Methylation patterns in dysplasia in inflammatory bowel disease patients.

Rosa, Isadora; Silva, Patrícia; da Mata, Sara; Magro, Fernando; Carneiro, Fátima; Peixoto, Armando; Silva, Marco; Sousa, Helena T; Roseira, Joana; Parra, José; Barosa, Rita; Vieira, Ana; Brito, Maria José; Lago, Paula; Coelho, André; Moleiro, Joana; Pereira da Silva, João; Fonseca, Ricardo; Albuquerque, Cristina; Dias Pereira, A

Rosa, Isadora; Silva, Patrícia; da Mata, Sara; Magro, Fernando; Carneiro, Fátima; Peixoto, Armando; Silva, Marco; Sousa, Helena T; Roseira, Joana; Parra, José; Barosa, Rita; Vieira, Ana; Brito, Maria José; Lago, Paula; Coelho, André; Moleiro, Joana; Pereira da Silva, João; Fonseca, Ricardo; Albuquerque, Cristina; Dias Pereira, A.

Rosa I; Gastroenterology Department, Instituto Português de Oncologia de Lisboa, Francisco Gentil, EPE, Lisboa, Portugal.
Silva P; Molecular Pathobiology Investigation Unit, Instituto Português de Oncologia de Lisboa, Francisco Gentil, EPE, Lisboa, Portugal.
da Mata S; Pathology Department, Instituto Português de Oncologia de Lisboa, Francisco Gentil, EPE, Lisboa, Portugal.
Magro F; Gastroenterology Department, Centro Hospitalar de São João, EPE, Porto, Portugal.
Carneiro F; Pathology Department, Centro Hospitalar de São João, EPE, Porto, Portugal.
Peixoto A; Gastroenterology Department, Centro Hospitalar de São João, EPE, Porto, Portugal.
Silva M; Gastroenterology Department, Centro Hospitalar de São João, EPE, Porto, Portugal.
Sousa HT; Gastroenterology Department, Centro Hospitalar Universitário do Algarve, EPE, Unidade de Portimão, Portimão, Portugal.
Roseira J; Algarve Biomedical Center, Campus Gambelas - Universidade do Algarve, Faro, Portugal.
Parra J; Gastroenterology Department, Centro Hospitalar Universitário do Algarve, EPE, Unidade de Portimão, Portimão, Portugal.
Barosa R; Algarve Biomedical Center, Campus Gambelas - Universidade do Algarve, Faro, Portugal.
Vieira A; Pathology Department, Centro Hospitalar Universitário do Algarve, EPE, Unidade de Portimão, Portimão, Portugal.
Brito MJ; Gastroenterology Department, Hospital Garcia de Orta, EPE, Almada, Portugal.
Lago P; Gastroenterology Department, Hospital Garcia de Orta, EPE, Almada, Portugal.
Coelho A; Pathology Department, Hospital Garcia de Orta, EPE, Almada, Portugal.
Moleiro J; Gastroenterology Department, Centro Hospitalar do Porto, EPE - Hospital de Santo António, Porto, Portugal.
Pereira da Silva J; Portuguese Inflammatory Bowel Diseases Study Group, Porto, Portugal.
Fonseca R; Gastroenterology Department, Instituto Português de Oncologia de Lisboa, Francisco Gentil, EPE, Lisboa, Portugal.
Albuquerque C; Gastroenterology Department, Instituto Português de Oncologia de Lisboa, Francisco Gentil, EPE, Lisboa, Portugal.
Dias Pereira A; Pathology Department, Instituto Português de Oncologia de Lisboa, Francisco Gentil, EPE, Lisboa, Portugal.

Scand J Gastroenterol ; 55(6): 646-655, 2020 Jun.

Article en En | MEDLINE | ID: mdl-32456486

ABSTRACT

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.

Asunto(s)

Adenoma/genética; Colitis Ulcerosa/genética; Colon/patología; Neoplasias del Colon/genética; Metilación de ADN/genética; Mucosa Intestinal/patología; Adenoma/patología; Adulto; Biomarcadores de Tumor/genética; Carcinogénesis/genética; Colitis Ulcerosa/patología; Neoplasias del Colon/patología; Estudios Transversales; Proteínas de Unión al ADN/genética; Femenino; Humanos; Masculino; Persona de Mediana Edad; Portugal; Regiones Promotoras Genéticas/genética

Palabras clave

Inflammatory bowel disease; cancer; dysplasia

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Texto completo: 1 Banco de datos: MEDLINE Asunto principal: Colitis Ulcerosa / Adenoma / Colon / Neoplasias del Colon / Metilación de ADN / Mucosa Intestinal Tipo de estudio: Clinical_trials / Observational_studies / Prevalence_studies / Risk_factors_studies Límite: Adult / Female / Humans / Male / Middle aged País como asunto: Europa Idioma: En Año: 2020 Tipo del documento: Article

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