Howard Dena R, Munir Talha, McParland Lucy, Rawstron Andy C, Chalmers Anna, Gregory Walter M, O'Dwyer John L, Smith Alison, Longo Roberta, Varghese Abraham, Smith Alexandra, Hillmen Peter
Clinical Trials Research Unit, Leeds Institute of Clinical Trials Research, University of Leeds, Leeds, UK.
Department of Haematology, St James's University Hospital, Leeds, UK.
Health Technol Assess. 2017 May;21(28):1-374. doi: 10.3310/hta21280.
The conventional frontline therapy for fit patients with chronic lymphocytic leukaemia (CLL) is fludarabine, cyclophosphamide and rituximab (FCR). Rituximab (Mabthera, Roche Products Ltd) targets the CD20 antigen, which is expressed at low levels in CLL. The standard dose of rituximab in CLL (375 mg/m in cycle 1 and 500 mg/m in cycles 2-6) was selected based on toxicity data only. Small doses of rituximab (as low as 20 mg) have biological activity in CLL, with an immediate reduction in circulating CLL cells and down-regulation of CD20. Phase II trials had suggested improved efficacy with the addition of mitoxantrone to FCR. The key assumption for the Attenuated dose Rituximab with ChemoTherapy In CLL (ARCTIC) trial was that the addition of mitoxantrone to fludarabine, cyclophosphamide and low-dose rituximab would be more effective than conventional FCR.
To assess whether fludarabine, cyclophosphamide, mitoxantrone and low-dose rituximab (FCM-miniR) (100 mg of rituximab per cycle) was non-inferior to FCR in frontline CLL. Complete response (CR) rate was the primary end point, with the secondary end points being progression-free survival (PFS), overall survival (OS), overall response rate, eradication of minimal residual disease (MRD), safety and cost-effectiveness.
ARCTIC was a UK multicentre, randomised, controlled, open, Phase IIB non-inferiority trial in previously untreated CLL. A total of 206 patients with previously untreated CLL who required treatment, according to the International Workshop on Chronic Lymphocytic Leukaemia criteria, were to be randomised to FCR or FCM-miniR. There was an independent Data Monitoring and Ethics Committee (DMEC) with a pre-planned interim efficacy assessment on 103 participants.
The DMEC's interim analysis led to early trial closure. Although the response rates in both arms were higher than anticipated, FCM-miniR had a lower CR rate than FCR. This was partly attributable to the higher toxicity associated with mitoxantrone. A total of 100 participants completed FCR, 79 completed FCM-miniR and 21 commenced FCM-miniR but switched to FCR following DMEC recommendations. The CR rate for participants receiving FCR was 76%, compared with 55% for FCM-miniR (adjusted odds ratio 0.37; 95% confidence interval 0.19 to 0.73). Key secondary end points also showed that FCR was superior, with more participants achieving MRD negativity (57% for FCR vs. 46% for FCM-miniR). More participants experienced a serious adverse reaction with FCM-miniR compared with FCR (50% vs. 41%). At a median of 37.3 months' follow-up, the PFS and OS rates are good compared with previous studies, with no significant difference between the treatment arms. The economic analysis indicates that because FCM-miniR is less effective than FCR, FCM-miniR is not expected to be cost-effective over a lifetime horizon, producing a mean cost-saving of -£7723, a quality-adjusted life-year loss of -0.73 and a resulting incremental net monetary loss of -£6780.
FCM-miniR is less well tolerated, with poorer response rates, than FCR, partly owing to the additional toxicity associated with mitoxantrone. In view of this, FCM-miniR will not be taken forward into a larger definitive Phase III trial. The trial demonstrated that oral FCR yields extremely high response rates compared with historical series with intravenous chemotherapy.
We shall compare the results of ARCTIC with those of the ADMIRE (Does the ADdition of Mitoxantrone Improve Response to FCR chemotherapy in patients with CLL?) trial, which compared FCR with FCM-R to assess the efficacy of low- versus standard-dose rituximab, allowing for the toxicity associated with mitoxantrone.
