Use of the ESMO-Magnitude of Clinical Benefit Scale to guide HTA recommendations on coverage and reimbursement for cancer medicines: a retrospective analysis

The Lancet Oncology Pub Date : 2024-12-02 DOI:10.1016/s1470-2045(24)00505-9

Panos Kanavos, Erica Visintin, Aris Angelis

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We evaluated which factors affect HTA outcomes and the time to positive HTA outcome, focussing on the role of clinical benefit evaluated with the European Society for Medical Oncology-Magnitude of Clinical Benefit Scale (ESMO-MCBS).<h3>Methods</h3>In this retrospective analysis, data were extracted from publicly available HTA reports and related sources from six country settings and their respective HTA agencies (Australia, Canada, England, France, the Canadian province of Quebec, and Scotland). We evaluated new cancer medicines for treating solid tumours in a non-curative setting with published ESMO-MCBS scores and that had been assessed by at least three HTA agencies between Jan 1, 2011, and Dec 31, 2020. Using ESMO-MCBS score as an independent variable, we did descriptive and multivariable regression analyses to evaluate: (1) factors associated with the time between marketing authorisation and positive (unrestricted [List] and restricted [List with Constraints]) HTA outcome; and (2) factors associated with HTA outcomes.<h3>Findings</h3>67 medicine–indication pairs used in non-curative settings were identified, totalling 360 HTA submissions (medicine–indication–country triplets) reviewed by the six HTA agencies. Factors significantly associated with a reduced interval between marketing authorisation and a positive (unrestricted or restricted) HTA outcome included a high ESMO-MCBS score (ie, 4 or 5, <em>vs</em> a low or average score of 1–3; hazard ratio [HR] per 1 month increment 1·42 [95% CI 1·11–1·81], p=0·0055), parallel review (<em>vs</em> standard marketing authorisation process; HR 1·69 [1·13–2·54], p=0·011), having a risk-sharing agreement or special funding arrangements (<em>vs</em> no funding agreement, HR 4·62 [95% CI 2·51–8·51], p<0·0001, and HR 4·16 [2·03–8·50], p=0·0001, respectively), and assessment by particular HTA agencies (pan-Canadian Oncology Drug Review <em>vs</em> National Institute for Health and Care Excellence [NICE], HR 2·82 [1·68–4·75], p=0·0001; and Haute Autorité de Santé <em>vs</em> NICE, HR 5·70 [2·87–11·33], p<0·0001). Accelerated marketing authorisation was significantly associated with a longer time to positive HTA outcome (<em>vs</em> standard authorisation process; HR 0·70 [95% CI 0·51–0·95], p=0·024). Positive HTA outcomes (both unrestricted and restricted) were significantly associated with a high ESMO-MCBS score (<em>vs</em> low or average ESMO-MCBS score; relative risk ratio [RRR] 14·10 [95% CI 3·54–56·20], p=0·0002, and RRR 4·52 [1·90–10·75], p=0·0006, respectively) and acknowledgment of unmet medical need (<em>vs</em> unmet need not recorded, RRR 22·73 [5·51–93·73], p<0·0001, and RRR 1·87 [1·18–2·97], p=0·0075, respectively). By contrast, positive HTA outcomes (unrestricted and restricted) were inversely associated with uncertainties regarding inputs to economic models informing HTA submissions (<em>vs</em> uncertainties not recorded, RRR 0·28 [0·10–0·78], p=0·014, and RRR 0·45 [0·25–0·82], p=0·010, respectively). 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Abstract

Background

Recommendations by countries’ health technology assessment (HTA) agencies are used to decide which new therapies warrant the allocation of limited health-care resources to make them available through publicly funded health systems. This process is of public health importance for balancing the dual aims of optimising patient outcomes while ensuring financial sustainability. We evaluated which factors affect HTA outcomes and the time to positive HTA outcome, focussing on the role of clinical benefit evaluated with the European Society for Medical Oncology-Magnitude of Clinical Benefit Scale (ESMO-MCBS).

