Comparison of Molecular, Clinicopathological, and Pedigree Differences Between Lynch-Like and Lynch Syndromes

Comparison of Molecular, Clinicopathological, and Pedigree Differences Between Lynch-Like and Lynch Syndromes

In this study, we compared the molecular, clinical, and pathological characteristics, as well as pedigrees, between patients with Lynch-like syndrome (LLS) and confirmed Lynch syndrome (LS) to develop appropriate management strategies for patients with LLS and their affected family members. Between...

Full description

Bibliographic Details
Main Authors: Yun Xu, Zonghao Huang, Cong Li, Congcong Zhu, Yuqin Zhang, Tian’an Guo, Fangqi Liu, Ye Xu
Format: Article
Language:English
Published: Frontiers Media S.A. 2020-08-01
Series:Frontiers in Genetics
Subjects:
colorectal cancer
Lynch syndrome
Lynch-like syndrome
pedigree
DNA mismatch repair
Online Access:https://www.frontiersin.org/article/10.3389/fgene.2020.00991/full
id doaj-9595fbab61694b53aa20fd02be96a46b
record_format Article
spelling doaj-9595fbab61694b53aa20fd02be96a46b2020-11-25T03:48:29ZengFrontiers Media S.A.Frontiers in Genetics1664-80212020-08-011110.3389/fgene.2020.00991564813Comparison of Molecular, Clinicopathological, and Pedigree Differences Between Lynch-Like and Lynch SyndromesYun Xu0Yun Xu1Zonghao Huang2Cong Li3Cong Li4Congcong Zhu5Yuqin Zhang6Tian’an Guo7Fangqi Liu8Ye Xu9Ye Xu10Department of Colorectal Surgery, Fudan University Shanghai Cancer Center, Shanghai, ChinaDepartment of Oncology, Shanghai Medical College, Fudan University, Shanghai, ChinaHospital Information Centre, Fudan University Shanghai Cancer Center, Shanghai, ChinaDepartment of Colorectal Surgery, Fudan University Shanghai Cancer Center, Shanghai, ChinaDepartment of Oncology, Shanghai Medical College, Fudan University, Shanghai, ChinaDepartment of Oncology, Shanghai Medical College, Fudan University, Shanghai, ChinaDepartment of Oncology, Shanghai Medical College, Fudan University, Shanghai, ChinaDepartment of Oncology, Shanghai Medical College, Fudan University, Shanghai, ChinaDepartment of Colorectal Surgery, Fudan University Shanghai Cancer Center, Shanghai, ChinaDepartment of Colorectal Surgery, Fudan University Shanghai Cancer Center, Shanghai, ChinaDepartment of Oncology, Shanghai Medical College, Fudan University, Shanghai, ChinaIn this study, we compared the molecular, clinical, and pathological characteristics, as well as pedigrees, between patients with Lynch-like syndrome (LLS) and confirmed Lynch syndrome (LS) to develop appropriate management strategies for patients with LLS and their affected family members. Between June 2008 and September 2018, 81 patients with LLS and 47 patients with LS who developed colorectal cancer (CRC) were enrolled in this study. Multigene panel testing included 139 genes and was performed for all patients. The variants identified in each group were described, and clinicopathological characteristics and pedigrees were compared between the two groups. In the LLS group, a total of 52 variants were detected in 44 (54.3%) patients. Among the 52 variants, 17 were variants of unknown significance in mismatch repair genes, and the other most frequently mutated genes were MUYTH, POLE, BRCA2, and GJB2. The proportion of early-onset patients was significantly higher among the LS probands than among the LLS probands (74.5 and 53.1%, respectively; χ2 = 5.712, P = 0.017). On the other hand, the proportion of primary CRC developed in the rectum was higher in the LLS group than in the LS group (25.9 and 10.6%, respectively; χ2 = 2.358, P = 0.046). There were no significant differences in the occurrence of metachronous CRC (P = 0.632) and extra-colorectal cancer (extra-CRC) (P = 0.145) between the two groups. However, analysis of pedigrees showed that more patients developed CRC in the LS families (P = 0.013), whereas more patients with extra-CRC were observed in the LLS families (P = 0.045). A higher prevalence of male patients was observed in the LLS families (P = 0.036). In conclusion, LLS should be classified as a mixed entity, containing cases of LS, other hereditary cancer syndromes, and sporadic CRC. The high risks of CRC and extra-CRCs, which were found in this study, suggest tailored management policy and surveillance should be formulated based on individual and family risk. The surveillance regimen can be based on the presence of confirmed pathogenic/likely pathogenic germline variant(s) and family history.https://www.frontiersin.org/article/10.3389/fgene.2020.00991/fullcolorectal cancerLynch syndromeLynch-like syndromepedigreeDNA mismatch repair
