Genomic profiling of multiple tissues in two patients with multiple endocrine neoplasia type 1

Akane NARUOKA; Sumiko OHNAMI; Takeshi NAGASHIMA; Masakuni SERIZAWA; Keiichi HATAKEYAMA; Keiichi OHSHIMA; Shumpei OHNAMI; Kenichi URAKAMI; Yasue HORIUCHI; Yoshimi KIYOZUMI; Hiroyuki MATSUBAYASHI; Masato ABE; Takuma OHISHI; Toru KAMEYA; Takashi SUGINO; Tetsuro ONITSUKA; Mitsuhiro ISAKA; Yasuhisa OHDE; Teiichi SUGIURA; Takaaki ITO; Katsuhiko UESAKA; Yasuto AKIYAMA; Masatoshi KUSUHARA; Ken YAMAGUCHI

doi:10.2220/biomedres.42.89

Communication

Genomic profiling of multiple tissues in two patients with multiple endocrine neoplasia type 1

Akane NARUOKA, Sumiko OHNAMI, Takeshi NAGASHIMA, Masakuni SERIZAWA, Keiichi HATAKEYAMA, Keiichi OHSHIMA, Shumpei OHNAMI, Kenichi URAKAMI, Yasue HORIUCHI, Yoshimi KIYOZUMI, Hiroyuki MATSUBAYASHI, Masato ABE, Takuma OHISHI, Toru KAMEYA, Takashi SUGINO, Tetsuro ONITSUKA, Mitsuhiro ISAKA, Yasuhisa OHDE, Teiichi SUGIURA, Takaaki ITO, Katsuhiko UESAKA, Yasuto AKIYAMA, Masatoshi KUSUHARA, Ken YAMAGUCHI

著者情報

Akane NARUOKA
Drug Discovery and Development Division, Shizuoka Cancer Center Research Institute
Sumiko OHNAMI
Cancer Diagnostics Research Division, Shizuoka Cancer Center Research Institute
Takeshi NAGASHIMA
Cancer Diagnostics Research Division, Shizuoka Cancer Center Research Institute
SRL Inc.
Masakuni SERIZAWA
Drug Discovery and Development Division, Shizuoka Cancer Center Research Institute
Keiichi HATAKEYAMA
Medical Genetics Division, Shizuoka Cancer Center Research Institute
Keiichi OHSHIMA
Medical Genetics Division, Shizuoka Cancer Center Research Institute
Shumpei OHNAMI
Cancer Diagnostics Research Division, Shizuoka Cancer Center Research Institute
Kenichi URAKAMI
Cancer Diagnostics Research Division, Shizuoka Cancer Center Research Institute
Yasue HORIUCHI
Division of Genetic Counseling, Shizuoka Cancer Center Hospital
Yoshimi KIYOZUMI
Division of Genetic Counseling, Shizuoka Cancer Center Hospital
Hiroyuki MATSUBAYASHI
Division of Genetic Counseling, Shizuoka Cancer Center Hospital
Masato ABE
Division of Pathology, Shizuoka Cancer Center Hospital
Takuma OHISHI
Division of Pathology, Shizuoka Cancer Center Hospital
Toru KAMEYA
Division of Pathology, Shizuoka Cancer Center Hospital
Takashi SUGINO
Division of Pathology, Shizuoka Cancer Center Hospital
Tetsuro ONITSUKA
Division of Head and Neck Surgery, Shizuoka Cancer Center Hospital
Mitsuhiro ISAKA
Division of Thoracic Surgery, Shizuoka Cancer Center Hospital
Yasuhisa OHDE
Division of Thoracic Surgery, Shizuoka Cancer Center Hospital
Teiichi SUGIURA
Division of Hepato-Biliary-Pancreatic Surgery, Shizuoka Cancer Center Hospital
Takaaki ITO
Division of Hepato-Biliary-Pancreatic Surgery, Shizuoka Cancer Center Hospital
Katsuhiko UESAKA
Division of Hepato-Biliary-Pancreatic Surgery, Shizuoka Cancer Center Hospital
Yasuto AKIYAMA
Immunotherapy Division, Shizuoka Cancer Center Research Institute
Masatoshi KUSUHARA
Shizuoka Cancer Center
Ken YAMAGUCHI
Shizuoka Cancer Center

ジャーナルフリー

2021 年 42 巻 2 号 p. 89-94

DOI https://doi.org/10.2220/biomedres.42.89

詳細

抄録

Multiple endocrine neoplasia type 1 (MEN1) is an autosomal dominant tumor syndrome. This hereditary cancer is caused by germline variants in MEN1. Two patients with MEN1 were identified via whole exome sequencing and gene expression profile analysis, conducted for 5,063 patients with various types of cancers. We obtained multiple tumors from each patient; tumors derived from these two MEN1 patients had a loss of the normal MEN1 allele and frequently chromosomal copy number changes. Thus, we investigated whether structural variants were present in the MEN1 patient genomes. Whole-genome sequencing revealed no catastrophic rearrangements, and the tumor samples had very low somatic variants. The two patients had germline variants in MEN1 and some chromosomal copy number changes including on chromosome 11. The only pathogenic variant detected was the MEN1 germline variant, and chromosomal rearrangements led to tumorigenesis in somatic cells. Furthermore, the MEN1 tumor samples displayed a specific signature characterized by T:A>C:G transition. Studies of multiple tumors obtained from single patients are rare in hereditary cancer syndromes, and our results provide insights that the second hit of the tumor suppressor gene MEN1 may be caused by a gross genome rearrangement, not a small insertion and deletion, nor a change in epigenetic regulation.

責任著者(Corresponding author)