Earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging.

Sullivan, FM; Mair, FS; Anderson, W; Armory, P; Briggs, AORCID logo; Chew, C; Dorward, A; Haughney, JORCID logo; Hogarth, F; Kendrick, D; +19 more...Littleford, R; McConnachie, A; McCowan, C; McMeekin, N; Patel, M; Rauchhaus, P; Ritchie, L; Robertson, C; Robertson, J; Robles-Zurita, J; Sarvesvaran, J; Sewell, H; Sproule, M; Taylor, T; Tello, A; Treweek, S; Vedhara, KORCID logo; Schembri, S; Early Diagnosis of Lung Cancer Scotland (ECLS) Team and (2021) Earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging. European Respiratory Journal, 57 (1). p. 2000670. ISSN 0903-1936 DOI: 10.1183/13993003.00670-2020
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The EarlyCDT-Lung test is a high-specificity blood-based autoantibody biomarker that could contribute to predicting lung cancer risk. We report on the results of a phase IV biomarker evaluation of whether using the EarlyCDT-Lung test and any subsequent computed tomography (CT) scanning to identify those at high risk of lung cancer reduces the incidence of patients with stage III/IV/unspecified lung cancer at diagnosis compared with the standard clinical practice at the time the study began.The Early Diagnosis of Lung Cancer Scotland (ECLS) trial was a randomised controlled trial of 12 208 participants at risk of developing lung cancer in Scotland in the UK. The intervention arm received the EarlyCDT-Lung test and, if test-positive, low-dose CT scanning 6-monthly for up to 2 years. EarlyCDT-Lung test-negative and control arm participants received standard clinical care. Outcomes were assessed at 2 years post-randomisation using validated data on cancer occurrence, cancer staging, mortality and comorbidities.At 2 years, 127 lung cancers were detected in the study population (1.0%). In the intervention arm, 33 out of 56 (58.9%) lung cancers were diagnosed at stage III/IV compared with 52 out of 71 (73.2%) in the control arm. The hazard ratio for stage III/IV presentation was 0.64 (95% CI 0.41-0.99). There were nonsignificant differences in lung cancer and all-cause mortality after 2 years.ECLS compared EarlyCDT-Lung plus CT screening to standard clinical care (symptomatic presentation) and was not designed to assess the incremental contribution of the EarlyCDT-Lung test. The observation of a stage shift towards earlier-stage lung cancer diagnosis merits further investigations to evaluate whether the EarlyCDT-Lung test adds anything to the emerging standard of low-dose CT.


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