Comparison of Tissue-Based Molecular Markers in Younger versus Older Patients with Colorectal Neoplasia
Emerging colorectal cancer trends demonstrate increased incidence and mortality in younger populations, prompting consideration of average-risk colorectal cancer screening initiation at age 45 versus 50 years. However, screening test performance characteristics in adults 45-49 years have been minima...
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Veröffentlicht in: | Cancer epidemiology, biomarkers & prevention biomarkers & prevention, 2020-08, Vol.29 (8), p.1570-1576 |
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Zusammenfassung: | Emerging colorectal cancer trends demonstrate increased incidence and mortality in younger populations, prompting consideration of average-risk colorectal cancer screening initiation at age 45 versus 50 years. However, screening test performance characteristics in adults 45-49 years have been minimally described. To inform the biologic rationale for multi-target stool DNA (mt-sDNA) screening in younger patients, we analyzed and compared tissue levels of methylation (
) and mutation (
) markers included in the FDA-approved, mt-sDNA assay (Cologuard; Exact Sciences Corporation).
Within 40-44, 45-49, and 50-64 year age groups, archived colorectal tissue specimens were identified for 211 sporadic colorectal cancer cases, 123 advanced precancerous lesions (APLs; adenomas >1 cm, high-grade dysplasia, ≥25% villous morphology, or sessile serrated polyp; 45-49 and 50-64 age groups only), and 204 histologically normal controls. Following DNA extraction,
, and
were quantified using QuARTS assays, relative to
(reference gene).
None of the molecular marker concentrations were significantly associated with age (
> 0.05 for all comparisons), with the exception of
concentration in APL samples (higher in older vs. younger cases;
= 0.008). However,
levels were also statistically higher in APL case versus normal control samples in both the 45-49 (
< 0.0001) and 50-64 (
< 0.0001) year age groups.
Overall, these findings support the potential for earlier onset of average-risk colorectal cancer screening with the mt-sDNA assay.
These novel data address an identified knowledge gap and strengthen the biologic basis for earlier-onset, average-risk screening with the mt-sDNA assay. |
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ISSN: | 1055-9965 1538-7755 |
DOI: | 10.1158/1055-9965.EPI-19-1598 |