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首页> 外文期刊>ClinicoEconomics and Outcomes Research >Economic Evaluation of Single versus Combination Immuno-Oncology Therapies: Application of a Novel Modelling Approach in Metastatic Melanoma
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Economic Evaluation of Single versus Combination Immuno-Oncology Therapies: Application of a Novel Modelling Approach in Metastatic Melanoma

机译:单一与组合免疫肿瘤疗法的经济评价:一种新型模拟方法在转移性黑色素瘤中的应用

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Background: Existing economic model frameworks may not adequately capture the atypical treatment response patterns in immuno-oncology (I-O) compared with conventional therapies and thus may fail to represent the full clinical value associated with disease dynamics and improved survival. Objective: A cost-effectiveness analysis (CEA) of the I-O Regimen (nivolumab/ipilimumab) versus ipilimumab alone in advanced melanoma was carried out by applying a 5-state partitioned survival model (PSM) as a case study, to explore the I-O treatment response and clinical outcomes. The findings were compared with those of a conventional 3-state PSM. Materials and?Methods: The case study extends the conventional 3-state PSM, by separating the pre-progression state into non-responders and responders, and the post-progression state into normal and I-O progression to account for delayed treatment effects preceding clinical response. Model states were populated using patient-level data (where possible), mapping from the best overall response (BOR), and survival analysis with flexible and traditional parametric methods. Survival functions were applied to progression-free survival (PFS) and overall survival (OS) endpoints across treatment arms using the 4-year follow-up data (data available at the time of the research; since then 5-year follow-up data have been published) from the CheckMate 067 trial. Information on BOR was used as a means of differentiating the I-O treatment response in addition to the outcomes of progression-free and progressed disease. A UK National Health Service and personal social services (NHS/PSS) perspective over a lifetime horizon was used with outcomes discounted at 3.5% annually. Results: The 5-state PSM generated an increase in quality adjusted life years (QALYs) in both treatment arms and gave a more granular description of patients’ health profiles compared with the traditional 3-state PSM. The incremental QALY increased by 13% (from 2.62 to 2.95 QALYs) and the incremental cost decreased by 12% (£ 29,125 to £ 25,678) with the 5-state model. In both models, the Regimen had an incremental cost-effectiveness ratio (ICER) relative to ipilimumab alone within the lower bound of the National Institute for Health and Care Excellence (NICE) reference range (£ 20,000 per QALY gained). Conclusion: A 5-state economic model, incorporating relevant I-O health states, can be more informative to gain insight into treatment response and progression differences that are not commonly captured in existing economic models. Clinical trial endpoints, including those relating to treatment response, which are not directly reported in ongoing I-O trials, can be mapped on to the proposed modelled health states (although assumptions are required to do so). Improvements in reporting treatment response in future I-O clinical trials could help to?further validate and improve the proposed model framework.
机译:背景:与常规疗法相比,现有的经济模型框架可能无法充分捕获免疫肿瘤学(I-O)中的非典型治疗响应模式,因此可能未能代表与疾病动态相关的全部临床价值和改善的存活。目的:通过将5状态分区生存模型(PSM)作为案例研究,进行IO方案(Nivolumab / Ipilimumab)与IpiLimumab的成本效益分析(Nivolumab / Ipilimumab)与Ipilemimab进行高级黑色素瘤,以探讨IO治疗反应和临床结果。将研究结果与传统的3态PSM的结果进行比较。材料和呢?方法:案例研究通过将前进状态分离成非响应者和响应者,并将前进状态分离成正常和IO进程来延伸常规的3态PSM,以考虑临床反应前后的延迟治疗效果。使用患者级数据(在可能)中填充模型状态,从最佳总响应(BOR)映射,以及具有灵活和传统参数方法的生存分析。使用4年的后续数据(研究时提供的数据提供的数据,将存活功能应用于无进展的存活(PFS)和整体存活(OS)端点;从那时起,从那时起5年的后续数据已发布)来自Checkmate 067试验。除了无进展和进展疾病的结果之外,硼的信息用作区分I-O治疗反应的方法。英国国家卫生服务和个人社会服务(NHS / PSS)在一生视野上的角度被使用,其结果每年折扣3.5%。结果:5州PSM在两种治疗臂中产生了质量调整的寿命(QALYS)的增加,并与传统的3态PSM相比,对患者健康型材的更粒度描述。增量QALY增加了13%(从2.62到2.95QALYS),增量成本下降了12%(29,125英镑至25,678英镑),5状态模型。在两种模型中,该方案在国家健康和护理研究所的下限(尼斯)参考范围内(QALY每年20,000英镑),该方案具有相对于IPILIMIMAB的增量成本效益率(ICER)。结论:纳入相关I-O卫生国家的5州经济模式可能更有信息,可以进入洞察力响应和进展差异,并在现有的经济模型中不常见。临床试验终点,包括与治疗反应有关的临床试验,这些临床目录在正在进行的I-O试验中没有直接报告,可以映射到拟议的建模的健康状态(尽管所需的假设需要这样做)。未来I-O临床试验中报告治疗响应的改进有助于?进一步验证和改进拟议的模型框架。

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