Comprehensive characterization of CRC with germline mutations reveals a distinct somatic mutational landscape and elevated cancer risk in the Chinese population

OBJECTIVE: Hereditary colorectal cancer (CRC) accounts for approximately 5%–10% of all CRC cases. The full profile of CRC-related germline mutations and the corresponding somatic mutational profile have not been fully determined in the Chinese population. METHODS: We performed the first population s...

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Autores principales: Yao, Jianfei, Zhen, Yunhuan, Fan, Jing, Gong, Yuan, Ye, Yumeng, Guo, Shaohua, Liu, Hongyi, Li, Xiaoyun, Li, Guosheng, Yang, Pan, Wang, Xiaohui, Liu, Danni, Huang, Tanxiao, Cao, Huiya, Suo, Peisu, Li, Yuemin, Yu, Jingbo, Song, Lele
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Compuscript 2022
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9196063/
https://www.ncbi.nlm.nih.gov/pubmed/35014770
http://dx.doi.org/10.20892/j.issn.2095-3941.2021.0190
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author Yao, Jianfei
Zhen, Yunhuan
Fan, Jing
Gong, Yuan
Ye, Yumeng
Guo, Shaohua
Liu, Hongyi
Li, Xiaoyun
Li, Guosheng
Yang, Pan
Wang, Xiaohui
Liu, Danni
Huang, Tanxiao
Cao, Huiya
Suo, Peisu
Li, Yuemin
Yu, Jingbo
Song, Lele
author_facet Yao, Jianfei
Zhen, Yunhuan
Fan, Jing
Gong, Yuan
Ye, Yumeng
Guo, Shaohua
Liu, Hongyi
Li, Xiaoyun
Li, Guosheng
Yang, Pan
Wang, Xiaohui
Liu, Danni
Huang, Tanxiao
Cao, Huiya
Suo, Peisu
Li, Yuemin
Yu, Jingbo
Song, Lele
author_sort Yao, Jianfei
collection PubMed
description OBJECTIVE: Hereditary colorectal cancer (CRC) accounts for approximately 5%–10% of all CRC cases. The full profile of CRC-related germline mutations and the corresponding somatic mutational profile have not been fully determined in the Chinese population. METHODS: We performed the first population study investigating the germline mutation status in more than 1,000 (n = 1,923) Chinese patients with CRC and examined their relationship with the somatic mutational landscape. Germline alterations were examined with a 58-gene next-generation sequencing panel, and somatic alterations were examined with a 605-gene panel. RESULTS: A total of 92 pathogenic (P) mutations were identified in 85 patients, and 81 likely pathogenic (LP) germline mutations were identified in 62 patients, accounting for 7.6% (147/1,923) of all patients. MSH2 and APC was the most mutated gene in the Lynch syndrome and non-Lynch syndrome groups, respectively. Patients with P/LP mutations had a significantly higher ratio of microsatellite instability, highly deficient mismatch repair, family history of CRC, and lower age. The somatic mutational landscape revealed a significantly higher mutational frequency in the P group and a trend toward higher copy number variations in the non-P group. The Lynch syndrome group had a significantly higher mutational frequency and tumor mutational burden than the non-Lynch syndrome group. Clustering analysis revealed that the Notch signaling pathway was uniquely clustered in the Lynch syndrome group, and the MAPK and cAMP signaling pathways were uniquely clustered in the non-Lynch syndrome group. Population risk analysis indicated that the overall odds ratio was 11.13 (95% CI: 8.289–15.44) for the P group and 20.68 (95% CI: 12.89–33.18) for the LP group. CONCLUSIONS: Distinct features were revealed in Chinese patients with CRC with germline mutations. The Notch signaling pathway was uniquely clustered in the Lynch syndrome group, and the MAPK and cAMP signaling pathways were uniquely clustered in the non-Lynch syndrome group. Patients with P/LP germline mutations exhibited higher CRC risk.