Methods

In this retrospective analysis, data were extracted from publicly available HTA reports and related sources from six country settings and their respective HTA agencies (Australia, Canada, England, France, the Canadian province of Quebec, and Scotland). We evaluated new cancer medicines for treating solid tumours in a non-curative setting with published ESMO-MCBS scores and that had been assessed by at least three HTA agencies between Jan 1, 2011, and Dec 31, 2020. Using ESMO-MCBS score as an independent variable, we did descriptive and multivariable regression analyses to evaluate: (1) factors associated with the time between marketing authorisation and positive (unrestricted [List] and restricted [List with Constraints]) HTA outcome; and (2) factors associated with HTA outcomes.

Findings

67 medicine–indication pairs used in non-curative settings were identified, totalling 360 HTA submissions (medicine–indication–country triplets) reviewed by the six HTA agencies. Factors significantly associated with a reduced interval between marketing authorisation and a positive (unrestricted or restricted) HTA outcome included a high ESMO-MCBS score (ie, 4 or 5, vs a low or average score of 1–3; hazard ratio [HR] per 1 month increment 1·42 [95% CI 1·11–1·81], p=0·0055), parallel review (vs standard marketing authorisation process; HR 1·69 [1·13–2·54], p=0·011), having a risk-sharing agreement or special funding arrangements (vs no funding agreement, HR 4·62 [95% CI 2·51–8·51], p<0·0001, and HR 4·16 [2·03–8·50], p=0·0001, respectively), and assessment by particular HTA agencies (pan-Canadian Oncology Drug Review vs National Institute for Health and Care Excellence [NICE], HR 2·82 [1·68–4·75], p=0·0001; and Haute Autorité de Santé vs NICE, HR 5·70 [2·87–11·33], p<0·0001). Accelerated marketing authorisation was significantly associated with a longer time to positive HTA outcome (vs standard authorisation process; HR 0·70 [95% CI 0·51–0·95], p=0·024). Positive HTA outcomes (both unrestricted and restricted) were significantly associated with a high ESMO-MCBS score (vs low or average ESMO-MCBS score; relative risk ratio [RRR] 14·10 [95% CI 3·54–56·20], p=0·0002, and RRR 4·52 [1·90–10·75], p=0·0006, respectively) and acknowledgment of unmet medical need (vs unmet need not recorded, RRR 22·73 [5·51–93·73], p<0·0001, and RRR 1·87 [1·18–2·97], p=0·0075, respectively). By contrast, positive HTA outcomes (unrestricted and restricted) were inversely associated with uncertainties regarding inputs to economic models informing HTA submissions (vs uncertainties not recorded, RRR 0·28 [0·10–0·78], p=0·014, and RRR 0·45 [0·25–0·82], p=0·010, respectively). Regarding country-relevant effects, inverse associations with positive HTA outcomes (both unrestricted and restricted) were observed for assessment in Quebec (vs England; RRR 1·15×10⁻⁶ [1·44×10⁻⁷–9·09×10⁻⁶], p<0·0001, and RRR 0·33 (0·24–0·46), p<0·0001, respectively) and for assessment in Australia (vs England; RRR 1·78×10⁻⁶ [1·04×10⁻⁸–3·00×10⁻⁴], p<0·0001, and RRR 0·30 [0·15–0·61], p=0·0008, respectively).

Interpretation

Several factors informed HTA outcomes for new cancer medicines. A high ESMO-MCBS score, defined as indicating substantial clinical benefit, increased the likelihood of a positive HTA outcome and shortened the interval between marketing authorisation and HTA outcome, and this association was not affected by other variables. Additional factors informing HTA outcomes include evidence uncertainties and unmet medical need. Country-relevant differences exist in the time-to-HTA outcome and the propensity of some countries to achieve positive (restricted or unrestricted) outcomes compared with others.

Funding

None.

