5‐Hydroxymethylcytosine signature in circulating cell‐free DNA as a potential diagnostic factor for early‐stage colorectal cancer and precancerous adenoma

Approximately 85% colorectal cancers (CRCs) are thought to evolve through the adenoma‐to‐carcinoma sequence associated with specific molecular alterations, including the 5‐hydroxymethylcytosine (5hmC) signature in circulating cell‐free DNA (cfDNA). To explore colorectal disease progression and evalu...

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Autores principales: Xiao, ZeWen, Wu, Wendy, Wu, Chunlong, Li, Man, Sun, Fuming, Zheng, Lu, Liu, Gaojing, Li, Xiaoling, Yun, Zhiyuan, Tang, Jiebing, Yu, Yang, Luo, Shengnan, Sun, Wenji, Feng, Xiaohong, Cheng, Qian, Tao, Xue, Wu, Shuangxiu, Tao, Ji
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2020
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7782095/
https://www.ncbi.nlm.nih.gov/pubmed/33107199
http://dx.doi.org/10.1002/1878-0261.12833
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author Xiao, ZeWen
Wu, Wendy
Wu, Chunlong
Li, Man
Sun, Fuming
Zheng, Lu
Liu, Gaojing
Li, Xiaoling
Yun, Zhiyuan
Tang, Jiebing
Yu, Yang
Luo, Shengnan
Sun, Wenji
Feng, Xiaohong
Cheng, Qian
Tao, Xue
Wu, Shuangxiu
Tao, Ji
author_facet Xiao, ZeWen
Wu, Wendy
Wu, Chunlong
Li, Man
Sun, Fuming
Zheng, Lu
Liu, Gaojing
Li, Xiaoling
Yun, Zhiyuan
Tang, Jiebing
Yu, Yang
Luo, Shengnan
Sun, Wenji
Feng, Xiaohong
Cheng, Qian
Tao, Xue
Wu, Shuangxiu
Tao, Ji
author_sort Xiao, ZeWen
collection PubMed
description Approximately 85% colorectal cancers (CRCs) are thought to evolve through the adenoma‐to‐carcinoma sequence associated with specific molecular alterations, including the 5‐hydroxymethylcytosine (5hmC) signature in circulating cell‐free DNA (cfDNA). To explore colorectal disease progression and evaluate the use of cfDNA as a potential diagnostic factor for CRC screening, here, we performed genome‐wide 5hmC profiling in plasma cfDNA and tissue genomic DNA (gDNA) acquired from 101 samples (63 plasma and 38 tissues), collected from 21 early‐stage CRC patients, 21 AD patients, and 21 healthy controls (HC). The gDNA and cfDNA 5hmC signatures identified in gene bodies and promoter regions in CRC and AD groups were compared with those in HC group. All the differential 5hmC‐modified regions (DhMRs) were gathered into four clusters: Disease‐enriched, AD‐enriched, Disease‐lost, and AD‐lost, with no overlap. AD‐related clusters, AD‐enriched and AD‐lost, displayed the unique 5hmC signals in AD patients. Disease‐enriched and Disease‐lost clusters indicated the general 5hmC changes when colorectal lesions occurred. Cancer patients with a confirmable adenoma history segmentally gathered in AD‐enriched clusters. KEGG functional enrichment and GO analyses determined distinct differential 5hmC‐modified profiles in cfDNA of HC individuals, AD, and CRC patients. All patients had comprehensive 5hmC signatures where Disease‐enriched and Disease‐lost DhMR clusters demonstrated similar epigenetic modifications, while AD‐enriched and AD‐lost DhMR clusters indicated complicated subpopulations in adenoma. Analysis of CRC patients with adenoma history showed exclusive 5hmC‐gain characteristics, consistent with the ‘parallel’ evolution hypothesis in adenoma, either developed through the adenoma‐to‐carcinoma sequence or not. These findings deepen our understanding of colorectal disease and suggest that the 5hmC modifications of different pathological subtypes (cancer patients with or without adenoma history) could be used to screen early‐stage CRC and assess adenoma malignancy with large‐scale follow‐up studies in the future.
