PP93 Health Technology Assessments For Rare Diseases In Australia: A Case Study On Cystic Fibrosis

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Himani Jaiswal, Anna D’Ausilio, Matthew Bending
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引用次数: 0

Abstract

Introduction

Currently, no cure exists for the 1 in 2,500 Australian babies born with potentially fatal cystic fibrosis (CF). The authors conducted a health technology assessment (HTA) case study analysis of all regulatory approved CF treatments in Australia from January 1994 to July 2022. Submissions were also made under the Therapeutics Goods Administration and Pharmaceutical Benefits Advisory Committee (TGA-PBAC) parallel process.

Methods

Public summary and source materials were researched to understand relevant clinical and health economic evidence requirements, and access decisions from Australia’s lead HTA body, PBAC.

Results

The review found that there are more than seven approved products in Australia. Of those, all four novel CF transmembrane conductance regulator (CFTR) modulating medications, which treat the underlying disease, received an orphan drug designation and were eventually listed. However, initial HTA decisions were mixed, with one recommended (25%), one not recommended (25%), and two deferred (50%). Clinical efficacy, cost-effectiveness, clinical need, as well as patient/carer-centric perspectives were most influential in HTA recommendations. Like other rare disease treatments, price, high incremental cost-effectiveness ratios (ICERs), uncertainty around cost-effectiveness and/or efficacy were key barriers to positive decisions. Notably, Australian stakeholders did not recommend CF medicines when their ICERs significantly exceeded a threshold of AUD200,000 (USD134,700) per quality-adjusted life year (QALY) gained. Administratively, Australia addresses risks associated with poor cost-effectiveness and high costs through managed access programs, risk-sharing agreements (RSA) and special pricing arrangements.

Recently approved elexacaftor-tezacaftor-ivacaftor would be inaccessible to many Australian patients without inclusion in the Pharmaceutical Benefits Scheme (PBS); this placement increases access by limiting patients’ payments to AUD42.50 (USD28.62) maximum per prescription. Alternatively, manufacturers of therapies for other chronic or rare life-threatening conditions can participate in Australia’s Highly Specialised Drugs Program and/or Life Saving Drugs Program to facilitate access.

Conclusions

Companies can accelerate and optimize market access by using the TGA-PBAC parallel process. Other Asia-Pacific countries can model components of Australia’s approach to advancing access to innovative, live-saving therapies.

PP93 澳大利亚罕见病卫生技术评估:囊性纤维化案例研究
目前,澳大利亚每2500名新生儿中就有1名患有潜在致命的囊性纤维化(CF),目前还没有治愈方法。作者对1994年1月至2022年7月澳大利亚所有监管部门批准的CF治疗进行了卫生技术评估(HTA)案例研究分析。在治疗药品管理局和药品福利咨询委员会(TGA-PBAC)平行程序下也提交了意见书。方法对公开摘要和原始资料进行研究,了解相关临床和卫生经济证据要求,以及澳大利亚HTA主要机构PBAC的获取决定。结果审查发现,有超过7种产品在澳大利亚获得批准。其中,所有四种治疗潜在疾病的新型CF跨膜传导调节剂(CFTR)调节药物都获得了孤儿药的称号,并最终上市。然而,最初的HTA决定是混合的,一个推荐(25%),一个不推荐(25%),两个延期(50%)。临床疗效、成本效益、临床需求以及以患者/护理为中心的观点对HTA的建议影响最大。与其他罕见病治疗一样,价格、高增量成本效益比(ICERs)、成本效益和/或疗效的不确定性是做出积极决策的主要障碍。值得注意的是,当澳大利亚利益相关者的ICERs显著超过每个质量调整生命年(QALY)获得的200,000澳元(134,700美元)的阈值时,他们不推荐CF药物。在行政方面,澳大利亚通过管理准入计划、风险分担协议(RSA)和特殊定价安排来解决与低成本效益和高成本相关的风险。如果不纳入药品福利计划(PBS),许多澳大利亚患者将无法获得最近批准的elexaftor - tezactor -ivacaftor;这种布局通过将患者每次处方的最高付款限制在42.50澳元(28.62美元)来增加可及性。另外,治疗其他慢性或罕见危及生命的疾病的药物制造商可以参加澳大利亚的高度专业化药物计划和/或救生药物计划,以促进获取。结论TGA-PBAC并行流程可加快和优化企业市场准入。其他亚太国家可以模仿澳大利亚促进获得创新、挽救生命的治疗方法的组成部分。
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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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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