PenTAG, Peninsula College of Medicine and Dentistry, Universities of Exeter and Plymouth, UK.
Health Technol Assess. 2011 May;15 Suppl 1:61-7. doi: 10.3310/hta15suppl1/07.
This paper presents a summary of the evidence review group (ERG) report into the clinical effectiveness and cost-effectiveness of ofatumumab for the treatment of refractory chronic lymphocytic leukaemia (CLL), based upon the manufacturer's submission (MS) to the National Institute for Health and Clinical Excellence (NICE) as part of the single technology appraisal process. The submitted clinical evidence included one study: a non-randomised, single-arm study. Two other studies were identified but both were non-comparative and provided evidence for therapies other than ofatumumab. For this reason these studies were not discussed in full in the main body of the submission. In the Hx-CD20-406 study, the overall response rate was 58% (99% confidence interval 40% to 74%, p < 0.001). Complete resolution of constitutional symptoms and improved performance status occurred in 57% of patients. Median progression-free survival (PFS) and overall survival (OS) times were 5.7 and 13.7 months, respectively. The most common adverse events during treatment were infusion reactions and infections, which were primarily grade 1 or 2 events. The MS concluded that ofatumumab provides a new, effective and well-tolerated therapy for patients with CLL who are refractory to both fludarabine and alemtuzumab [double refractory (DR)]. The ERG undertook a critical appraisal of the submission. The ERG had a number of concerns regarding the manufacturer's estimates of effectiveness based on evidence from a single-arm, non-randomised study. An 'area-under-the-curve' or 'partitioned-survival' model was used to project expected clinical and economic outcomes for patients with DR CLL who were assumed to receive ofatumumab or best supportive care (BSC). The model had a three-state structure: 'alive pre-progression', 'alive post progression' and 'dead'. Overall, the modelling approach is reasonable given the limited evidence available for the drug in the patient population under review. However, a number of uncertainties were identified in the economic evaluation; for example, the BSC arm used data from patients in the Hx-CD20-406 study who did not respond to ofatumumab treatment - 'non-responders' - and the ofatumumab arm used data from all of those treated in the Hx-CD20-406 study. Further uncertainty arose regarding the choice of utilities, the omission of 17p and 11q chromosomal deletions as factors in the Cox proportional hazards models for PFS and OS, and the omission of the costs of drugs in progressive disease. It was felt that these factors biased cost-effectiveness in favour of ofatumumab. When revisions were made to the assumptions in the model based on the ERG's review of the published and submitted evidence, the revised base-case incremental cost-effectiveness ratio for ofatumumab increased to £ 81,500 per quality-adjusted life-year. The final appraisal determination was issued by NICE in September 2010 (www.nice.org.uk/nicemedia/live/12264/50758/50758.pdf).
本文总结了制药公司向英国国家卫生与临床优化研究所(NICE)提交的 OFLUMEN 用于治疗难治性慢性淋巴细胞白血病(CLL)的临床疗效和成本效益评估报告,作为单一技术评估过程的一部分。提交的临床证据包括一项研究:一项非随机、单臂研究。另外两项研究虽然被识别出来,但都不具有可比性,并且提供的是除奥法木单抗以外的治疗方法的证据。因此,这些研究在提交材料的正文部分没有被详细讨论。在 Hx-CD20-406 研究中,总缓解率为 58%(99%置信区间为 40%至 74%,p<0.001)。57%的患者出现了症状完全缓解和体能状态改善。无进展生存期(PFS)和总生存期(OS)中位数分别为 5.7 个月和 13.7 个月。治疗期间最常见的不良反应是输注反应和感染,主要为 1 级或 2 级事件。该报告总结称,奥法木单抗为氟达拉滨和阿仑单抗均耐药的 CLL 患者提供了一种新的、有效且耐受性良好的治疗方法[双重难治(DR)]。ERG 对提交材料进行了严格审查。ERG 对制药公司基于单臂、非随机研究证据得出的有效性估计存在一些担忧。使用“曲线下面积”或“分割生存”模型来预测假定接受奥法木单抗或最佳支持治疗(BSC)的 DR CLL 患者的预期临床和经济结局。该模型具有三状态结构:“无进展前存活”、“无进展后存活”和“死亡”。总的来说,考虑到药物在审查人群中的有限证据,该建模方法是合理的。然而,在经济评估中确定了一些不确定性;例如,BSC 组使用了 Hx-CD20-406 研究中未对奥法木单抗治疗有反应的患者(“无应答者”)的数据,而奥法木单抗组使用了 Hx-CD20-406 研究中所有接受治疗的患者的数据。在选择效用、在 PFS 和 OS 的 Cox 比例风险模型中忽略 17p 和 11q 染色体缺失以及忽略进展性疾病的药物成本方面,也存在进一步的不确定性。人们认为这些因素使成本效益有利于奥法木单抗。当根据 ERG 对已发表和提交证据的审查对模型假设进行修订时,奥法木单抗的修订后增量成本效益比增加到每 QALY 81500 英镑。NICE 于 2010 年 9 月发布了最终评估决定(www.nice.org.uk/nicemedia/live/12264/50758/50758.pdf)。
