Performance of volume and diameter thresholds in malignancy prediction of solid nodules in lung cancer screening

Andrew W Creamer; Carolyn Horst; Ruth Prendecki; Priyam Verghese; Amyn Bhamani; Helen Hall; Sophie Tisi; Jennifer L Dickson; Chuen R Khaw; John McCabe; Tanita Limani; Kylie Gyertson; Anne-Marie Hacker; Jonathan Teague; Laura Farrelly; Shrinkhala Dawadi; Neal Navani; Allan Hackshaw; Anand Devaraj; Arjun Nair; SUMMIT Consortium; Sam M Janes

doi:10.1136/thorax-2024-222086

Performance of volume and diameter thresholds in malignancy prediction of solid nodules in lung cancer screening

Thorax. 2025 Jun 2:thorax-2024-222086. doi: 10.1136/thorax-2024-222086. Online ahead of print.

Authors

Andrew W Creamer¹, Carolyn Horst¹, Ruth Prendecki¹, Priyam Verghese¹, Amyn Bhamani¹, Helen Hall¹, Sophie Tisi¹, Jennifer L Dickson¹, Chuen R Khaw¹, John McCabe¹, Tanita Limani², Kylie Gyertson², Anne-Marie Hacker³, Jonathan Teague³, Laura Farrelly³, Shrinkhala Dawadi³, Neal Navani², Allan Hackshaw³, Anand Devaraj^{4

5}, Arjun Nair²; SUMMIT Consortium; Sam M Janes⁶

Collaborators

SUMMIT Consortium:
Sam M Janes, Jennifer L Dickson, Carolyn Horst, Sophie Tisi, Helen Hall, Priyam Verghese, Andrew Creamer, Thomas Callender, Ruth Prendecki, Amyn Bhamani, Chuen Ryan Khaw, Mamta Ruparel, Allan Hackshaw, Laura Farrelly, Jon Teague, Anne-Marie Mullin, Kitty Chan, Rachael Sarpong, Malavika Suresh, Samantha L Quaife, Arjun Nair, Anand Devaraj, Kylie Gyertson, Vicky Bowyer, Ethaar El-Emir, Judy Airebamen, Alice Cotton, Kaylene Phua, Elodie Murali, Simranjit Mehta, Janine Zylstra, Karen Parry-Billings, Columbus Ife, April Neville, Paul Robinson, Laura Green, Zahra Hanif, Helen Kiconco, Ricardo McEwen, Dominique Arancon, Nicholas Beech, Derya Ovayolu, Christine Hosein, Sylvia Patricia Enes, Qin April Neville, Jane Rowlands, Aashna Samson, Urja Patel, Fahmida Hoque, Hina Pervez, Sofia Nnorom, Moksud Miah, Julian McKee, Mark Clark, Jeannie Eng, Fanta Bojang, Claire Levermore, Anant Patel, Sara Lock, Rajesh Banka, Angshu Bhowmik, Ugo Ekeowa, Zaheer Mangera, William M Ricketts, Neal Navani, Terry O'Shaughnessy, Charlotte Cash, Magali Taylor, Samanjit Hare, Tunku Aziz, Stephen Ellis, Anthony Edey, Graham Robinson, Alberto Villanueva, Hasti Robbie, Elena Stefan, Charlie Sayer, Nick Screaton, Navinah Nundlall, Lyndsey Gallagher, Andrew Crossingham, Thea Buchan, Tanita Limani, Kate Gowers, Kate Davies, John McCabe, Joseph Jacob, Karen Sennett, Tania Anastasiadis, Andrew Perugia, James Rusius

Affiliations

¹ Lungs for Living Research Centre, UCL Respiratory, University College London, London, UK.
² University College London Hospitals NHS Foundation Trust, London, UK.
³ Cancer Research UK and UCL Cancer Trials Centre, University College London, London, UK.
⁴ Royal Brompton Hospital, London, UK.
⁵ National Heart and Lung Institute, Imperial College, London, UK.
⁶ Lungs for Living Research Centre, UCL Respiratory, University College London, London, UK s.janes@ucl.ac.uk.

PMID: 40456600
DOI: 10.1136/thorax-2024-222086

Abstract

Background: Prospective validation and comparison of the performance of nodule management protocols is limited. The aim of this study was to examine the performance of size and risk thresholds for assessing malignancy in solid nodules at baseline low-dose CT (LDCT) in a lung cancer screening (LCS) programme.

Methods: This was an observational study using data from the SUMMIT Study, a prospective longitudinal study investigating LDCT for LCS. Participants were 55-77 years old and met either the United States Preventative Services Task Force (2013) criteria or had a PLCO_m2012 risk of ≥1.3%. LDCTs were reported using computer-aided detection software (Veolity, MeVIS) with semiautomated volumetry. Cancer outcomes were reported for solid nodules reported at baseline CT, with participants represented by the single largest solid nodule where more than one was present. Malignancy risk was stratified by long-axis diameter and volume using predefined size thresholds taken from British Thoracic Society and European Position statement guidelines: a 5/6 mm long axis diameter or 80/100 mm³ volume 'rule out' thresholds for low-risk nodules and ≥300 mm³ or ≥8 mm diameter with or without Brock score ≥10% 'Rule in' thresholds for high-risk nodules.Pearson's χ² test was used to calculate statistical significance for nominal variables, McNemar's test for comparison of sensitivity/specificity and DeLong' test for comparison of areas under the receiver operating characteristic curve (AUROC). Optimal thresholds were determined with Youden's J statistic. Net benefit calculations were undertaken to compare the existing thresholds with 95% CIs calculated by bootstrap sampling.

Results: 11 355 participants were included. Crude risk of malignancy in solid nodules at baseline LDCT was 3.8% (228/5929). Risk of malignancy in solid nodules <6 mm long-axis diameter or <100 mm³ volume was equivalent to that in participants with no nodules at baseline LDCT (0.88% and 0.84% vs 0.77%, p=0.4600 and p=0.7932, respectively). A <80 mm³ volume and <5 mm diameter 'rule out' threshold achieved sensitivity 86.8% and 93.4%, specificity 65.4% and 24.64%, and negative predictive value (NPV) 99.2% and 98.9%, respectively. The <80 mm³ volume threshold encompassed 63.3% of participants with a baseline solid nodule compared with 24.0% by the <5 mm diameter threshold.For nodules ≥8 mm diameter, the addition of a risk score (Brock ≥10%) was associated with a significant net benefit when compared with using size threshold alone by net effect analysis (31.24; 95% CI 26.19 to 35.89).

Conclusions: Solid nodules <100 mm³ or <6 mm diameter are not associated with increased risk of lung cancer compared with participants with no nodules at baseline LDCT. Volumetric rule-out thresholds achieve equivalent NPV to long-axis diameter thresholds while encompassing significantly more participants, reducing the number of interval scans required.

Keywords: Imaging/CT MRI etc; Lung Cancer.