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Biased expression of mutant alleles in cancer-related genes in esophageal squamous cell carcinoma

Authors :
Masahiko Takahashi
Kazuyoshi Hosomichi
Hirofumi Nakaoka
Haruhito Sakata
Naoya Uesato
Kentaro Murakami
Masayuki Kano
Takeshi Toyozumi
Yasunori Matsumoto
Tetsuro Isozaki
Nobufumi Sekino
Ryota Otsuka
Itsuro Inoue
Hisahiro Matsubara
Source :
Esophagus. 19:294-302
Publication Year :
2022
Publisher :
Springer Science and Business Media LLC, 2022.

Abstract

Recent progress of large-scale international studies has provided comprehensive catalogs of somatic mutations in cancers. Additionally, it has become evident that allelic imbalance in the abundance of somatic mutations between DNA and RNA were pervasive in various types of cancer. However, the allelic imbalance of the abundance of somatic mutations in esophageal squamous cell carcinoma (ESCC) has not been fully analyzed.We performed exome sequencing for 25 Japanese patients with ESCC to detect a comprehensive catalog of somatic mutations in ESCC. Additionally, we performed mRNA sequencing to evaluate the allelic imbalance of the identified somatic mutations at the transcriptional level by comparing the mutant allele frequencies between RNA and DNA.The exome sequencing showed that TP53 and ZNF750 were significantly mutated genes. The expression levels of TP53 and ZNF750 were different depending on the mutation status. In almost all the tumors with missense mutations in TP53 and ZNF750, the mutant allele frequencies were higher in the RNA sequencing than those in the exome sequencing, indicating that the mutant alleles were preferentially expressed. By examining the allelic imbalances for all the identified missense mutations, we demonstrated that genes showing preferential expressions of the mutant alleles were involved in the pathways including cell cycle, cell death, and chromatin modification.The results of this study suggest that the allelic imbalance of the abundance of somatic mutations plays important roles in the initiation and progression of ESCC by modulating cancer-related biological pathways.

Details

ISSN :
16129067 and 16129059
Volume :
19
Database :
OpenAIRE
Journal :
Esophagus
Accession number :
edsair.doi.dedup.....877d42edaabf60f17040d1718a087c10