The Largest Chinese Cohort Study Indicates Homologous Recombination Pathway Gene Mutations as Another Major Genetic Risk Factor for Colorectal Cancer with Heterogeneous Clinical Phenotypes

While genetic factors were associated with over 30% of colorectal cancer (CRC) patients, mutations in CRC-susceptibility genes were identified in only 5% to 10% of these patients. Besides, previous studies on hereditary CRC were largely designed to analyze germline mutations in patients with single...

Descripción completa

Detalles Bibliográficos
Autores principales: Xu, Yun, Liu, Kai, Li, Cong, Li, Minghan, Liu, Fangqi, Zhou, Xiaoyan, Sun, Menghong, Ranganathan, Megha, Zhang, Liying, Wang, Sheng, Hu, Xin, Xu, Ye
Formato: Online Artículo Texto
Lenguaje:English
Publicado: AAAS 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10581333/
https://www.ncbi.nlm.nih.gov/pubmed/37854294
http://dx.doi.org/10.34133/research.0249
_version_ 1785122119780139008
author Xu, Yun
Liu, Kai
Li, Cong
Li, Minghan
Liu, Fangqi
Zhou, Xiaoyan
Sun, Menghong
Ranganathan, Megha
Zhang, Liying
Wang, Sheng
Hu, Xin
Xu, Ye
author_facet Xu, Yun
Liu, Kai
Li, Cong
Li, Minghan
Liu, Fangqi
Zhou, Xiaoyan
Sun, Menghong
Ranganathan, Megha
Zhang, Liying
Wang, Sheng
Hu, Xin
Xu, Ye
author_sort Xu, Yun
collection PubMed
description While genetic factors were associated with over 30% of colorectal cancer (CRC) patients, mutations in CRC-susceptibility genes were identified in only 5% to 10% of these patients. Besides, previous studies on hereditary CRC were largely designed to analyze germline mutations in patients with single genetic high-risk factor, which limited understanding of the association between genotype and phenotypes. From January 2015 to December 2018, we retrospectively enrolled 2,181 patients from 8,270 consecutive CRC cases, covering 5 categories of genetic high-risk factors. Leukocyte genomic DNA was analyzed for germline mutations in cancer predisposition genes. The germline mutations under each category were detected and analyzed in association with CRC susceptibility, clinical phenotypes, and prognoses. A total of 462 pathogenic variants were detected in 19.3% of enrolled CRC patients. Mismatch repair gene mutation was identified in 9.1% of patients, most prevalent across all high-risk groups. Homologous recombination (HR) gene mutations were detected in 6.5% of cases, penetrated in early-onset and extra-colonic cancer risk groups. Mutations in HR genes, including BARD1, RAD50, and ATM, were found to increase CRC risk with odds ratios of 2.8-, 3.1-, and 3.1-fold, respectively. CRC patients with distinct germline mutations manifested heterogeneous phenotypes in clinicopathology and long-term prognoses. Thus, germline mutation screenings should be performed for CRC patients with any of those genetic risk factors. This study also reveals that HR gene mutations may be another major driver for increased CRC risk.
format Online
Article
Text
id pubmed-10581333
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher AAAS
record_format MEDLINE/PubMed
spelling pubmed-105813332023-10-18 The Largest Chinese Cohort Study Indicates Homologous Recombination Pathway Gene Mutations as Another Major Genetic Risk Factor for Colorectal Cancer with Heterogeneous Clinical Phenotypes Xu, Yun Liu, Kai Li, Cong Li, Minghan Liu, Fangqi Zhou, Xiaoyan Sun, Menghong Ranganathan, Megha Zhang, Liying Wang, Sheng Hu, Xin Xu, Ye Research (Wash D C) Research Article While genetic factors were associated with over 30% of colorectal cancer (CRC) patients, mutations in CRC-susceptibility genes were identified in only 5% to 10% of these patients. Besides, previous studies on hereditary CRC were largely designed to analyze germline mutations in patients with single genetic high-risk factor, which limited understanding of the association between genotype and phenotypes. From January 2015 to December 2018, we retrospectively enrolled 2,181 patients from 8,270 consecutive CRC cases, covering 5 categories of genetic high-risk factors. Leukocyte genomic DNA was analyzed for germline mutations in cancer predisposition genes. The germline mutations under each category were detected and analyzed in association with CRC susceptibility, clinical phenotypes, and prognoses. A total of 462 pathogenic variants were detected in 19.3% of enrolled CRC patients. Mismatch repair gene mutation was identified in 9.1% of patients, most prevalent across all high-risk groups. Homologous recombination (HR) gene mutations were detected in 6.5% of cases, penetrated in early-onset and extra-colonic cancer risk groups. Mutations in HR genes, including BARD1, RAD50, and ATM, were found to increase CRC risk with odds ratios of 2.8-, 3.1-, and 3.1-fold, respectively. CRC patients with distinct germline mutations manifested heterogeneous phenotypes in clinicopathology and long-term prognoses. Thus, germline mutation screenings should be performed for CRC patients with any of those genetic risk factors. This study also reveals that HR gene mutations may be another major driver for increased CRC risk. AAAS 2023-10-17 /pmc/articles/PMC10581333/ /pubmed/37854294 http://dx.doi.org/10.34133/research.0249 Text en Copyright © 2023 Yun Xu et al. https://creativecommons.org/licenses/by/4.0/Exclusive licensee Science and Technology Review Publishing House. No claim to original U.S. Government Works. Distributed under a Creative Commons Attribution License 4.0 (CC BY 4.0) (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Xu, Yun
Liu, Kai
Li, Cong
Li, Minghan
Liu, Fangqi
Zhou, Xiaoyan
Sun, Menghong
Ranganathan, Megha
Zhang, Liying
Wang, Sheng
Hu, Xin
Xu, Ye
The Largest Chinese Cohort Study Indicates Homologous Recombination Pathway Gene Mutations as Another Major Genetic Risk Factor for Colorectal Cancer with Heterogeneous Clinical Phenotypes
title The Largest Chinese Cohort Study Indicates Homologous Recombination Pathway Gene Mutations as Another Major Genetic Risk Factor for Colorectal Cancer with Heterogeneous Clinical Phenotypes
title_full The Largest Chinese Cohort Study Indicates Homologous Recombination Pathway Gene Mutations as Another Major Genetic Risk Factor for Colorectal Cancer with Heterogeneous Clinical Phenotypes
title_fullStr The Largest Chinese Cohort Study Indicates Homologous Recombination Pathway Gene Mutations as Another Major Genetic Risk Factor for Colorectal Cancer with Heterogeneous Clinical Phenotypes
title_full_unstemmed The Largest Chinese Cohort Study Indicates Homologous Recombination Pathway Gene Mutations as Another Major Genetic Risk Factor for Colorectal Cancer with Heterogeneous Clinical Phenotypes
title_short The Largest Chinese Cohort Study Indicates Homologous Recombination Pathway Gene Mutations as Another Major Genetic Risk Factor for Colorectal Cancer with Heterogeneous Clinical Phenotypes
title_sort largest chinese cohort study indicates homologous recombination pathway gene mutations as another major genetic risk factor for colorectal cancer with heterogeneous clinical phenotypes
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10581333/
https://www.ncbi.nlm.nih.gov/pubmed/37854294
http://dx.doi.org/10.34133/research.0249
work_keys_str_mv AT xuyun thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT liukai thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT licong thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT liminghan thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT liufangqi thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT zhouxiaoyan thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT sunmenghong thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT ranganathanmegha thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT zhangliying thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT wangsheng thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT huxin thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT xuye thelargestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT xuyun largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT liukai largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT licong largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT liminghan largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT liufangqi largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT zhouxiaoyan largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT sunmenghong largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT ranganathanmegha largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT zhangliying largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT wangsheng largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT huxin largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes
AT xuye largestchinesecohortstudyindicateshomologousrecombinationpathwaygenemutationsasanothermajorgeneticriskfactorforcolorectalcancerwithheterogeneousclinicalphenotypes

Ejemplares similares