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

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 t...

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Autores principales: Sullivan, Frank M., Mair, Frances S., Anderson, William, Armory, Pauline, Briggs, Andrew, Chew, Cindy, Dorward, Alistair, Haughney, John, Hogarth, Fiona, Kendrick, Denise, Littleford, Roberta, McConnachie, Alex, McCowan, Colin, McMeekin, Nicola, Patel, Manish, Rauchhaus, Petra, Ritchie, Lewis, Robertson, Chris, Robertson, John, Robles-Zurita, Jose, Sarvesvaran, Joseph, Sewell, Herbert, Sproule, Michael, Taylor, Thomas, Tello, Agnes, Treweek, Shaun, Vedhara, Kavita, Schembri, Stuart
Formato: Online Artículo Texto
Lenguaje:English
Publicado: European Respiratory Society 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7806972/
https://www.ncbi.nlm.nih.gov/pubmed/32732334
http://dx.doi.org/10.1183/13993003.00670-2020
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author Sullivan, Frank M.
Mair, Frances S.
Anderson, William
Armory, Pauline
Briggs, Andrew
Chew, Cindy
Dorward, Alistair
Haughney, John
Hogarth, Fiona
Kendrick, Denise
Littleford, Roberta
McConnachie, Alex
McCowan, Colin
McMeekin, Nicola
Patel, Manish
Rauchhaus, Petra
Ritchie, Lewis
Robertson, Chris
Robertson, John
Robles-Zurita, Jose
Sarvesvaran, Joseph
Sewell, Herbert
Sproule, Michael
Taylor, Thomas
Tello, Agnes
Treweek, Shaun
Vedhara, Kavita
Schembri, Stuart
author_facet Sullivan, Frank M.
Mair, Frances S.
Anderson, William
Armory, Pauline
Briggs, Andrew
Chew, Cindy
Dorward, Alistair
Haughney, John
Hogarth, Fiona
Kendrick, Denise
Littleford, Roberta
McConnachie, Alex
McCowan, Colin
McMeekin, Nicola
Patel, Manish
Rauchhaus, Petra
Ritchie, Lewis
Robertson, Chris
Robertson, John
Robles-Zurita, Jose
Sarvesvaran, Joseph
Sewell, Herbert
Sproule, Michael
Taylor, Thomas
Tello, Agnes
Treweek, Shaun
Vedhara, Kavita
Schembri, Stuart
author_sort Sullivan, Frank M.
collection PubMed
description 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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spelling pubmed-78069722021-01-21 Earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging Sullivan, Frank M. Mair, Frances S. Anderson, William Armory, Pauline Briggs, Andrew Chew, Cindy Dorward, Alistair Haughney, John Hogarth, Fiona Kendrick, Denise Littleford, Roberta McConnachie, Alex McCowan, Colin McMeekin, Nicola Patel, Manish Rauchhaus, Petra Ritchie, Lewis Robertson, Chris Robertson, John Robles-Zurita, Jose Sarvesvaran, Joseph Sewell, Herbert Sproule, Michael Taylor, Thomas Tello, Agnes Treweek, Shaun Vedhara, Kavita Schembri, Stuart Eur Respir J Original Articles 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. European Respiratory Society 2021-01-14 /pmc/articles/PMC7806972/ /pubmed/32732334 http://dx.doi.org/10.1183/13993003.00670-2020 Text en Copyright ©ERS 2021 http://creativecommons.org/licenses/by/4.0/This version is distributed under the terms of the Creative Commons Attribution Non-Commercial Licence 4.0.
spellingShingle Original Articles
Sullivan, Frank M.
Mair, Frances S.
Anderson, William
Armory, Pauline
Briggs, Andrew
Chew, Cindy
Dorward, Alistair
Haughney, John
Hogarth, Fiona
Kendrick, Denise
Littleford, Roberta
McConnachie, Alex
McCowan, Colin
McMeekin, Nicola
Patel, Manish
Rauchhaus, Petra
Ritchie, Lewis
Robertson, Chris
Robertson, John
Robles-Zurita, Jose
Sarvesvaran, Joseph
Sewell, Herbert
Sproule, Michael
Taylor, Thomas
Tello, Agnes
Treweek, Shaun
Vedhara, Kavita
Schembri, Stuart
Earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging
title Earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging
title_full Earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging
title_fullStr Earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging
title_full_unstemmed Earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging
title_short Earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging
title_sort earlier diagnosis of lung cancer in a randomised trial of an autoantibody blood test followed by imaging
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7806972/
https://www.ncbi.nlm.nih.gov/pubmed/32732334
http://dx.doi.org/10.1183/13993003.00670-2020
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