Article,
ATRT-SHH comprises three molecular subgroups with characteristic clinical and histopathological features and prognostic significance
Contributors
Federico, Antonio
0000-0001-9650-2256
[1]
[2]
[3]
Thomas, Christian
0000-0002-6642-7774
[4]
Kordes, Uwe
0000-0001-6375-2320
[9]
[10]
Hauser, Peter
0000-0002-8307-8975
[13]
Keyvani, Kathy
0000-0003-2558-5159
[14]
van Landeghem, Frank K. H.
0000-0002-9404-7031
[15]
Scheie, David
0000-0002-8692-1198
[16]
[17]
Pietsch, Torsten
0000-0003-0763-6506
[21]
Affiliations
- [1] German Canc Consortium DKTK, Heidelberg, Germany [NORA names: Germany; Europe, EU; OECD];
- [2] German Canc Consortium DKTK, Heidelberg, Germany [NORA names: Germany; Europe, EU; OECD];
- [3] Hopp Childrens Canc Ctr KITZ, Heidelberg, Germany [NORA names: Germany; Europe, EU; OECD];
- [4] Univ Hosp Munster, Inst Neuropathol, Pottkamp 2, D-48149 Munster, Germany [NORA names: Germany; Europe, EU; OECD];
- [5] EU RHAB Registry, Augsburg, Germany [NORA names: Germany; Europe, EU; OECD];
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Abstract
Atypical teratoid/rhabdoid tumor (ATRT) is an aggressive central nervous system tumor characterized by loss of SMARCB1/INI1 protein expression and comprises three distinct molecular groups, ATRT-TYR, ATRT-MYC and ATRT-SHH. ATRT-SHH represents the largest molecular group and is heterogeneous with regard to age, tumor location and epigenetic profile. We, therefore, aimed to investigate if heterogeneity within ATRT-SHH might also have biological and clinical importance. Consensus clustering of DNA methylation profiles and confirmatory t-SNE analysis of 65 ATRT-SHH yielded three robust molecular subgroups, i.e., SHH-1A, SHH-1B and SHH-2. These subgroups differed by median age of onset (SHH-1A: 18 months, SHH-1B: 107 months, SHH-2: 13 months) and tumor location (SHH-1A: 88% supratentorial; SHH-1B: 85% supratentorial; SHH-2: 93% infratentorial, often extending to the pineal region). Subgroups showed comparable SMARCB1 mutational profiles, but pathogenic/likely pathogenic SMARCB1 germline variants were over-represented in SHH-2 (63%) as compared to SHH-1A (20%) and SHH-1B (0%). Protein expression of proneural marker ASCL1 (enriched in SHH-1B) and glial markers OLIG2 and GFAP (absent in SHH-2) as well as global mRNA expression patterns differed, but all subgroups were characterized by overexpression of SHH as well as Notch pathway members. In a Drosophila model, knockdown of Snr1 (the fly homologue of SMARCB1) in hedgehog activated cells not only altered hedgehog signaling, but also caused aberrant Notch signaling and formation of tumor-like structures. Finally, on survival analysis, molecular subgroup and age of onset (but not ASCL1 staining status) were independently associated with overall survival, older patients (> 3 years) harboring SHH-1B experiencing relatively favorable outcome. In conclusion, ATRT-SHH comprises three subgroups characterized by SHH and Notch pathway activation, but divergent molecular and clinical features. Our data suggest that molecular subgrouping of ATRT-SHH has prognostic relevance and might aid to stratify patients within future clinical trials.
