Freyer G, Rougier P, Bugat R, Droz J P, Marty M, Bleiberg H, Mignard D, Awad L, Herait P, Culine S, Trillet-Lenoir V
Medical Oncology Unit and EA 643, Centre Hospitalier Lyon-Sud, Pierre-Bénite, Lyon, France.
Br J Cancer. 2000 Aug;83(4):431-7. doi: 10.1054/bjoc.2000.1303.
Our purpose was to determine, in patients with metastatic colorectal carcinoma treated with irinotecan single-agent after 5-FU failure, the most significant predictive parameters for tumour response, progression-free survival and toxicity. Between October 1992 and April 1995, 455 patients with 5-FU resistant metastatic colorectal carcinoma entered four consecutive phase II trials. The first two studies assessed tumour response, the other two were randomized studies which assessed the efficacy of racecadotril to prevent irinotecan-induced diarrhoea. Due to homogeneous main eligibility criterias, data from those studies could be pooled for statistical analysis. Potential clinical and biological predictive factors (PF) for toxicity, tumour growth control, e.g. response or stabilization and progression-free survival (PFS), were studied in multivariate analysis. 363 patients were evaluable for response, 432 were evaluable for PFS, 368 for neutropenia and 416 for delayed diarrhoea, respectively. Normal baseline haemoglobin level (Hb), time since diagnosis of colorectal carcinoma, grade 3 or 4 neutropenia or diarrhoea at first cycle and a low number of organs involved were the most PF for tumour growth control (P<0.05). Significant prognostic variables for PFS were WHO Performance Status, liver and lymph-node involvement, time since diagnosis, age and CEA value (P < or =0.02). Six groups of patients based on the number of unfavourable prognostic factors are presented. Baseline bilirubin, haemoglobin level, number of organs involved and time from diagnosis were PF for neutropenia; PS, serum creatinine, leukocyte count, time from 5-FU progression and prior abdominopelvic irradiation were PF for delayed diarrhoea (P< or =0.05). These PF should help clinicians to anticipate for a given patient the probability to observe a response/stabilization or a toxicity. These results should also be prospectively confirmed in ongoing or future trials using irinotecan, both as a single agent and in combination with other drugs.
我们的目的是确定在5-氟尿嘧啶(5-FU)治疗失败后接受伊立替康单药治疗的转移性结直肠癌患者中,对肿瘤反应、无进展生存期和毒性最具显著预测性的参数。1992年10月至1995年4月期间,455例对5-FU耐药的转移性结直肠癌患者连续参加了四项II期试验。前两项研究评估肿瘤反应,另外两项是随机研究,评估消旋卡多曲预防伊立替康所致腹泻的疗效。由于主要入选标准相同,这些研究的数据可汇总进行统计分析。在多变量分析中研究了毒性、肿瘤生长控制(如反应或稳定)和无进展生存期(PFS)的潜在临床和生物学预测因素(PF)。分别有363例患者可评估反应,432例可评估PFS,368例可评估中性粒细胞减少,416例可评估延迟性腹泻。正常的基线血红蛋白水平(Hb)、结直肠癌诊断后的时间、首个周期出现3级或4级中性粒细胞减少或腹泻以及受累器官数量少是肿瘤生长控制的最主要PF(P<0.05)。PFS的显著预后变量为世界卫生组织(WHO)体能状态、肝脏和淋巴结受累情况、诊断后的时间、年龄和癌胚抗原(CEA)值(P≤0.02)。根据不良预后因素数量列出了六组患者。基线胆红素、血红蛋白水平、受累器官数量和诊断后的时间是中性粒细胞减少的PF;体能状态、血清肌酐、白细胞计数、5-FU进展后的时间和先前的腹盆腔放疗是延迟性腹泻的PF(P≤0.05)。这些PF应有助于临床医生预测特定患者出现反应/稳定或毒性的概率。这些结果也应在正在进行的或未来使用伊立替康单药及与其他药物联合治疗的试验中得到前瞻性证实。