Current Controlled Trials ISRCTN16544962.
This project was funded by the NIHR Health Technology Assessment programme and will be published in full in ; Vol. 21, No. 28. See the NIHR Journals Library website for further project information.
对于适合接受治疗的慢性淋巴细胞白血病(CLL)患者,传统的一线治疗方案是氟达拉滨、环磷酰胺和利妥昔单抗(FCR)。利妥昔单抗(美罗华,罗氏产品有限公司)靶向CD20抗原,该抗原在CLL中低水平表达。CLL中利妥昔单抗的标准剂量(第1周期为375mg/m²,第2 - 6周期为500mg/m²)仅基于毒性数据选定。小剂量利妥昔单抗(低至20mg)在CLL中具有生物学活性,可使循环中的CLL细胞立即减少并下调CD20。II期试验表明,在FCR方案中加入米托蒽醌可提高疗效。CLL中减剂量利妥昔单抗联合化疗(ARCTIC)试验的关键假设是,在氟达拉滨、环磷酰胺和低剂量利妥昔单抗方案中加入米托蒽醌比传统的FCR方案更有效。
评估氟达拉滨、环磷酰胺、米托蒽醌和低剂量利妥昔单抗(FCM - miniR,每周期100mg利妥昔单抗)在一线CLL治疗中是否不劣于FCR。完全缓解(CR)率是主要终点,次要终点包括无进展生存期(PFS)、总生存期(OS)、总缓解率、微小残留病(MRD)清除率、安全性和成本效益。
ARCTIC是一项在英国进行的多中心、随机、对照、开放的IIB期非劣效性试验,针对既往未治疗过的CLL患者。根据慢性淋巴细胞白血病国际研讨会标准,共有206例需要治疗的既往未治疗过的CLL患者被随机分配至FCR或FCM - miniR组。设有独立的数据监测和伦理委员会(DMEC),并预先计划对103名参与者进行中期疗效评估。
DMEC的中期分析导致试验提前结束。尽管两组的缓解率均高于预期,但FCM - miniR的CR率低于FCR。这部分归因于与米托蒽醌相关的较高毒性。共有100名参与者完成了FCR治疗,79名完成了FCM - miniR治疗,21名开始接受FCM - miniR治疗,但根据DMEC的建议转而接受FCR治疗。接受FCR治疗的参与者的CR率为76%,而FCM - miniR为55%(调整后的优势比为0.37;95%置信区间为0.19至0.73)。关键次要终点也表明FCR更优,更多参与者实现了MRD阴性(FCR为57%,FCM - miniR为46%)。与FCR相比,接受FCM - miniR治疗的参与者发生严重不良反应的更多(50%对41%)。在中位随访37.3个月时,与既往研究相比,PFS和OS率良好,治疗组之间无显著差异。经济分析表明,由于FCM - miniR的疗效低于FCR,预计FCM - miniR在终身范围内不具有成本效益,平均节省成本为 - 7723英镑,质量调整生命年损失为 - 0.73,导致增量净货币损失为 - 6780英镑。
FCM - miniR的耐受性不如FCR,缓解率较差,部分原因是与米托蒽醌相关的额外毒性。鉴于此,FCM - miniR不会推进到更大规模的确定性III期试验。该试验表明,与既往静脉化疗的历史系列相比,口服FCR产生的缓解率极高。
我们将把ARCTIC试验的结果与ADMIRE(米托蒽醌的加入是否能改善CLL患者对FCR化疗的反应?)试验的结果进行比较,该试验比较了FCR与FCM - R,以评估低剂量与标准剂量利妥昔单抗的疗效,并考虑了与米托蒽醌相关的毒性。
当前受控试验ISRCTN16544962。
该项目由英国国家卫生研究院卫生技术评估计划资助,将全文发表于;第21卷,第28期。有关更多项目信息,请访问英国国家卫生研究院期刊图书馆网站。
