Hotspot Mutations in H3F3A and IDH1 Define Distinct Epigenetic and Biological Subgroups of Glioblastoma

dc.contributor.author	Sturm, Dominik
dc.contributor.author	Witt, Hendrik
dc.contributor.author	Hovestadt, Volker
dc.contributor.author	Khuong-Quang, Dong-Anh
dc.contributor.author	Jones, David TW
dc.contributor.author	Carolin, Konermann
dc.contributor.author	Elke, Pfaff
dc.contributor.author	Martje, Tönjes
dc.contributor.author	Martin, Sill
dc.contributor.author	Sebastian, Bender
dc.contributor.author	Marcel, Kool
dc.contributor.author	Marc, Zapatka
dc.contributor.author	Natalia, Becker
dc.contributor.author	Manuela, Zucknick
dc.contributor.author	Thomas, Hielscher
dc.contributor.author	Xiao-Yang, Liu
dc.contributor.author	Adam, M Fontebasso
dc.contributor.author	Marina, Ryzhova
dc.contributor.author	Steffen, Albrecht
dc.contributor.author	Karine, Jacob
dc.contributor.author	Marietta, Wolter
dc.contributor.author	Martin, Ebinger
dc.contributor.author	Martin, U Schuhmann
dc.contributor.author	Timothy, van Meter
dc.contributor.author	Michael, C Frühwald
dc.contributor.author	Holger, Hauch
dc.contributor.author	Arnulf, Pekrun
dc.contributor.author	Bernhard, Radlwimmer
dc.contributor.author	Tim, Niehues
dc.contributor.author	Gregor, von Komorowski
dc.contributor.author	Matthias, Dürken
dc.contributor.author	Andreas, E Kulozik
dc.contributor.author	Jenny, Madden
dc.contributor.author	Andrew, Donson
dc.contributor.author	Nicholas, K Foreman
dc.contributor.author	Rachid, Drissi
dc.contributor.author	Maryam, Fouladi
dc.contributor.author	Wolfram, Scheurlen
dc.contributor.author	Andreas, von Deimling
dc.contributor.author	Camelia, Monoranu
dc.contributor.author	Wolfgang, Roggendorf
dc.contributor.author	Christel, Herold-Mende
dc.contributor.author	Andreas, Unterberg
dc.contributor.author	Christof, M Kramm
dc.contributor.author	Jörg, Felsberg
dc.contributor.author	Christian, Hartmann
dc.contributor.author	Benedikt, Wiestler
dc.contributor.author	Wolfgang, Wick
dc.contributor.author	Till, Milde
dc.contributor.author	Olaf, Witt
dc.contributor.author	Anders, M Lindroth
dc.contributor.author	Jeremy, Schwartzentruber
dc.contributor.author	Damien, Faury
dc.contributor.author	Adam, Fleming
dc.contributor.author	Magdalena, Zakrzewska
dc.contributor.author	Pawel, P Liberski
dc.contributor.author	Krzysztof, Zakrzewski
dc.contributor.author	Hauser, Péter
dc.contributor.author	Garami, Miklós
dc.contributor.author	Klekner, Álmos
dc.contributor.author	Bognár, László
dc.contributor.author	Sorana, Morrissy
dc.contributor.author	Florence, Cavalli
dc.contributor.author	Michael, D Taylor
dc.contributor.author	Peter, van Sluis
dc.contributor.author	Jan, Koste
dc.contributor.author	Rogier, Versteeg
dc.contributor.author	Richard, Volckmann
dc.contributor.author	Tom, Mikkelsen
dc.contributor.author	Kenneth, Aldape
dc.contributor.author	Guido, Reifenberger
dc.contributor.author	V Peter, Collins
dc.contributor.author	Jacek, Majewski
dc.contributor.author	Andrey, Korshunov
dc.contributor.author	Peter, Lichter
dc.contributor.author	Christoph, Plass
dc.contributor.author	Nada, Jabado
dc.contributor.author	Stefan, M Pfister
dc.contributor.author
dc.date.accessioned	2017-01-12T11:06:24Z
dc.date.available	2017-01-12T11:06:24Z
dc.date.issued	2012
dc.identifier	84867606428
dc.identifier.citation	pagination=425-437; journalVolume=22; journalIssueNumber=4; journalTitle=CANCER CELL;
dc.identifier.uri	http://repo.lib.semmelweis.hu//handle/123456789/3901
dc.identifier.uri	doi:10.1016/j.ccr.2012.08.024
dc.description.abstract	Glioblastoma (GBM) is a brain tumor that carries a dismal prognosis and displays considerable heterogeneity. We have recently identified recurrent H3F3A mutations affecting two critical amino acids (K27 and G34) of histone H3.3 in one-third of pediatric GBM. Here, we show that each H3F3A mutation defines an epigenetic subgroup of GBM with a distinct global methylation pattern, and that they are mutually exclusive with IDH1 mutations, which characterize a third mutation-defined subgroup. Three further epigenetic subgroups were enriched for hallmark genetic events of adult GBM and/or established transcriptomic signatures. We also demonstrate that the two H3F3A mutations give rise to GBMs in separate anatomic compartments, with differential regulation of transcription factors OLIG1, OLIG2, and FOXG1, possibly reflecting different cellular origins.
dc.relation.ispartof	urn:issn:1535-6108
dc.title	Hotspot Mutations in H3F3A and IDH1 Define Distinct Epigenetic and Biological Subgroups of Glioblastoma
dc.type	Journal Article
dc.date.updated	2016-12-06T14:36:53Z
dc.language.rfc3066	en
dc.identifier.mtmt	2102584
dc.identifier.wos	000310113900005
dc.identifier.pubmed	23079654
dc.contributor.department	SE/AOK/K/II. Sz. Gyermekgyógyászati Klinika
dc.contributor.institution	Semmelweis Egyetem
dc.mtmt.swordnote	Klekner Álmos: Alulírott Dr. Klekner Álmos nyilatkozom, hogy az alábbi közleményekben szerzőként szerepelek. Minden közlemény tudományos együttműködés keretében született (nem study és nem szponzorált vizsgálat) és mind a mintagyűjtésben, mintafeldolgozásban, mind pedig a közleményekhez szükséges adatfeldolgozásban és elemzésben aktív szerepem volt. Dr. Bognár László nyilatkozom, hogy jelen közlemény létrejöttében szerzőként működtem közre. (2016.05.06.)