Multiple Recurrent Genetic Events Converge on Control of Histone Lysine Methylation in Medulloblastoma

Overview

Journal Nat Genet

Specialty Genetics

Date 2009 Mar 10

PMID 19270706

Citations 229

Authors

Paul A Northcott

Yukiko Nakahara

Xiaochong Wu

Lars Feuk

David W Ellison

Sid Croul

Stephen Mack

Paul N Kongkham

John Peacock

Adrian Dubuc

Young-Shin Ra

Karen Zilberberg

Jessica McLeod

Stephen W Scherer

J Sunil Rao

Charles G Eberhart

Wiesia Grajkowska

Yancey Gillespie

Boleslaw Lach

Richard Grundy

Ian F Pollack

Ronald L Hamilton

Timothy van Meter

Carlos G Carlotti

Frederick Boop

Darrell Bigner

Richard J Gilbertson

James T Rutka

Michael D Taylor

Affiliations

Soon will be listed here.

Abstract

We used high-resolution SNP genotyping to identify regions of genomic gain and loss in the genomes of 212 medulloblastomas, malignant pediatric brain tumors. We found focal amplifications of 15 known oncogenes and focal deletions of 20 known tumor suppressor genes (TSG), most not previously implicated in medulloblastoma. Notably, we identified previously unknown amplifications and homozygous deletions, including recurrent, mutually exclusive, highly focal genetic events in genes targeting histone lysine methylation, particularly that of histone 3, lysine 9 (H3K9). Post-translational modification of histone proteins is critical for regulation of gene expression, can participate in determination of stem cell fates and has been implicated in carcinogenesis. Consistent with our genetic data, restoration of expression of genes controlling H3K9 methylation greatly diminishes proliferation of medulloblastoma in vitro. Copy number aberrations of genes with critical roles in writing, reading, removing and blocking the state of histone lysine methylation, particularly at H3K9, suggest that defective control of the histone code contributes to the pathogenesis of medulloblastoma.

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