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spelling pubmed-77820952021-01-08 5‐Hydroxymethylcytosine signature in circulating cell‐free DNA as a potential diagnostic factor for early‐stage colorectal cancer and precancerous adenoma Xiao, ZeWen Wu, Wendy Wu, Chunlong Li, Man Sun, Fuming Zheng, Lu Liu, Gaojing Li, Xiaoling Yun, Zhiyuan Tang, Jiebing Yu, Yang Luo, Shengnan Sun, Wenji Feng, Xiaohong Cheng, Qian Tao, Xue Wu, Shuangxiu Tao, Ji Mol Oncol Research Articles Approximately 85% colorectal cancers (CRCs) are thought to evolve through the adenoma‐to‐carcinoma sequence associated with specific molecular alterations, including the 5‐hydroxymethylcytosine (5hmC) signature in circulating cell‐free DNA (cfDNA). To explore colorectal disease progression and evaluate the use of cfDNA as a potential diagnostic factor for CRC screening, here, we performed genome‐wide 5hmC profiling in plasma cfDNA and tissue genomic DNA (gDNA) acquired from 101 samples (63 plasma and 38 tissues), collected from 21 early‐stage CRC patients, 21 AD patients, and 21 healthy controls (HC). The gDNA and cfDNA 5hmC signatures identified in gene bodies and promoter regions in CRC and AD groups were compared with those in HC group. All the differential 5hmC‐modified regions (DhMRs) were gathered into four clusters: Disease‐enriched, AD‐enriched, Disease‐lost, and AD‐lost, with no overlap. AD‐related clusters, AD‐enriched and AD‐lost, displayed the unique 5hmC signals in AD patients. Disease‐enriched and Disease‐lost clusters indicated the general 5hmC changes when colorectal lesions occurred. Cancer patients with a confirmable adenoma history segmentally gathered in AD‐enriched clusters. KEGG functional enrichment and GO analyses determined distinct differential 5hmC‐modified profiles in cfDNA of HC individuals, AD, and CRC patients. All patients had comprehensive 5hmC signatures where Disease‐enriched and Disease‐lost DhMR clusters demonstrated similar epigenetic modifications, while AD‐enriched and AD‐lost DhMR clusters indicated complicated subpopulations in adenoma. Analysis of CRC patients with adenoma history showed exclusive 5hmC‐gain characteristics, consistent with the ‘parallel’ evolution hypothesis in adenoma, either developed through the adenoma‐to‐carcinoma sequence or not. These findings deepen our understanding of colorectal disease and suggest that the 5hmC modifications of different pathological subtypes (cancer patients with or without adenoma history) could be used to screen early‐stage CRC and assess adenoma malignancy with large‐scale follow‐up studies in the future. John Wiley and Sons Inc. 2020-11-14 2021-01 /pmc/articles/PMC7782095/ /pubmed/33107199 http://dx.doi.org/10.1002/1878-0261.12833 Text en © 2020 The Authors. Molecular Oncology published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
Xiao, ZeWen
Wu, Wendy
Wu, Chunlong
Li, Man
Sun, Fuming
Zheng, Lu
Liu, Gaojing
Li, Xiaoling
Yun, Zhiyuan
Tang, Jiebing
Yu, Yang
Luo, Shengnan
Sun, Wenji
Feng, Xiaohong
Cheng, Qian
Tao, Xue
Wu, Shuangxiu
Tao, Ji
5‐Hydroxymethylcytosine signature in circulating cell‐free DNA as a potential diagnostic factor for early‐stage colorectal cancer and precancerous adenoma
title 5‐Hydroxymethylcytosine signature in circulating cell‐free DNA as a potential diagnostic factor for early‐stage colorectal cancer and precancerous adenoma
title_full 5‐Hydroxymethylcytosine signature in circulating cell‐free DNA as a potential diagnostic factor for early‐stage colorectal cancer and precancerous adenoma
title_fullStr 5‐Hydroxymethylcytosine signature in circulating cell‐free DNA as a potential diagnostic factor for early‐stage colorectal cancer and precancerous adenoma
title_full_unstemmed 5‐Hydroxymethylcytosine signature in circulating cell‐free DNA as a potential diagnostic factor for early‐stage colorectal cancer and precancerous adenoma
title_short 5‐Hydroxymethylcytosine signature in circulating cell‐free DNA as a potential diagnostic factor for early‐stage colorectal cancer and precancerous adenoma
title_sort 5‐hydroxymethylcytosine signature in circulating cell‐free dna as a potential diagnostic factor for early‐stage colorectal cancer and precancerous adenoma
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7782095/
https://www.ncbi.nlm.nih.gov/pubmed/33107199
http://dx.doi.org/10.1002/1878-0261.12833
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