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使用esmo -临床效益等级量表来指导HTA关于癌症药物覆盖和报销的建议：回顾性分析

背景：各国卫生技术评估机构的建议用于决定哪些新疗法值得分配有限的卫生保健资源，以便通过公共资助的卫生系统提供这些新疗法。这一过程对于平衡优化患者治疗结果和确保财政可持续性的双重目标具有重要的公共卫生意义。我们评估了哪些因素会影响HTA结果和达到HTA阳性结果的时间，重点关注临床获益的作用，临床获益量表（ESMO-MCBS）由欧洲肿瘤医学学会评估。方法回顾性分析的数据来自6个国家及其各自的HTA机构（澳大利亚、加拿大、英国、法国、加拿大魁北克省和苏格兰）的公开HTA报告和相关资料。我们使用已公布的ESMO-MCBS评分，评估了用于治疗非治愈性实体肿瘤的新型抗癌药物，这些药物已在2011年1月1日至2020年12月31日期间由至少三家HTA机构评估。使用ESMO-MCBS评分作为自变量，我们进行了描述性和多变量回归分析来评估：(1)与上市许可和积极（不受限制的[列表]和受限制的[列表约束]）HTA结果之间时间相关的因素；(2)与HTA结果相关的因素。6家HTA机构共审查了360份HTA申请（药物适应症-国家三联），确定了67对用于非治疗环境的药物适应症对。与上市许可和HTA阳性（无限制或限制性）结果之间的间隔缩短显著相关的因素包括ESMO-MCBS评分较高(即4或5分，而低或平均得分为1-3分；风险比[HR]每1个月增加1.42 [95% CI 1.11 - 1.81], p= 0.0055)，平行审查(与标准上市许可程序相比；HR 1.69 [1.13 - 2.54], p= 0.011)，有风险分担协议或特殊资金安排（相对于没有资金协议，HR 4.62 [95% CI 2.51 - 8.51], p= 0.0001, HR 4.16 [2.03 - 8.50], p= 0.0001），以及特定HTA机构的评估(泛加拿大肿瘤药物审查与国家卫生与护理卓越研究所[NICE]， HR 2.82 [1.68 - 4.75], p= 0.0001；和法国高级汽车与NICE， HR 5.70 [2.87 - 11.33], p< 0.0001)。加速上市许可与获得积极HTA结果的时间较长显著相关(与标准许可程序相比；HR 0.70 [95% CI 0.51 ~ 0.95], p= 0.024]。HTA阳性结果（非限制性和限制性）与高ESMO-MCBS评分显著相关(相对于低或平均ESMO-MCBS评分；相对风险比[RRR] 14.10 [95% CI为3.54 ~ 56.20],p= 0.0002， RRR为4.52 [1.90 ~ 10.75],p= 0.0006)和未满足的医疗需求承认（与未满足的需求相比，RRR为22.73 [5.51 ~ 9.73]，RRR为0.0001，RRR为1.87 [1.18 ~ 2.97],p= 0.0075）。相比之下，积极的HTA结果（不受限制的和受限制的）与提交HTA的经济模型输入的不确定性呈负相关（与未记录的不确定性相比，RRR为0.28 [0.10 - 0.78],p= 0.014， RRR为0.45 [0.25 - 0.82],p= 0.010）。关于国家相关的影响，在魁北克省(vs英格兰；RRR为1·15×10−6[1·44×10−7-9·09×10−6]，p< 0.0001； RRR为0.33 (0.24 - 0.46),p< 0.0001)，并在澳大利亚进行评估(vs英国；RRR为1·78×10−6[1·04×10−8-3·00×10−4]，p<为0.0001，RRR为0.30 [0.15 - 0.61],p= 0.0008)。有几个因素影响了新的癌症药物的HTA结果。较高的ESMO-MCBS评分（定义为表明实质性临床获益）增加了HTA阳性结果的可能性，缩短了上市许可和HTA结果之间的间隔，并且这种关联不受其他变量的影响。影响HTA结果的其他因素包括证据不确定和未满足的医疗需求。与其他国家相比，在达到hta结果的时间和一些国家实现积极（受限制或不受限制）结果的倾向方面存在与国家相关的差异。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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The Lancet Oncology

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