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依维莫司、镥[177Lu]DOTATATE 和舒尼替尼治疗晚期、不可切除或转移性神经内分泌肿瘤且疾病进展:系统评价和成本效果分析。

Everolimus, lutetium-177 DOTATATE and sunitinib for advanced, unresectable or metastatic neuroendocrine tumours with disease progression: a systematic review and cost-effectiveness analysis.

机构信息

Peninsula Technology Assessment Group (PenTAG), University of Exeter, Exeter, UK.

Plymouth Oncology Centre, Plymouth Hospitals NHS Trust, Plymouth, UK.

出版信息

Health Technol Assess. 2018 Sep;22(49):1-326. doi: 10.3310/hta22490.

DOI:10.3310/hta22490
PMID:30209002
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6151360/
Abstract

BACKGROUND

Neuroendocrine tumours (NETs) are a group of heterogeneous cancers that develop in cells in the diffuse neuroendocrine system.

OBJECTIVES

To estimate the clinical effectiveness of three interventions [everolimus (Afinitor; Novartis International AG, Basel, Switzerland), lutetium-177 DOTATATE (177Lu-DOTATATE) (Lutathera; Imaging Equipment Ltd, Radstock, UK) and sunitinib (Sutent; Pfizer Inc., New York, NY, USA)] for treating unresectable or metastatic NETs with disease progression and establish the cost-effectiveness of these interventions.

DATA SOURCES

The following databases were searched from inception to May 2016: MEDLINE, MEDLINE In-Process & Other Non-Indexed Citations, MEDLINE Daily, Epub Ahead of Print, EMBASE, Cochrane Central Register of Controlled Trials and Web of Science.

REVIEW METHODS

We systematically reviewed the clinical effectiveness and cost-effectiveness literature on everolimus, 177Lu-DOTATATE and sunitinib for treating advanced, unresectable or metastatic progressive NETs. The following NET locations were considered separately: pancreas, gastrointestinal (GI) tract and lung, and GI tract (midgut only). We wrote a survival partition cohort-based economic evaluation in Microsoft Excel 2013 (Microsoft Corporation, Redmond, WA, USA) from the UK NHS and Personal Social Services perspective. This comprised three health states: (1) progression-free survival (PFS), (2) progressed disease and (3) death.

RESULTS

Three randomised controlled trials (RCTs), RADIANT-3 [RAD001 in Advanced Neuroendocrine Tumors, Third Trial; pancreatic NETs (pNETs): everolimus vs. best supportive care (BSC)], A6181111 (pNETs: sunitinib vs. BSC) and RADIANT-4 (RAD001 in Advanced Neuroendocrine Tumors, Fourth Trial; GI and lung NETs: everolimus vs. BSC), met the inclusion criteria for the clinical effectiveness systematic review. The risk of bias was low. Although the NETTER-1 (Neuroendocrine Tumors Therapy) RCT, of 177Lu-DOTATATE plus 30 mg of octreotide (Sandostatin, Novartis) compared with 60 mg of octreotide, was excluded from the review, we nonetheless present the results of this trial, as it informs our estimate of the cost-effectiveness of 177Lu-DOTATATE. The pNETs trials consistently found that the interventions improved PFS and overall survival (OS) compared with BSC. Our indirect comparison found no significant difference in PFS between everolimus and sunitinib. Estimates of OS gain were confounded because of high rates of treatment switching. After adjustment, our indirect comparison suggested a lower, but non-significant, hazard of death for sunitinib compared with everolimus. In GI and lung NETs, everolimus significantly improved PFS compared with BSC and showed a non-significant trend towards improved OS compared with BSC. Adverse events were more commonly reported following treatment with targeted interventions than after treatment with BSC. In the base case for pNETs, assuming list prices, we estimated incremental cost-effectiveness ratios (ICERs) for everolimus compared with BSC of £45,493 per quality-adjusted life-year (QALY) and for sunitinib compared with BSC of £20,717 per QALY. These ICERs increased substantially without the adjustment for treatment switching. For GI and lung NETs, we estimated an ICER for everolimus compared with BSC of £44,557 per QALY. For GI (midgut) NETs, the ICERs were £199,233 per QALY for everolimus compared with BSC and £62,158 per QALY for a scenario analysis comparing 177Lu-DOTATATE with BSC. We judge that no treatment meets the National Institute for Health and Care Excellence's (NICE) end-of-life criteria, although we cannot rule out that sunitinib in the A6181111 trial does.

LIMITATIONS

A RCT with included comparators was not identified for 177Lu-DOTATATE. The indirect treatment comparison that our economic analysis was based on was of a simple Bucher type, unadjusted for any differences in the baseline characteristics across the two trials.

CONCLUSIONS

Given NICE's current stated range of £20,000-30,000 per QALY for the cost-effectiveness threshold, based on list prices, only sunitinib might be considered good value for money in England and Wales.

