Health Services and Systems Research, Duke-NUS Medical School, 8 College Road, Singapore, 169857, Singapore.
Division of Medical Oncology, National Cancer Centre Singapore, Singapore, 168583, Singapore.
Lung Cancer. 2024 May;191:107794. doi: 10.1016/j.lungcan.2024.107794. Epub 2024 Apr 15.
Liquid biopsy is complementary to tissue biopsy for lung cancer profiling, yet evidence of the cost-effectiveness is limited. This could retard implementation and reimbursement in clinical practice. The aim of this study is to estimate the cost-effectiveness of profiling strategies that include liquid biopsy and to identify the optimal profiling approach for newly diagnosed advanced non-squamous non-small cell lung cancer (NSCLC) in an Asian population using Singapore as an example.
A decision tree and partitioned-survival model was developed from the Singapore healthcare system's perspective to evaluate the cost-effectiveness of five molecular profiling strategies: either tissue or plasma next-generation sequencing (NGS) alone, a concurrent, and two sequential approaches. Model inputs were informed by local data or published literature. Sensitivity analyses and scenario analyses were undertaken to understand the robustness of the conclusions for decision making. The optimal strategy at different willingness-to-pay (WTP) thresholds was presented by cost-effectiveness acceptability frontier and the expected loss curve.
The sequential tissue-plasma NGS approach revealed an additional 0.0981 quality adjusted life years (QALYs) for an extra cost of S$3,074 over a 20-year time horizon compared to tissue NGS alone, resulting in an incremental cost-effectiveness ratio (ICER) of S$31,318/QALY and an incremental net monetary benefit of S$1,343 per patient. The findings were sensitive to the costs of pembrolizumab and osimertinib and the probabilities of re-biopsy after tissue NGS. Sequential plasma-tissue NGS and plasma NGS alone were more costly and less effective than alternatives.
The sequential tissue-plasma NGS approach generated the highest net monetary benefit and was the optimal testing strategy when WTP was S$45,000/QALY. It retained superiority but understandably with a higher ICER when expensive, non-first line treatments were included. Overall, its routine clinical practice should be proactively considered for newly diagnosed advanced non-squamous NSCLC in an Asian population.
液体活检是肺癌分析的组织活检的补充,但成本效益的证据有限。这可能会阻碍其在临床实践中的实施和报销。本研究旨在估计包括液体活检的分析策略的成本效益,并使用新加坡作为范例,为新诊断的晚期非鳞状非小细胞肺癌(NSCLC)患者确定最佳的分析方法。
从新加坡医疗保健系统的角度出发,使用决策树和分区生存模型来评估五种分子分析策略的成本效益:单独进行组织或液体下一代测序(NGS)、同时进行、两种顺序进行。模型输入信息来自当地数据或已发表的文献。进行了敏感性分析和情景分析,以了解结论对于决策的稳健性。在不同的意愿支付(WTP)阈值下,通过成本效益接受性边界和预期损失曲线呈现出最佳策略。
与单独进行组织 NGS 相比,顺序组织-液体 NGS 方法在 20 年的时间范围内额外增加了 0.0981 个质量调整生命年(QALYs),额外花费 3074 新元,增量成本效益比(ICER)为 31318 新元/QALY,每位患者的增量净货币收益为 1343 新元。研究结果对 pembrolizumab 和 osimertinib 的成本以及组织 NGS 后再次活检的概率敏感。顺序液体-组织 NGS 和液体 NGS 单独进行比替代方法更昂贵且效果更差。
顺序组织-液体 NGS 方法产生了最高的净货币收益,当 WTP 为 45000 新元/QALY 时,是最佳的测试策略。当纳入昂贵的非一线治疗药物时,它保留了优势,但相应的 ICER 更高。总体而言,在亚洲人群中,对于新诊断的晚期非鳞状 NSCLC,应积极考虑其常规临床实践。
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