Impact of screening and follow‐up colonoscopy adenoma sensitivity on colorectal cancer screening outcomes in the CRC‐AIM microsimulation model

Deborah A. Fisher; Leila Saoud; Kristen Hassmiller Lich; A. Mark Fendrick; A. Burak Ozbay; Bijan J. Borah; Michael Matney; Marcus Parton; Paul J. Limburg

doi:10.1002/cam4.3662

Cancer Medicine (Apr 2021)

Impact of screening and follow‐up colonoscopy adenoma sensitivity on colorectal cancer screening outcomes in the CRC‐AIM microsimulation model

Deborah A. Fisher,
Leila Saoud,
Kristen Hassmiller Lich,
A. Mark Fendrick,
A. Burak Ozbay,
Bijan J. Borah,
Michael Matney,
Marcus Parton,
Paul J. Limburg

Affiliations

Deborah A. Fisher: Department of Medicine Division of Gastroenterology Duke University Durham NC USA
Leila Saoud: Exact Sciences Corporation Madison WI USA
Kristen Hassmiller Lich: Department of Health Policy & Management Gillings School of Global Public Health University of North Carolina at Chapel Hill Chapel Hill NC USA
A. Mark Fendrick: Division of Gastroenterology University of Michigan Ann Arbor MI USA
A. Burak Ozbay: Exact Sciences Corporation Madison WI USA
Bijan J. Borah: Department of Health Services Research Mayo Clinic Rochester MN USA
Michael Matney: Exact Sciences Corporation Madison WI USA
Marcus Parton: Exact Sciences Corporation Madison WI USA
Paul J. Limburg: Division of Gastroenterology and Hepatology Mayo Clinic Rochester MN USA

DOI: https://doi.org/10.1002/cam4.3662
Journal volume & issue: Vol. 10, no. 8
pp. 2855 – 2864

Abstract

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Abstract Background Real‐world data for patients with positive colorectal cancer (CRC) screening stool‐tests demonstrate that adenoma detection rates are lower when endoscopists are blinded to the stool‐test results. This suggests adenoma sensitivity may be lower for screening colonoscopy than for follow‐up to a known positive stool‐based test. Previous CRC microsimulation models assume identical sensitivities between screening and follow‐up colonoscopies after positive stool‐tests. The Colorectal Cancer and Adenoma Incidence and Mortality Microsimulation Model (CRC‐AIM) was used to explore the impact on screening outcomes when assuming different adenoma sensitivity between screening and combined follow‐up/surveillance colonoscopies. Methods Modeled screening strategies included colonoscopy every 10 years, triennial multitarget stool DNA (mt‐sDNA), or annual fecal immunochemical test (FIT) from 50 to 75 years. Outcomes were reported per 1000 individuals without diagnosed CRC at age 40. Base‐case adenoma sensitivity values were identical for screening and follow‐up/surveillance colonoscopies. Ranges of adenoma sensitivity values for colonoscopy performance were developed using different slopes of odds ratio adjustments and were designated as small, medium, or large impact scenarios. Results As the differences in adenoma sensitivity for screening versus follow‐up/surveillance colonoscopies became greater, life‐years gained (LYG) and reductions in CRC‐related incidence and mortality versus no screening increased for mt‐sDNA and FIT and decreased for screening colonoscopy. The LYG relative to screening colonoscopy reached >90% with FIT in the base‐case scenario and with mt‐sDNA in a “medium impact” scenario. Conclusions Assuming identical adenoma sensitivities for screening and follow‐up/surveillance colonoscopies underestimate the potential benefits of stool‐based screening strategies.

Published in Cancer Medicine

ISSN: 2045-7634 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://onlinelibrary.wiley.com/journal/20457634

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