FUTURE WORK

Further analysis of individual patient data from RADIANT-3 would allow assessment of the robustness of our findings. The data were not made available to us by the company sponsoring the trial.

STUDY REGISTRATION

This study is registered as PROSPERO CRD42016041303.

FUNDING

The National Institute for Health Research Health Technology Assessment programme.

摘要

背景

神经内分泌肿瘤(NETs)是一组异质性癌症,起源于弥散性神经内分泌系统中的细胞。

目的

评估三种干预措施[依维莫司(Afinitor;诺华国际公司,巴塞尔,瑞士)、镥-177 DOTATATE(177Lu-DOTATATE)(Lutathera;Imaging Equipment Ltd,Radstock,英国)和舒尼替尼(Sutent;辉瑞公司,纽约,NY,美国)]治疗不可切除或转移性 NETs 伴疾病进展的临床疗效,并确定这些干预措施的成本效益。

数据来源

从成立到 2016 年 5 月,我们对以下数据库进行了检索:MEDLINE、MEDLINE In-Process & Other Non-Indexed Citations、MEDLINE Daily、Epub Ahead of Print、EMBASE、Cochrane 对照试验中心注册库和 Web of Science。

研究方法

我们系统地回顾了依维莫司、177Lu-DOTATATE 和舒尼替尼治疗晚期、不可切除或转移性进展性 NETs 的临床疗效和成本效益文献。我们分别考虑了以下 NET 位置:胰腺、胃肠道(GI)和肺,以及 GI(仅中肠)。我们使用 Microsoft Excel 2013(Microsoft Corporation,雷德蒙德,WA,美国)从英国国民保健制度和个人社会服务的角度编写了基于生存分区队列的经济评价。该评价包含三个健康状态:(1)无进展生存期(PFS)、(2)进展性疾病和(3)死亡。

结果

有三项随机对照试验(RCTs)符合临床疗效系统评价的纳入标准,分别为 RAD001 在高级神经内分泌肿瘤中的应用研究(RADIANT-3;胰腺 NETs(pNETs):依维莫司对比最佳支持治疗(BSC))、A6181111(pNETs:舒尼替尼对比 BSC)和 RAD001 在高级神经内分泌肿瘤中的应用研究(RADIANT-4;GI 和肺 NETs:依维莫司对比 BSC)。NETTER-1(神经内分泌肿瘤治疗)RCT 被排除在系统评价之外,因为 177Lu-DOTATATE 加 30mg 奥曲肽(善龙,诺华)对比 60mg 奥曲肽的结果没有被纳入,但我们仍然报告了该试验的结果,因为它为我们对 177Lu-DOTATATE 的成本效益估计提供了信息。pNETs 试验一致发现,与 BSC 相比,这些干预措施提高了 PFS 和总生存期(OS)。我们的间接比较发现,依维莫司与舒尼替尼在 PFS 方面没有显著差异。OS 获益的估计受到治疗转换率高的影响。经过调整后,我们的间接比较表明,舒尼替尼与依维莫司相比,死亡的风险较低,但无统计学意义。在 GI 和肺 NETs 中,与 BSC 相比,依维莫司显著改善了 PFS,并且与 BSC 相比,OS 也有改善的趋势,但无统计学意义。与 BSC 相比,靶向治疗的不良反应更为常见。在 pNETs 的基础病例中,假设使用标价,我们估计依维莫司与 BSC 相比的增量成本效益比(ICER)为每质量调整生命年(QALY)45493 英镑,舒尼替尼与 BSC 相比的 ICER 为每 QALY 20717 英镑。如果不调整治疗转换,这些 ICERs 将大幅增加。对于 GI 和肺 NETs,我们估计依维莫司与 BSC 相比的 ICER 为每 QALY 44557 英镑。对于 GI(中肠)NETs,依维莫司与 BSC 相比的 ICER 为 199233 英镑/ QALY,与 177Lu-DOTATATE 与 BSC 相比的情景分析相比,ICER 为 62158 英镑/ QALY。我们判断没有一种治疗方法符合国家卫生与临床优化研究所(NICE)的临终标准,尽管我们不能排除 A6181111 试验中的舒尼替尼符合该标准。

局限性

没有确定针对 177Lu-DOTATATE 的 RCT 作为对照。我们的经济分析所基于的间接治疗比较是一种简单的 Bucher 类型,没有调整两个试验之间的基线特征差异。

结论

考虑到 NICE 目前对成本效益阈值的标价为 20000-30000 英镑/QALY,仅舒尼替尼在英格兰和威尔士可能具有良好的性价比。

未来工作

进一步分析 RADIANT-3 的个体患者数据将有助于评估我们研究结果的稳健性。公司没有向我们提供与这项试验相关的数据。

研究注册

本研究已在 PROSPERO 注册,注册号为 CRD42016041303。

资金

英国国家卫生研究院卫生技术评估计划。