%)、肺部毒性(7.7%)、过敏反应(7.7%)以及晒伤(1.9%)。
用卟吩姆钠进行的PDT对肿瘤侵犯局限于小面积(≤1 cm)的中心型早期肺癌患者有极佳疗效。
