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在等待索拉非尼安全性数据的同时,对肝癌患者在肝移植前使用索拉非尼的成本效益分析。

Use of sorafenib in patients with hepatocellular carcinoma before liver transplantation: a cost-benefit analysis while awaiting data on sorafenib safety.

机构信息

Unità di Chirurgia Oncologica, Istituto Oncologico Veneto, IRCCS, Padova, Italy.

出版信息

Hepatology. 2010 Jan;51(1):165-73. doi: 10.1002/hep.23260.

Abstract

UNLABELLED

The role of bridging therapies for patients with hepatocellular carcinoma (HCC) on the waiting list for liver transplantation (LT) remains controversial. There is strong evidence to support the effectiveness of sorafenib in extending the time to progression of HCC. Using a Markov model, we compared two strategies: one using sorafenib as neoadjuvant therapy before LT (Strategy A), and the other using no bridging therapy in the first 6 months (Strategy B). Reference case: T2 HCC patient with compensated cirrhosis. The benefit of sorafenib in delaying time to HCC progression was expressed as the hazard ratio (HR) and taken from recently published randomized trials. The endpoints considered were: survival benefit measured in quality-adjusted life days (QALDs), transplant probability, costs (C) in euro, willingness to pay (WTP), and net health benefit (NHB), where NHB = survival benefit - C/WTP. The calculated WTP of sorafenib in Italy was 346 euro per QALD. Probabilistic sensitivity analysis showed a median survival benefit of 94 QALDs (10% percentile = 38, 90% percentile = 210). In the base-case scenario (HR = 0.47, monthly dropout probability = 5%, median time to LT = 3 months), the gain in LT probability due to sorafenib was 5% and it increased proportionally with increasing median times to LT and decreasing HR. In the cost-benefit analysis, the incremental NHB of Strategy A versus Strategy B was 37 QALDs; it increased as sorafenib HR decreased and when median times to LT were shorter than 6 months, whereas for longer times it gradually dropped, particularly when Strategy B included effective locoregional treatments.

CONCLUSION

Sorafenib neoadjuvant therapy is cost-effective by comparison with no therapy for T2-HCC patients waiting for LT, particularly for median times to LT under 6 months.

摘要

背景

肝癌(HCC)患者在等待肝移植(LT)时使用桥接治疗的作用仍存在争议。有强有力的证据支持索拉非尼在延长 HCC 进展时间方面的有效性。本研究采用马尔可夫模型比较了两种策略:一种是在 LT 前使用索拉非尼作为新辅助治疗(策略 A),另一种是在前 6 个月不使用桥接治疗(策略 B)。参考病例:代偿性肝硬化 T2 HCC 患者。最近发表的随机试验中的风险比(HR)用于表示索拉非尼在延迟 HCC 进展时间方面的获益。考虑的终点包括:以质量调整生命天数(QALDs)衡量的生存获益、移植概率、欧元成本(C)、意愿支付(WTP)和净健康收益(NHB),其中 NHB = 生存获益-C/WTP。在意大利,索拉非尼的计算 WTP 为 346 欧元/QALD。概率敏感性分析显示,中位生存获益为 94 QALDs(10%分位数=38,90%分位数=210)。在基准案例中(HR=0.47,每月失访概率=5%,LT 中位时间=3 个月),索拉非尼使 LT 概率增加了 5%,并且随着 LT 中位时间的增加和 HR 的降低而成比例增加。在成本效益分析中,策略 A 与策略 B 相比,NHB 的增量为 37 QALDs;当索拉非尼 HR 降低且 LT 中位时间短于 6 个月时,它会增加,而当 LT 中位时间较长时,它会逐渐下降,尤其是当策略 B 包含有效的局部区域治疗时。

结论

对于等待 LT 的 T2-HCC 患者,与不进行治疗相比,索拉非尼新辅助治疗具有成本效益,尤其是当 LT 中位时间小于 6 个月时。

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