Assessment of epigenetic alterations in early colorectal lesions containing BRAF mutations

To clarify the molecular and clinicopathological characteristics of colorectal serrated lesions, we assessed the DNA methylation of cancer-associated genes in a cohort of BRAF-mutant precancerous lesions from 94 individuals. We then compared those results with the lesions' clinicopathological f...

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Autores principales: Sawada, Takeshi, Yamamoto, Eiichiro, Yamano, Hiro-o, Nojima, Masanori, Harada, Taku, Maruyama, Reo, Ashida, Masami, Aoki, Hironori, Matsushita, Hiro-o, Yoshikawa, Kenjiro, Harada, Eiji, Tanaka, Yoshihito, Wakita, Shigenori, Niinuma, Takeshi, Kai, Masahiro, Eizuka, Makoto, Sugai, Tamotsu, Suzuki, Hiromu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5085213/
https://www.ncbi.nlm.nih.gov/pubmed/27145369
http://dx.doi.org/10.18632/oncotarget.9044
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author Sawada, Takeshi
Yamamoto, Eiichiro
Yamano, Hiro-o
Nojima, Masanori
Harada, Taku
Maruyama, Reo
Ashida, Masami
Aoki, Hironori
Matsushita, Hiro-o
Yoshikawa, Kenjiro
Harada, Eiji
Tanaka, Yoshihito
Wakita, Shigenori
Niinuma, Takeshi
Kai, Masahiro
Eizuka, Makoto
Sugai, Tamotsu
Suzuki, Hiromu
author_facet Sawada, Takeshi
Yamamoto, Eiichiro
Yamano, Hiro-o
Nojima, Masanori
Harada, Taku
Maruyama, Reo
Ashida, Masami
Aoki, Hironori
Matsushita, Hiro-o
Yoshikawa, Kenjiro
Harada, Eiji
Tanaka, Yoshihito
Wakita, Shigenori
Niinuma, Takeshi
Kai, Masahiro
Eizuka, Makoto
Sugai, Tamotsu
Suzuki, Hiromu
author_sort Sawada, Takeshi
collection PubMed
description To clarify the molecular and clinicopathological characteristics of colorectal serrated lesions, we assessed the DNA methylation of cancer-associated genes in a cohort of BRAF-mutant precancerous lesions from 94 individuals. We then compared those results with the lesions' clinicopathological features, especially colorectal subsites. The lesions included hyperplastic polyps (n = 16), traditional serrated adenomas (TSAs) (n = 15), TSAs with sessile serrated adenomas (SSAs) (n = 6), SSAs (n = 49) and SSAs with dysplasia (n = 16). The prevalence of lesions exhibiting the CpG island methylator phenotype (CIMP) was lower in the sigmoid colon and rectum than in other bowel subsites, including the cecum, ascending, transverse and descending colon. In addition, several cancer-associated genes showed higher methylation levels within lesions in the proximal to sigmoid colon than in the sigmoid colon and rectum. These results indicate that the methylation status of lesions with BRAF mutation is strongly associated with their location, histological findings and neoplastic pathways. By contrast, no difference in aberrant DNA methylation was observed in normal-appearing background colonic mucosa along the bowel subsites, which may indicate the absence of an epigenetic field defect.
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spelling pubmed-50852132016-10-31 Assessment of epigenetic alterations in early colorectal lesions containing BRAF mutations Sawada, Takeshi Yamamoto, Eiichiro Yamano, Hiro-o Nojima, Masanori Harada, Taku Maruyama, Reo Ashida, Masami Aoki, Hironori Matsushita, Hiro-o Yoshikawa, Kenjiro Harada, Eiji Tanaka, Yoshihito Wakita, Shigenori Niinuma, Takeshi Kai, Masahiro Eizuka, Makoto Sugai, Tamotsu Suzuki, Hiromu Oncotarget Research Paper To clarify the molecular and clinicopathological characteristics of colorectal serrated lesions, we assessed the DNA methylation of cancer-associated genes in a cohort of BRAF-mutant precancerous lesions from 94 individuals. We then compared those results with the lesions' clinicopathological features, especially colorectal subsites. The lesions included hyperplastic polyps (n = 16), traditional serrated adenomas (TSAs) (n = 15), TSAs with sessile serrated adenomas (SSAs) (n = 6), SSAs (n = 49) and SSAs with dysplasia (n = 16). The prevalence of lesions exhibiting the CpG island methylator phenotype (CIMP) was lower in the sigmoid colon and rectum than in other bowel subsites, including the cecum, ascending, transverse and descending colon. In addition, several cancer-associated genes showed higher methylation levels within lesions in the proximal to sigmoid colon than in the sigmoid colon and rectum. These results indicate that the methylation status of lesions with BRAF mutation is strongly associated with their location, histological findings and neoplastic pathways. By contrast, no difference in aberrant DNA methylation was observed in normal-appearing background colonic mucosa along the bowel subsites, which may indicate the absence of an epigenetic field defect. Impact Journals LLC 2016-04-27 /pmc/articles/PMC5085213/ /pubmed/27145369 http://dx.doi.org/10.18632/oncotarget.9044 Text en Copyright: © 2016 Sawada et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Sawada, Takeshi
Yamamoto, Eiichiro
Yamano, Hiro-o
Nojima, Masanori
Harada, Taku
Maruyama, Reo
Ashida, Masami
Aoki, Hironori
Matsushita, Hiro-o
Yoshikawa, Kenjiro
Harada, Eiji
Tanaka, Yoshihito
Wakita, Shigenori
Niinuma, Takeshi
Kai, Masahiro
Eizuka, Makoto
Sugai, Tamotsu
Suzuki, Hiromu
Assessment of epigenetic alterations in early colorectal lesions containing BRAF mutations
title Assessment of epigenetic alterations in early colorectal lesions containing BRAF mutations
title_full Assessment of epigenetic alterations in early colorectal lesions containing BRAF mutations
title_fullStr Assessment of epigenetic alterations in early colorectal lesions containing BRAF mutations
title_full_unstemmed Assessment of epigenetic alterations in early colorectal lesions containing BRAF mutations
title_short Assessment of epigenetic alterations in early colorectal lesions containing BRAF mutations
title_sort assessment of epigenetic alterations in early colorectal lesions containing braf mutations
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5085213/
https://www.ncbi.nlm.nih.gov/pubmed/27145369
http://dx.doi.org/10.18632/oncotarget.9044
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