β-地中海贫血输血依赖性β-地中海贫血β-基因自体细胞(β-细胞)基因添加治疗的经济评价。

Anuraag R Kansal, Odette S Reifsnider, Sarah B Brand, Neil Hawkins, Anna Coughlan, Shujun Li, Lael Cragin, Clark Paramore, Andrew C Dietz, J Jaime Caro
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引用次数: 9

摘要

背景:输血依赖性β-地中海贫血(TDT)的标准治疗(SoC)需要终身定期输血以及螯合以减少铁的积累。目的:研究人造血干细胞(“人造血干细胞”)的成本效益;LentiGlobin (β-地中海贫血)一次性基因添加治疗与TDT终身SoC治疗的比较。研究设计:微模拟模型根据输血需求决定组织铁水平的因果序列模拟TDT的生命过程,而组织铁水平又决定铁超载并发症的风险,从而增加死亡率。临床试验数据告知细胞临床参数;SoC对铁含量的影响来自现实世界的研究;铁超载并发症发生率和死亡率基于已发表的文献。背景:美国;参与者:年龄2-50岁的TDT患者干预措施:将Beti-cel与SoC进行比较。主要结果测量:使用质量调整生命年(QALYs)的增量成本效益比(ICER)结果:该模型预测,与SoC相比,beti-cel增加3.8折现生命年(LYs)或6.9 QALYs。镍氢电池的贴现寿命成本为228万美元(如果不包括镍氢电池成本,则为572,107美元),镍氢电池的贴现寿命成本为204万美元,每个QALY获得的收益为34,833美元。结论:与SoC相比,Beti-cel治疗TDT患者更具成本效益。这是由于更长的寿命和终身SoC的成本抵消。
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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Economic evaluation of betibeglogene autotemcel (Beti-cel) gene addition therapy in transfusion-dependent β-thalassemia.

Background: Standard of care (SoC) for transfusion-dependent β-thalassemia (TDT) requires lifelong, regular blood transfusions as well as chelation to reduce iron accumulation. Objective: This study investigates the cost-effectiveness of betibeglogene autotemcel ('beti-cel'; LentiGlobin for β-thalassemia) one-time, gene addition therapy compared to lifelong SoC for TDT. Study design: Microsimulation model simulated the lifetime course of TDT based on a causal sequence in which transfusion requirements determine tissue iron levels, which in turn determine risk of iron overload complications that increase mortality. Clinical trial data informed beti-cel clinical parameters; effects of SoC on iron levels came from real-world studies; iron overload complication rates and mortality were based on published literature. Setting: USA; commercial payer perspective Participants: TDT patients age 2-50 Interventions: Beti-cel is compared to SoC. Main outcome measure: Incremental cost-effectiveness ratio (ICER) utilizing quality-adjusted life-years (QALYs) Results: The model predicts beti-cel adds 3.8 discounted life years (LYs) or 6.9 QALYs versus SoC. Discounted lifetime costs were $2.28 M for beti-cel ($572,107 if excluding beti-cel cost) and $2.04 M for SoC, with a resulting ICER of $34,833 per QALY gained. Conclusion: Beti-cel is cost-effective for TDT patients compared to SoC. This is due to longer survival and cost offset of lifelong SoC.

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4.90
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审稿时长
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