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Original Article

Methylation patterns in dysplasia in inflammatory bowel disease patients

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Pages 646-655 | Received 03 Feb 2020, Accepted 04 May 2020, Published online: 26 May 2020
 

Abstract

Background and aims: Inflammatory Bowel Disease (IBD) with colonic involvement increases colorectal cancer risk. However, the distinction between IBD related and sporadic dysplasia in IBD patients is difficult. Some data favors the importance of abnormal DNA methylation in IBD-related carcinogenesis. We aimed to define methylation patterns in patients with colonic cancer or dysplasia diagnosis following an IBD diagnosis.

Methods: Multicentric cross-sectional study-91 samples from colonic mucosa with/without dysplasia from 9 patients with IBD-related dysplasia/cancer and 26 patients with IBD and sporadic dysplasia/cancer were included. Methylation patterns of CpG islands in the promoter regions of 67 genes were studied by Methylation-specific Multiplex Ligation-dependent Probe Amplification.

Results: Mean age at IBD diagnosis: 42 ± 16 years;at dysplasia diagnosis: 56 ± 14 years. Twenty-ninepatients had ulcerative colitis. Twenty-five patients had at least 1 lesion endoscopically described as adenoma-like, 4 at least 1 non-adenoma like, 3 had cancer and 3 had dysplasia in flat mucosa. No patient had both adenoma-like and non-adenoma-like lesions. Patients with an IBD-related lesion were significantly younger at IBD diagnosis (p = .003) and at dysplasia/cancer diagnosis (p = .039). Promoter methylation of IGF2, RARB, ESR1, CHFR, CDH13, WT1, GATA5, WIF1genes was significantly associated to dysplasia/cancer; methylation of MSH6, TIMP3 was significantly associated to IBD-related dysplasia/cancer. Promoter methylation of MSH6, MSH3, RUNX3, CRABP1, TP73, RARB, CDH13, PAX5, WT1, THBS1, TP53, SFRP1, WIF1, APAF1, BCL2 genes was significantly associated to active IBD.

Conclusions: Methylation analysis, namely of MSH6, may contribute to the classification of dysplastic lesions in IBD– to be further tested in prospective studies.

Acknowledgments

GEDII provided administrative and data collection and analysis support. GEDII’s scientific committee critically reviewed the manuscript.

Disclosure statement

Isadora Rosa reports grants, personal fees or non-financial support from ABBVIE, FERRING, MSD, TAKEDA, PHARMAKERN, JANSSEN, and DR FALK PHARMA, outside the submitted work; Helena Tavares de Sousa reports personal fees or non-financial support from ABBVIE, FERRING, MSD, TAKEDA, PHARMAKERN, JANSSEN, PFIZER and DR FALK PHARMA; Joana Roseira reports personal fees or non-financial support from ABBVIE, MSD, TAKEDA, JANSSEN, PfFIZER and DR FALK PHARMA; the remaining authors have nothing to disclose.

Author contributions

I.R., P.S., S.M., R.F., C.A. and GEDII participated in the conception and design of the study; all authors collected and analyzed data for the study; P.S., S.M., R. F. and C.A. did the central pathology and molecular analysis; I.R. drafted the article. All authors revised the article critically for important intellectual content and gave approval of the final version to be submitted.

Additional information

Funding

This work was supported by a funding grant from Grupo de Estudos em Doença Inflamatória Intestinal (GEDII), Portugal, a non-profit Portuguese research organization.

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