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β-地中海贫血慢性铁过载患者地拉罗司的终生成本-效用分析:英国视角。

Lifetime cost-utility analyses of deferasirox in beta-thalassaemia patients with chronic iron overload: a UK perspective.

机构信息

University of Adelaide, Adelaide, Australia.

出版信息

Clin Drug Investig. 2012 Dec;32(12):805-15. doi: 10.1007/s40261-012-0008-2.

Abstract

BACKGROUND AND OBJECTIVES

Regular blood transfusions for beta-thalassaemia patients lead to the accumulation of iron deposits in the body. In order to remove such deposits, iron chelation therapy is required. Subcutaneously administered deferoxamine has been the gold standard chelation therapy for over 40 years. Deferasirox is a newer chelation therapy that is taken orally once daily. The objective of this study was to estimate the long-term costs and quality-adjusted life-years (QALYs) associated with deferoxamine and deferasirox in a cohort of transfusion-dependent beta-thalassaemia patients from a UK health service perspective.

METHODS

A 50-year annual cycle state transition model comprised three core health states: alive without cardiac complications, alive with cardiac complications, and dead, as well as representing other chronic complications of iron overload: diabetes, hypogonadism, hypoparathyroidism and hypothyroidism. The model was calibrated to identify sets of convergent input parameter values that predicted observed overall survival by mean lifetime compliance with chelation therapy. A pivotal non-inferiority trial informed the main estimates of the effectiveness of deferasirox, which were applied to the calibrated model. Using cost values for the year 2011, costs and utilities were summed over patients' lifetimes to estimate lifetime costs and QALY gains.

RESULTS

Mean lifetime treatment costs for patients receiving deferoxamine were £70,000 higher than deferasirox. Drug acquisition costs were £100,000 higher for deferasirox, but administration costs associated with deferoxamine were £170,000 higher. Higher compliance associated with oral deferasirox administration led to fewer complications. Combined with the quality-of-life effects of an oral mode of administration, an average gain of 4.85 QALYs for deferasirox was estimated. In the base case, deferasirox dominates deferoxamine, i.e., costs less and patients gain more QALYs. The key parameter is the proportion of deferoxamine patients using balloon infusers. Sensitivity analyses showed that even when the proportion of patients using balloon infusers is decreased from 79 to 25 %, the incremental cost per QALY gained remains well under £20,000.

CONCLUSION

Higher drug acquisition costs for deferasirox are offset by the avoidance of infusion-related equipment costs. Combined with health benefits derived from an oral mode of administration and improved compliance, deferasirox has a high probability of being a cost-effective intervention compared with deferoxamine.

摘要

背景与目的

对于β-地中海贫血患者,定期输血会导致体内铁沉积的积累。为了去除这些沉积物,需要进行铁螯合治疗。皮下注射去铁胺已成为 40 多年来的金标准螯合疗法。地拉罗司是一种新型的螯合疗法,每天口服一次。本研究的目的是从英国医疗服务的角度,评估依赖输血的β-地中海贫血患者接受去铁胺和地拉罗司治疗的长期成本和质量调整生命年(QALY)。

方法

一个 50 年的年度循环状态转移模型包括三个核心健康状态:无心脏并发症存活、有心脏并发症存活和死亡,以及代表铁过载的其他慢性并发症:糖尿病、性腺功能减退症、甲状旁腺功能减退症和甲状腺功能减退症。该模型经过校准,以确定一组收敛的输入参数值,这些值通过平均终生螯合治疗依从性来预测观察到的总生存期。一项关键性非劣效性试验为地拉罗司的有效性提供了主要估计值,这些估计值被应用于校准模型。使用 2011 年的成本值,对患者的终生成本和 QALY 收益进行了总结,以估计终生成本和 QALY 收益。

结果

接受去铁胺治疗的患者的平均终生治疗成本比地拉罗司高出 70,000 英镑。地拉罗司的药物购置成本高出 100,000 英镑,但与去铁胺相关的管理成本高出 170,000 英镑。由于口服地拉罗司治疗的依从性较高,并发症较少。结合口服给药方式的生活质量影响,估计地拉罗司的平均 QALY 增益为 4.85。在基础情况下,地拉罗司优于去铁胺,即成本更低,患者获得更多的 QALY。关键参数是使用气球输注器的去铁胺患者的比例。敏感性分析表明,即使将使用气球输注器的患者比例从 79%降至 25%,每增加一个 QALY 的增量成本仍远低于 20,000 英镑。

结论

地拉罗司的药物购置成本较高,但可避免输注相关设备成本。结合口服给药方式带来的健康益处和改善的依从性,与去铁胺相比,地拉罗司极有可能成为一种具有成本效益的干预措施。

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