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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Multimodal lung cancer screening using the ITALUNG biomarker panel and low dose computed tomography. Results of the ITALUNG biomarker study
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Multimodal lung cancer screening using the ITALUNG biomarker panel and low dose computed tomography. Results of the ITALUNG biomarker study

机译:使用Italung Biomarker面板和低剂量计算断层扫描的多式肺癌筛选。 Italung Biomarker研究的结果

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Asymptomatic high-risk subjects, randomized in the intervention arm of the ITALUNG trial (1,406 screened for lung cancer), were enrolled for the ITALUNG biomarker study (n = 1,356), in which samples of blood and sputum were analyzed for plasma DNA quantification (cut off 5 ng/ml), loss of heterozygosity and microsatellite instability. The ITALUNG biomarker panel (IBP) was considered positive if at least one of the two biomarkers included in the panel was positive. Subjects with and without lung cancer diagnosis at the end of the screening cycle with LDCT (n = 517) were evaluated. Out of 18 baseline screen detected lung cancer cases, 17 were IBP positive (94%). Repeat screen-detected lung cancer cases were 18 and 12 of them positive at baseline IBP test (66%). Interval cancer cases (2-years) and biomarker tests after a suspect Non Calcific Nodule follow-up were investigated. The single test versus multimodal screening measures of accuracy were compared in a simulation within the screened ITALUNG intervention arm, considering screen-detected and interval cancer cases. Sensitivity was 90% at baseline screening. Specificity was 71 and 61% for LDCT and IBP as baseline single test, and improved at 89% with multimodal, combined screening. The positive predictive value was 4.3% for LDCT at baseline and 10.6% for multimodal screening. Multimodal screening could improve the screening efficiency at baseline and strategies for future implementation are discussed. If IBP was used as primary screening test, the LDCT burden might decrease of about 60%.
机译:在Italung试验的干预臂(肺癌的1,406筛选的1,406筛选)中随机进行了无症状的高风险主体,用于伊朗普生物标志物研究(n = 1,356),其中分析了血浆和痰液的样品进行血浆DNA定量(切断5 ng / ml),损失杂合性和微卫星不稳定性。如果小组中包含的两个生物标志物中的至少一种是阳性的,则ITALUNG Biomarker面板(IBP)被认为是阳性的。评价筛选循环结束时的受试者和没有肺癌诊断,评价LDCT(n = 517)。在18个基线筛选中检测到肺癌病例,17例为IBP阳性(94%)。重复筛选肺癌病例为18和12,在基线IBP测试(66%)。嫌疑人无钙结构随访后,间隔癌病例(2年)和生物标志物试验。在筛选的Italung干预臂内的模拟中,考虑筛选和间隔癌症病例,将单一测试与多峰筛选准确度进行比较。基线筛选敏感度为90%。 LDCT和IBP为基线单次测试的特异性为71%和61%,并在89%的情况下提高了多式联运,组合筛选。基线LDCT的阳性预测值为4.3%,多式联筛选的10.6%。多模式筛查可以提高基线的筛选效率,并讨论了未来实施的策略。如果IBP被用作主要筛查测试,则LDCT负担可能降低约60%。

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