Cancers (Dec 2022)

Integrative Clinical and DNA Methylation Analyses in a Population-Based Cohort Identifies <i>CDH17</i> and <i>LRP2</i> as Risk Recurrence Factors in Stage II Colon Cancer

  • Benjamin Tournier,
  • Romain Aucagne,
  • Caroline Truntzer,
  • Cyril Fournier,
  • François Ghiringhelli,
  • Caroline Chapusot,
  • Laurent Martin,
  • Anne Marie Bouvier,
  • Sylvain Manfredi,
  • Valérie Jooste,
  • Mary B. Callanan,
  • Côme Lepage

DOI
https://doi.org/10.3390/cancers15010158
Journal volume & issue
Vol. 15, no. 1
p. 158

Abstract

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Stage II colon cancer (CC), although diagnosed early, accounts for 16% of CC deaths. Predictors of recurrence risk could mitigate this but are currently lacking. By using a DNA methylation-based clinical screening in real-world (n = 383) and in TCGA-derived cohorts of stage II CC (n = 134), we have devised a novel 40 CpG site-based classifier that can segregate stage II CC into four previously undescribed disease sub-classes that are characterised by distinct molecular features, including activation of MYC/E2F-dependant proliferation signatures. By multivariate analyses, hypermethylation of 2 CpG sites at genes CDH17 and LRP2, respectively, was found to independently confer either significantly increased (CDH17; p-value, 0.0203) or reduced (LRP2; p-value, 0.0047) risk of CC recurrence. Functional enrichment and immune cell infiltration analyses, on RNAseq data from the TCGA cohort, revealed cases with hypermethylation at CDH17 to be enriched for KRAS, epithelial-mesenchymal transition and inflammatory functions (via IL2/STAT5), associated with infiltration by ‘exhausted’ T cells. By contrast, LRP2 hypermethylated cases showed enrichment for mTORC1, DNA repair pathways and activated B cell signatures. These findings will be of value for improving personalised care paths and treatment in stage II CC patients.

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