博赛泼维治疗初治慢性丙型肝炎 1 型感染患者的成本效果建模研究:基于美国的研究。
Boceprevir for previously untreated patients with chronic hepatitis C Genotype 1 infection: a US-based cost-effectiveness modeling study.
出版信息
BMC Infect Dis. 2013 Apr 27;13:190. doi: 10.1186/1471-2334-13-190.
BACKGROUND
SPRINT-2 demonstrated that boceprevir (BOC), an oral hepatitis C virus (HCV) nonstructural 3 (NS3) protease inhibitor, added to peginterferon alfa-2b (P) and ribavirin (R) significantly increased sustained virologic response rates over PR alone in previously untreated adult patients with chronic HCV genotype 1. We estimated the long-term impact of triple therapy vs. dual therapy on the clinical burden of HCV and performed a cost-effectiveness evaluation.
METHODS
A Markov model was used to estimate the incidence of liver complications, discounted costs (2010 US$), quality-adjusted life years (QALYs), and incremental cost-effectiveness ratios (ICERs) of three treatment strategies for treatment-naïve patients with chronic HCV genotype 1. The model simulates the treatment regimens studied in SPRINT-2 in which PR was administered for 4 weeks followed by: 1) placebo plus PR for 44 weeks (PR48); 2) BOC plus PR using response guided therapy (BOC/RGT); and 3) BOC plus PR for 44 weeks (BOC/PR48) and makes projections within and beyond the trial. HCV-related state-transition probabilities, costs, and utilities were obtained from previously published studies. All costs and QALYs were discounted at 3%.
RESULTS
The model projected approximately 38% and 43% relative reductions in the lifetime incidence of liver complications in the BOC/RGT and BOC/PR48 regimens compared with PR48, respectively. Treatment with BOC/RGT is associated with an incremental cost of $10,348 and an increase of 0.62 QALYs compared to treatment with PR48. Treatment with BOC/PR48 is associated with an incremental cost of $35,727 and an increase of 0.65 QALYs compared to treatment with PR48. The ICERs were $16,792/QALY and $55,162/QALY for the boceprevir-based treatment groups compared with PR48, respectively. The ICER for BOC/PR48 compared with BOC/RGT was $807,804.
CONCLUSION
The boceprevir-based regimens used in the SPRINT-2 trial were projected to substantially reduce the lifetime incidence of liver complications and increase the QALYs in treatment-naive patients with hepatitis C genotype 1. It was also demonstrated that boceprevir-based regimens offer patients the possibility of experiencing great clinical benefit with a shorter duration of therapy. Both boceprevir-based treatment strategies were projected to be cost-effective at a reasonable threshold in the US when compared to treatment with PR48.
背景
SPRINT-2 研究表明,在未经治疗的慢性丙型肝炎基因型 1 成年患者中,与聚乙二醇干扰素 alfa-2b(P)和利巴韦林(R)联合应用,口服丙型肝炎病毒(HCV)非结构 3(NS3)蛋白酶抑制剂 boceprevir(BOC)可显著提高持续病毒学应答率,优于 PR 单药治疗。我们估计三联治疗与双联治疗对 HCV 临床负担的长期影响,并进行了成本效益评估。
方法
采用 Markov 模型估计三种治疗方案(初治慢性丙型肝炎基因型 1 患者)对 HCV 相关并发症的发生率、贴现成本(2010 年美国美元)、质量调整生命年(QALY)和增量成本效益比(ICER)。该模型模拟了 SPRINT-2 研究中的治疗方案,其中 PR 治疗 4 周后,分别采用以下方案:1)安慰剂联合 PR 治疗 44 周(PR48);2)根据应答指导的 BOC 联合 PR 治疗(BOC/RGT);3)BOC 联合 PR 治疗 44 周(BOC/PR48),并在试验内和试验外进行预测。HCV 相关状态转移概率、成本和效用来自先前发表的研究。所有成本和 QALY 均贴现 3%。
结果
模型预测,与 PR48 相比,BOC/RGT 和 BOC/PR48 方案可使终生 HCV 相关并发症发生率分别降低约 38%和 43%。与 PR48 相比,BOC/RGT 治疗的增量成本为 10348 美元,QALY 增加 0.62。与 PR48 相比,BOC/PR48 治疗的增量成本为 35727 美元,QALY 增加 0.65。与 PR48 相比,基于 BOC 的治疗组的 ICER 分别为 16792 美元/QALY 和 55162 美元/QALY。BOC/PR48 与 BOC/RGT 相比的 ICER 为 807804 美元。
结论
SPRINT-2 试验中的 BOC 治疗方案预计可显著降低初治慢性丙型肝炎基因型 1 患者的终生 HCV 相关并发症发生率,并提高 QALY。此外,该方案还表明,与 PR48 相比,基于 BOC 的治疗方案可在较短的治疗时间内为患者提供获得更大临床获益的可能性。在考虑了美国合理的阈值后,两种基于 BOC 的治疗策略都被认为是具有成本效益的。
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