| Literature DB >> 33594177 |
Masahiro Sekiguchi1, Masafumi Seki1, Tomoko Kawai2, Kenichi Yoshida3, Misa Yoshida1, Tomoya Isobe1, Noriko Hoshino4, Ryota Shirai5, Mio Tanaka6, Ryota Souzaki7, Kentaro Watanabe1, Yuki Arakawa8, Yasuhito Nannya3, Hiromichi Suzuki3, Yoichi Fujii9, Keisuke Kataoka10, Yuichi Shiraishi11, Kenichi Chiba11, Hiroko Tanaka12, Teppei Shimamura13, Yusuke Sato9, Aiko Sato-Otsubo1, Shunsuke Kimura1,14, Yasuo Kubota1, Mitsuteru Hiwatari1, Katsuyoshi Koh8, Yasuhide Hayashi15, Yutaka Kanamori16, Mureo Kasahara17, Kenichi Kohashi18, Motohiro Kato5, Takako Yoshioka19, Kimikazu Matsumoto5, Akira Oka1, Tomoaki Taguchi7, Masashi Sanada20, Yukichi Tanaka6, Satoru Miyano11, Kenichiro Hata2, Seishi Ogawa3,21,22, Junko Takita23,24.
Abstract
Although hepatoblastoma is the most common pediatric liver cancer, its genetic heterogeneity and therapeutic targets are not well elucidated. Therefore, we conducted a multiomics analysis, including mutatome, DNA methylome, and transcriptome analyses, of 59 hepatoblastoma samples. Based on DNA methylation patterns, hepatoblastoma was classified into three clusters exhibiting remarkable correlation with clinical, histological, and genetic features. Cluster F was largely composed of cases with fetal histology and good outcomes, whereas clusters E1 and E2 corresponded primarily to embryonal/combined histology and poor outcomes. E1 and E2, albeit distinguishable by different patient age distributions, were genetically characterized by hypermethylation of the HNF4A/CEBPA-binding regions, fetal liver-like expression patterns, upregulation of the cell cycle pathway, and overexpression of NQO1 and ODC1. Inhibition of NQO1 and ODC1 in hepatoblastoma cells induced chemosensitization and growth suppression, respectively. Our results provide a comprehensive description of the molecular basis of hepatoblastoma and rational therapeutic strategies for high-risk cases.Year: 2020 PMID: 33594177 DOI: 10.1038/s41698-020-0125-y
Source DB: PubMed Journal: NPJ Precis Oncol ISSN: 2397-768X