collection DOAJ
language English
format Article
sources DOAJ
author Yun Xu
Yun Xu
Zonghao Huang
Cong Li
Cong Li
Congcong Zhu
Yuqin Zhang
Tian’an Guo
Fangqi Liu
Ye Xu
Ye Xu
spellingShingle Yun Xu
Yun Xu
Zonghao Huang
Cong Li
Cong Li
Congcong Zhu
Yuqin Zhang
Tian’an Guo
Fangqi Liu
Ye Xu
Ye Xu
Comparison of Molecular, Clinicopathological, and Pedigree Differences Between Lynch-Like and Lynch Syndromes
Frontiers in Genetics
colorectal cancer
Lynch syndrome
Lynch-like syndrome
pedigree
DNA mismatch repair
author_facet Yun Xu
Yun Xu
Zonghao Huang
Cong Li
Cong Li
Congcong Zhu
Yuqin Zhang
Tian’an Guo
Fangqi Liu
Ye Xu
Ye Xu
author_sort Yun Xu
title Comparison of Molecular, Clinicopathological, and Pedigree Differences Between Lynch-Like and Lynch Syndromes
title_short Comparison of Molecular, Clinicopathological, and Pedigree Differences Between Lynch-Like and Lynch Syndromes
title_full Comparison of Molecular, Clinicopathological, and Pedigree Differences Between Lynch-Like and Lynch Syndromes
title_fullStr Comparison of Molecular, Clinicopathological, and Pedigree Differences Between Lynch-Like and Lynch Syndromes
title_full_unstemmed Comparison of Molecular, Clinicopathological, and Pedigree Differences Between Lynch-Like and Lynch Syndromes
title_sort comparison of molecular, clinicopathological, and pedigree differences between lynch-like and lynch syndromes
publisher Frontiers Media S.A.
series Frontiers in Genetics
issn 1664-8021
publishDate 2020-08-01
description In this study, we compared the molecular, clinical, and pathological characteristics, as well as pedigrees, between patients with Lynch-like syndrome (LLS) and confirmed Lynch syndrome (LS) to develop appropriate management strategies for patients with LLS and their affected family members. Between June 2008 and September 2018, 81 patients with LLS and 47 patients with LS who developed colorectal cancer (CRC) were enrolled in this study. Multigene panel testing included 139 genes and was performed for all patients. The variants identified in each group were described, and clinicopathological characteristics and pedigrees were compared between the two groups. In the LLS group, a total of 52 variants were detected in 44 (54.3%) patients. Among the 52 variants, 17 were variants of unknown significance in mismatch repair genes, and the other most frequently mutated genes were MUYTH, POLE, BRCA2, and GJB2. The proportion of early-onset patients was significantly higher among the LS probands than among the LLS probands (74.5 and 53.1%, respectively; χ2 = 5.712, P = 0.017). On the other hand, the proportion of primary CRC developed in the rectum was higher in the LLS group than in the LS group (25.9 and 10.6%, respectively; χ2 = 2.358, P = 0.046). There were no significant differences in the occurrence of metachronous CRC (P = 0.632) and extra-colorectal cancer (extra-CRC) (P = 0.145) between the two groups. However, analysis of pedigrees showed that more patients developed CRC in the LS families (P = 0.013), whereas more patients with extra-CRC were observed in the LLS families (P = 0.045). A higher prevalence of male patients was observed in the LLS families (P = 0.036). In conclusion, LLS should be classified as a mixed entity, containing cases of LS, other hereditary cancer syndromes, and sporadic CRC. The high risks of CRC and extra-CRCs, which were found in this study, suggest tailored management policy and surveillance should be formulated based on individual and family risk. The surveillance regimen can be based on the presence of confirmed pathogenic/likely pathogenic germline variant(s) and family history.
topic colorectal cancer
Lynch syndrome
Lynch-like syndrome
pedigree
DNA mismatch repair
url https://www.frontiersin.org/article/10.3389/fgene.2020.00991/full
work_keys_str_mv AT yunxu comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT yunxu comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT zonghaohuang comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT congli comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT congli comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT congcongzhu comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT yuqinzhang comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT tiananguo comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT fangqiliu comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT yexu comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
AT yexu comparisonofmolecularclinicopathologicalandpedigreedifferencesbetweenlynchlikeandlynchsyndromes
_version_ 1724498788787159040

Similar Items