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Journal of Cancer Research and Clinical Oncology

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01-01-2021 | Gastric Cancer | Original Article – Cancer Research

Analysis of genomic pathogenesis according to the revised Bethesda guidelines and additional criteria

Authors: Jin Cheon Kim, Jong Hwan Kim, Ye Jin Ha, Chan Wook Kim, Ka Hee Tak, Yong Sik Yoon, Yi Hong Kwon, Seon Ae Roh, Dong-Hyung Cho, Seon-Kyu Kim, Seon-Young Kim, Yong Sung Kim

Published in: Journal of Cancer Research and Clinical Oncology | Issue 1/2021

Abstract

Purpose

As few genotype–phenotype correlations are available for nonsyndromic hereditary colorectal cancer (CRC), we implemented genomic analysis on the basis of the revised Bethesda guideline (RBG) and extended (12 items) to verify possible subtypes.

Methods

Patients with sporadic CRC (n = 249) were enrolled, stratified according to the revised Bethesda guidelines (RBG+ and RBG− groups) plus additional criteria. Exome/transcriptome analyses (n = 98) and cell-based functional assays were conducted.

Results

We detected 469 somatic and 830 germline gene mutations differing significantly between the positive and negative groups, associated with 12 RBG items/additional criteria. Twenty-one genes had significantly higher mutation rates in left, relative to right, colon cancer, while USP40, HCFC1, and HSPG2 mutation rates were higher in rectal than colon cancer. FAT4 mutation rates were lower in early-onset CRC, in contrast to increased rates in microsatellite instability (MSI)-positive tumors, potentially defining an early-onset microsatellite-stable subtype. The mutation rates of COL6A5 and MGAM2 were significantly and SETD5 was assumably, associated CRC pedigree with concurrent gastric cancer (GC). The predicted deleterious/damaging germline variants, SH2D4A rs35647122, was associated with synchronous/metachronous CRC with related tumors, while NUP160 rs381660 and KRTAP27-1 rs2244485 were potentially associated with a GC pedigree and less strictly defined hereditary CRC, respectively. SH2D4A and NUP160 acted as oncogenic facilitators.

Conclusion

Our limited genomic analysis for RBG and additional items suggested that specific somatic alterations in the respective items may enlighten relevant pathogenesis along with the knowledge of germline mutations. Further validation is needed to indicate appropriate surveillance in suspected individuals.

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Title: Analysis of genomic pathogenesis according to the revised Bethesda guidelines and additional criteria
Authors: Jin Cheon Kim
Jong Hwan Kim
Ye Jin Ha
Chan Wook Kim
Ka Hee Tak
Yong Sik Yoon
Yi Hong Kwon
Seon Ae Roh
Dong-Hyung Cho
Seon-Kyu Kim
Seon-Young Kim
Yong Sung Kim
Publication date: 01-01-2021
Publisher: Springer Berlin Heidelberg
Keywords: Gastric Cancer
Gastric Cancer
Colorectal Cancer
Colorectal Cancer
Colon Cancer
Colon Cancer
Published in: Journal of Cancer Research and Clinical Oncology / Issue 1/2021
Print ISSN: 0171-5216
Electronic ISSN: 1432-1335
DOI: https://doi.org/10.1007/s00432-020-03391-8

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