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NELSON筛查方案检测肺癌的分期和组织学特异性敏感性——一项建模研究

Stage- and histology-specific sensitivity for the detection of lung cancer of the NELSON screening protocol-A modeling study.

作者信息

de Nijs Koen, Ten Haaf Kevin, Hubert Juul, Moldovanu Dana, van der Aalst Carlijn M, Groen Harry J M, de Jong Pim A, Heuvelmans Marjolein A, Oudkerk Matthijs, de Koning Harry J

机构信息

Department of Public Health, Erasmus MC-University Medical Center Rotterdam, Rotterdam, The Netherlands.

Faculty of Medical Sciences, University of Groningen, Groningen, The Netherlands.

出版信息

Int J Cancer. 2025 Jul 11. doi: 10.1002/ijc.70045.

Abstract

The Dutch-Belgian lung cancer (LC) screening trial (Nederlands-Leuvens Longkanker Screenings Onderzoek [NELSON]) demonstrated low-dose computed tomography (CT) reduces LC mortality by 24% among men. The NELSON protocol differed from previous trials in the eligibility criteria, the use of volume-based nodule management, and increasing screening intervals. The early-stage sensitivity of the protocol is pivotal in determining the optimal screening strategy, such as the interval and age range. The MIcrosimulation SCreening ANalysis-Lung natural history model was used to reproduce LC incidence and mortality by detection method (clinical or screen-detected), sex, histology, and stage in the NELSON trial based on individual-level data. We evaluated screening effectiveness by stage and histology, accounting for population characteristics, trial design, and LC epidemiology. We find stage IA non-small cell LC (NSCLC) sensitivity of 24.6% (other NSCLC) to 41.0% (adenocarcinoma) at baseline screening. At repeat screening rounds, we find this increased to 70.9% for stage IA adenocarcinoma. For stage IB, the sensitivity by histology ranges from 26.4% to 77.1%; for stage II, 39.6%-81.9%. Upon detection, the probability of LC mortality prevention is estimated at 83% for stage IA. The sensitivity for detecting early-stage LC is found to depend on the histology of cancer and is increased for adenocarcinoma at repeat screenings. Despite a low rate of referral to follow-up screening in the NELSON trial, early-stage CT sensitivity and the probability of mortality prevention were similar to previous estimates from the National Lung cancer Screening Trial. Previously demonstrated screening effectiveness may be maintained when implementing new programs, while reducing unnecessary follow-up when considering NELSON evidence.

摘要

荷兰-比利时肺癌(LC)筛查试验(荷兰鲁汶肺癌筛查研究[NELSON])表明,低剂量计算机断层扫描(CT)可使男性LC死亡率降低24%。NELSON方案在纳入标准、基于体积的结节管理方法以及增加筛查间隔方面与以往试验不同。该方案的早期敏感性对于确定最佳筛查策略(如筛查间隔和年龄范围)至关重要。基于个体水平数据,使用微模拟筛查分析-肺癌自然史模型来重现NELSON试验中按检测方法(临床检测或筛查发现)、性别、组织学和分期划分的LC发病率和死亡率。我们根据人群特征、试验设计和LC流行病学情况,按分期和组织学评估了筛查效果。我们发现,在基线筛查时,IA期非小细胞肺癌(NSCLC)的敏感性为24.6%(其他NSCLC)至41.0%(腺癌)。在重复筛查轮次中,我们发现IA期腺癌的敏感性增至70.9%。对于IB期,按组织学划分的敏感性范围为26.4%至77.1%;对于II期,为39.6%至81.9%。一经检测,IA期LC死亡预防概率估计为83%。发现早期LC的检测敏感性取决于癌症的组织学类型,且在重复筛查时腺癌的敏感性会增加。尽管NELSON试验中后续筛查的转诊率较低,但早期CT敏感性和死亡预防概率与国家肺癌筛查试验先前的估计值相似。在实施新方案时,先前已证明的筛查效果可能得以维持,同时在考虑NELSON研究证据时可减少不必要的后续检查。

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