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spelling pubmed-91960632022-06-24 Comprehensive characterization of CRC with germline mutations reveals a distinct somatic mutational landscape and elevated cancer risk in the Chinese population Yao, Jianfei Zhen, Yunhuan Fan, Jing Gong, Yuan Ye, Yumeng Guo, Shaohua Liu, Hongyi Li, Xiaoyun Li, Guosheng Yang, Pan Wang, Xiaohui Liu, Danni Huang, Tanxiao Cao, Huiya Suo, Peisu Li, Yuemin Yu, Jingbo Song, Lele Cancer Biol Med Original Article OBJECTIVE: Hereditary colorectal cancer (CRC) accounts for approximately 5%–10% of all CRC cases. The full profile of CRC-related germline mutations and the corresponding somatic mutational profile have not been fully determined in the Chinese population. METHODS: We performed the first population study investigating the germline mutation status in more than 1,000 (n = 1,923) Chinese patients with CRC and examined their relationship with the somatic mutational landscape. Germline alterations were examined with a 58-gene next-generation sequencing panel, and somatic alterations were examined with a 605-gene panel. RESULTS: A total of 92 pathogenic (P) mutations were identified in 85 patients, and 81 likely pathogenic (LP) germline mutations were identified in 62 patients, accounting for 7.6% (147/1,923) of all patients. MSH2 and APC was the most mutated gene in the Lynch syndrome and non-Lynch syndrome groups, respectively. Patients with P/LP mutations had a significantly higher ratio of microsatellite instability, highly deficient mismatch repair, family history of CRC, and lower age. The somatic mutational landscape revealed a significantly higher mutational frequency in the P group and a trend toward higher copy number variations in the non-P group. The Lynch syndrome group had a significantly higher mutational frequency and tumor mutational burden than the non-Lynch syndrome group. Clustering analysis revealed that the Notch signaling pathway was uniquely clustered in the Lynch syndrome group, and the MAPK and cAMP signaling pathways were uniquely clustered in the non-Lynch syndrome group. Population risk analysis indicated that the overall odds ratio was 11.13 (95% CI: 8.289–15.44) for the P group and 20.68 (95% CI: 12.89–33.18) for the LP group. CONCLUSIONS: Distinct features were revealed in Chinese patients with CRC with germline mutations. The Notch signaling pathway was uniquely clustered in the Lynch syndrome group, and the MAPK and cAMP signaling pathways were uniquely clustered in the non-Lynch syndrome group. Patients with P/LP germline mutations exhibited higher CRC risk. Compuscript 2022-05-15 2022-01-12 /pmc/articles/PMC9196063/ /pubmed/35014770 http://dx.doi.org/10.20892/j.issn.2095-3941.2021.0190 Text en Copyright: © 2022, Cancer Biology & Medicine https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (CC BY) 4.0 (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution and reproduction in any medium, provided the original author and source are credited.
spellingShingle Original Article
Yao, Jianfei
Zhen, Yunhuan
Fan, Jing
Gong, Yuan
Ye, Yumeng
Guo, Shaohua
Liu, Hongyi
Li, Xiaoyun
Li, Guosheng
Yang, Pan
Wang, Xiaohui
Liu, Danni
Huang, Tanxiao
Cao, Huiya
Suo, Peisu
Li, Yuemin
Yu, Jingbo
Song, Lele
Comprehensive characterization of CRC with germline mutations reveals a distinct somatic mutational landscape and elevated cancer risk in the Chinese population
title Comprehensive characterization of CRC with germline mutations reveals a distinct somatic mutational landscape and elevated cancer risk in the Chinese population
title_full Comprehensive characterization of CRC with germline mutations reveals a distinct somatic mutational landscape and elevated cancer risk in the Chinese population
title_fullStr Comprehensive characterization of CRC with germline mutations reveals a distinct somatic mutational landscape and elevated cancer risk in the Chinese population
title_full_unstemmed Comprehensive characterization of CRC with germline mutations reveals a distinct somatic mutational landscape and elevated cancer risk in the Chinese population
title_short Comprehensive characterization of CRC with germline mutations reveals a distinct somatic mutational landscape and elevated cancer risk in the Chinese population
title_sort comprehensive characterization of crc with germline mutations reveals a distinct somatic mutational landscape and elevated cancer risk in the chinese population
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9196063/
https://www.ncbi.nlm.nih.gov/pubmed/35014770
http://dx.doi.org/10.20892/j.issn.2095-3941.2021.0190
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