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Literature DB >> 27881822

Lowered H3K27me3 and DNA hypomethylation define poorly prognostic pediatric posterior fossa ependymomas.

Jill Bayliss¹, Piali Mukherjee², Chao Lu³, Siddhant U Jain⁴, Chan Chung¹, Daniel Martinez⁵, Benjamin Sabari³, Ashley S Margol⁶, Pooja Panwalkar¹, Abhijit Parolia^1,7, Melike Pekmezci⁸, Richard C McEachin⁹, Marcin Cieslik^1,7, Benita Tamrazi¹⁰, Benjamin A Garcia¹¹, Gaspare La Rocca¹², Mariarita Santi⁵, Peter W Lewis⁴, Cynthia Hawkins^13,14, Ari Melnick², C David Allis³, Craig B Thompson¹², Arul M Chinnaiyan^1,7, Alexander R Judkins¹⁵, Sriram Venneti¹⁶.

Abstract

Childhood posterior fossa (PF) ependymomas cause substantial morbidity and mortality. These tumors lack recurrent genetic mutations, but a subset of these ependymomas exhibits CpG island (CpGi) hypermethylation [PF group A (PFA)], implicating epigenetic alterations in their pathogenesis. Further, histological grade does not reliably predict prognosis, highlighting the importance of developing more robust prognostic markers. We discovered global H3K27me3 reduction in a subset of these tumors (PF-ve ependymomas) analogous to H3K27M mutant gliomas. PF-ve tumors exhibited many clinical and biological similarities with PFA ependymomas. Genomic H3K27me3 distribution showed an inverse relationship with CpGi methylation, suggesting that CpGi hypermethylation drives low H3K27me3 in PF-ve ependymomas. Despite CpGi hypermethylation and global H3K27me3 reduction, these tumors showed DNA hypomethylation in the rest of the genome and exhibited increased H3K27me3 genomic enrichment at limited genomic loci similar to H3K27M mutant gliomas. Combined integrative analysis of PF-ve ependymomas with H3K27M gliomas uncovered common epigenetic deregulation of select factors that control radial glial biology, and PF radial glia in early human development exhibited reduced H3K27me3. Finally, H3K27me3 immunostaining served as a biomarker of poor prognosis and delineated radiologically invasive tumors, suggesting that reduced H3K27me3 may be a prognostic indicator in PF ependymomas.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：
Histones

Year: 2016 PMID： 27881822 PMCID： PMC5123566 DOI： 10.1126/scitranslmed.aah6904

Source DB: PubMed Journal: Sci Transl Med ISSN： 1946-6234 Impact factor: 17.956

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