Rebattu P, Quantin X, Ardiet C, Morere J F, Azarian M R, Schuller-Lebeau M P, Pujol J L
Cancer Institute Centre Léon Bérard 28, rue Laënnec, 69373 Lyon, Cedex, France.
Lung Cancer. 2001 Aug-Sep;33(2-3):277-87. doi: 10.1016/s0169-5002(00)00243-9.
The good efficacy-toxicity ratio of both docetaxel and gemcitabine in non-small cell lung cancer (NSCLC) stimulates the investigation of the combination of these drugs as a first line chemotherapy. This two-step study firstly aimed at determining the maximum tolerated and recommended doses of docetaxel given every 3 weeks in combination with a fixed dose of gemcitabine; the phase I study paid particular attention to pharmacokinetics. Afterwards, the safety and efficacy of the recommended dose was carefully assessed in the phase II-step.
The following range of docetaxel dosages were tested in the phase I study; 60, 75, 85, and 100 mg m(-2) given on day 8 in combination with gemcitabine 1000 mg m(-2) delivered on days 1 and 8 of a 3-week cycle. Haematopoietic growth factors were not allowed. The treatment was delivered on an outpatient basis. Main eligibility criteria consisted of stage III b or IV histologically proven NSCLC, Eastern Co-operative Oncology Group (ECOG) performance status PS < or =2, age < or =70 years, measurable disease, adequate blood counts, chemistry, and no symptomatic brain metastasis.
Four centres enrolled 49 patients (eight having been pre-treated); 16 in phase I and 33 in phase II. The maximal tolerated dose was almost reached at the last dose level (i.e. docetaxel, 100 mg m(-2)). Consequently, we considered the 85 mg m(-2) level as the recommended dose. There was a positive relationship of the docetaxel dose to the area under the curve of this drug. Toxicity was assessable in all patients. Among the 200 cycles delivered, 192 were assessable for this feature. Main toxicity was grade 3-4 neutropenia affecting 23 patients (47% of the population; 23% of the cycles). Six febrile episodes were recorded leading to two treatment-related deaths. Another patient died from congestive cardiac failure. In addition, six patients experienced interstitial pneumonitis, (one half considered as severe), two of them having received the recommended dose. All patients recovered from this toxicity after corticosteroids. Fourteen patients out of the whole population (29%; 95% CI [17-43], including ten patients receiving the recommended dose), achieved an objective response. Median follow-up was 14 months (range, 0.3-29.4). Median survival was 11.2 months (95% CI [8.3-13.2]), and the 1-year survival rate was 45%.
Gemcitabine, 1000 mg m(-2) days 1 and 8 in combination with docetaxel, 85 mg m(-2), day 8, given every 3 weeks could be considered as an active regimen with manageable toxicities in locally advanced or metastatic NSCLC. This study deserves further comparisons with classical platinum-based regimens.
多西他赛和吉西他滨在非小细胞肺癌(NSCLC)中良好的疗效-毒性比促使人们研究这两种药物联合作为一线化疗方案。这项分两步进行的研究首先旨在确定每3周给予一次的多西他赛与固定剂量吉西他滨联合使用时的最大耐受剂量和推荐剂量;I期研究特别关注药代动力学。之后,在II期研究中仔细评估了推荐剂量的安全性和疗效。
在I期研究中测试了以下多西他赛剂量范围;第8天给予60、75、85和100mg/m²,与3周周期第1天和第8天给予的1000mg/m²吉西他滨联合使用。不允许使用造血生长因子。治疗在门诊进行。主要入选标准包括组织学证实的IIIb期或IV期NSCLC、东部肿瘤协作组(ECOG)体能状态评分为PS≤2、年龄≤70岁、可测量的疾病、足够的血细胞计数、化学指标,且无有症状的脑转移。
四个中心共纳入49例患者(8例曾接受过预处理);I期16例,II期33例。在最后一个剂量水平(即多西他赛100mg/m²)几乎达到了最大耐受剂量。因此,我们将85mg/m²水平视为推荐剂量。多西他赛剂量与该药物曲线下面积呈正相关。所有患者的毒性均可评估。在给予的200个周期中,192个周期可评估该特征。主要毒性为3-4级中性粒细胞减少,影响23例患者(占总人群的47%;占周期的23%)。记录到6次发热发作,导致2例与治疗相关的死亡。另1例患者死于充血性心力衰竭。此外,6例患者发生间质性肺炎(其中一半被认为严重),其中2例接受了推荐剂量。所有患者在使用皮质类固醇后从这种毒性中恢复。全部患者中有14例(29%;95%CI[17-43],包括10例接受推荐剂量的患者)获得客观缓解。中位随访时间为14个月(范围0.3-29.4个月)。中位生存期为11.2个月(95%CI[8.3-13.2]),1年生存率为45%。
每3周在第1天和第8天给予1000mg/m²吉西他滨,第8天给予85mg/m²多西他赛联合方案可被视为局部晚期或转移性NSCLC中一种毒性可管理的有效方案。本研究值得与经典的铂类方案进行进一步比较。
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