Distinct molecular profile of diffuse cerebellar gliomas

Masashi Nomura; Akitake Mukasa; Genta Nagae; Shogo Yamamoto; Kenji Tatsuno; Hiroki Ueda; Shiro Fukuda; Takayoshi Umeda; Tomonari Suzuki; Ryohei Otani; Keiichi Kobayashi; Takashi Maruyama; Shota Tanaka; Shunsaku Takayanagi; Takahide Nejo; Satoshi Takahashi; Koichi Ichimura; Taishi Nakamura; Yoshihiro Muragaki; Yoshitaka Narita; Motoo Nagane; Keisuke Ueki; Ryo Nishikawa; Junji Shibahara; Hiroyuki Aburatani; Nobuhito Saito

doi:10.1007/s00401-017-1771-1

Distinct molecular profile of diffuse cerebellar gliomas

Acta Neuropathol. 2017 Dec;134(6):941-956. doi: 10.1007/s00401-017-1771-1. Epub 2017 Aug 29.

Authors

Masashi Nomura^{1

2}, Akitake Mukasa³, Genta Nagae², Shogo Yamamoto², Kenji Tatsuno², Hiroki Ueda², Shiro Fukuda², Takayoshi Umeda², Tomonari Suzuki⁴, Ryohei Otani⁵, Keiichi Kobayashi⁶, Takashi Maruyama⁷, Shota Tanaka¹, Shunsaku Takayanagi¹, Takahide Nejo¹, Satoshi Takahashi¹, Koichi Ichimura⁸, Taishi Nakamura⁹, Yoshihiro Muragaki⁷, Yoshitaka Narita¹⁰, Motoo Nagane⁶, Keisuke Ueki⁵, Ryo Nishikawa⁴, Junji Shibahara¹¹, Hiroyuki Aburatani¹², Nobuhito Saito¹

Affiliations

¹ Department of Neurosurgery, Graduate School of Medicine, The University of Tokyo, 7-3-1 Hongo, Bunkyo-ku, Tokyo, 113-8655, Japan.
² Genome Science Division, Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, 4-6-1 Komaba, Meguro-ku, Tokyo, 153-8904, Japan.
³ Department of Neurosurgery, Graduate School of Medicine, The University of Tokyo, 7-3-1 Hongo, Bunkyo-ku, Tokyo, 113-8655, Japan. mukasa-nsu@umin.ac.jp.
⁴ Department of Neuro-Oncology/Neurosurgery, Saitama International Medical Center, Saitama Medical University, 1397-1 Yamane, Hidaka-shi, Saitama, 350-1298, Japan.
⁵ Department of Neurosurgery, Dokkyo Medical University, 880 Kitakobayashi, Mibu-machi, Shimotsuga-gun, Tochigi, 321-0293, Japan.
⁶ Department of Neurosurgery, Kyorin University Faculty of Medicine, 6-20-2 Shinkawa, Mitaka, Tokyo, 181-8611, Japan.
⁷ Department of Neurosurgery, Tokyo Women's Medical University, 8-1, Kawada-cho, Shinjuku-ku, Tokyo, 162-8666, Japan.
⁸ Division of Brain Tumor Translational Research, National Cancer Center Research Institute, 5-1-1 Tsukiji, Chuo-ku, Tokyo, 104-0045, Japan.
⁹ Department of Neurosurgery, Graduate School of Medicine, Yokohama City University, 3-9, Fukuura, Kanazawa-ku, Yokohama, 236-0004, Japan.
¹⁰ Department of Neurosurgery and Neuro-Oncology, National Cancer Center Hospital, 5-1-1 Tsukiji, Chuo-ku, Tokyo, 104-0045, Japan.
¹¹ Department of Pathology, Kyorin University Faculty of Medicine, 6-20-2 Shinkawa, Mitaka, Tokyo, 181-8611, Japan.
¹² Genome Science Division, Research Center for Advanced Science and Technology (RCAST), The University of Tokyo, 4-6-1 Komaba, Meguro-ku, Tokyo, 153-8904, Japan. haburata-tky@umin.ac.jp.

Abstract

Recent studies have demonstrated that tumor-driving alterations are often different among gliomas that originated from different brain regions and have underscored the importance of analyzing molecular characteristics of gliomas stratified by brain region. Therefore, to elucidate molecular characteristics of diffuse cerebellar gliomas (DCGs), 27 adult, mostly glioblastoma cases were analyzed. Comprehensive analysis using whole-exome sequencing, RNA sequencing, and Infinium methylation array (n = 17) demonstrated their distinct molecular profile compared to gliomas in other brain regions. Frequent mutations in chromatin-modifier genes were identified including, noticeably, a truncating mutation in SETD2 (n = 4), which resulted in loss of H3K36 trimethylation and was mutually exclusive with H3F3A K27M mutation (n = 3), suggesting that epigenetic dysregulation may lead to DCG tumorigenesis. Alterations that cause loss of p53 function including TP53 mutation (n = 9), PPM1D mutation (n = 2), and a novel type of PPM1D fusion (n = 1), were also frequent. On the other hand, mutations and copy number changes commonly observed in cerebral gliomas were infrequent. DNA methylation profile analysis demonstrated that all DCGs except for those with H3F3A mutations were categorized in the "RTK I (PDGFRA)" group, and those DCGs had a gene expression signature that was highly associated with PDGFRA. Furthermore, compared with the data of 315 gliomas derived from different brain regions, promoter methylation of transcription factors genes associated with glial development showed a characteristic pattern presumably reflecting their tumor origin. Notably, SOX10, a key transcription factor associated with oligodendroglial differentiation and PDGFRA regulation, was up-regulated in both DCG and H3 K27M-mutant diffuse midline glioma, suggesting their developmental and biological commonality. In contrast, SOX10 was silenced by promoter methylation in most cerebral gliomas. These findings may suggest potential tailored targeted therapy for gliomas according to their brain region, in addition to providing molecular clues to identify the region-related cellular origin of DCGs.

Keywords: Cerebellum; DNA methylation; Gene expression; Genomics; Glioma.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Aged, 80 and over
Cerebellar Neoplasms / genetics*
Cerebellar Neoplasms / metabolism*
Cerebellar Neoplasms / pathology
Cerebellar Neoplasms / surgery
Cerebellum / diagnostic imaging
Cerebellum / metabolism
Cerebellum / pathology
Cerebellum / surgery
Epigenesis, Genetic
Gene Expression Regulation, Neoplastic
Genetic Predisposition to Disease
Glioma / genetics*
Glioma / metabolism*
Glioma / pathology
Glioma / surgery
Humans
Middle Aged