Subgroup-specific structural variation across 1,000 medulloblastoma genomes

Paul A. Northcott; David Shih; John Peacock; Livia Garzia; A. Sorana Morrissy; Thomas Zichner; Adrian M. Stütz; Andrey Korshunov; Jüri Reimand; Steven E. Schumacher; Rameen Beroukhim; David W. Ellison; Christian R. Marshall; Anath C. Lionel; Stephen C. Mack; Adrian M. Dubuc; Yuan Yao; Vijay Ramaswamy; Betty Luu; Adi Rolider; Florence M.G. Cavalli; Xin Wang; Marc Remke; Xiaochong Wu; Readman Chiu; Andy Chu; Eric Chuah; Richard Corbett; Gemma R Hoad; Shaun D. Jackman; Yisu Li; Allan Lo; Karen Mungall; Ka Ming Nip; Jenny Q. Qian; Anthony Raymond; Nina Thiessen; Richard Varhol; İnanç Birol; Richard A. Moore; Andrew J. Mungall; Robert A. Holt; Daisuke Kawauchi; Martine F. Roussel; Marcel Kool; David Jones; Hendrick Witt; Africa Fernández-L; Anna Marie Kenney; Robert J. Wechsler‐Reya; Peter B. Dirks; Tzvi Aviv; Wiesława Grajkowska; Marta Perek‐Polnik; Christine Haberler; Olivier Delattre; Stéphanie Reynaud; François Doz; Sarah S. Pernet-Fattet; Byung-Kyu Cho; Seung‐Ki Kim; Kyu‐Chang Wang; Wolfram Scheurlen; Charles G. Eberhart; Michelle Fèvre‐Montange; Anne Jouvet; Ian F. Pollack; Xing Fan; Karin M. Muraszko; G. Yancey Gillespie; Concezio Di Rocco; Luca Massimi; Erna Michiels; Nanne K. Kloosterhof; Pim J. French; Johan M. Kros; James M. Olson; Richard G. Ellenbogen; Karel Zitterbart; Leoš Křen; Reid C. Thompson; Michael K. Cooper; Bolesław Lach; Roger E. McLendon; Darell D. Bigner; Adam M. Fontebasso; Steffen Albrecht; Nada Jabado; Janet C. Lindsey; Simon Bailey; Nalin Gupta; William A. Weiss; László Bognár; Álmos Klekner; Timothy Van Meter; Toshihiro Kumabe; Teiji Tominaga; Samer K. Elbabaa; Jeffrey R. Leonard; Joshua B. Rubin; Linda M. Liau; Erwin G. Van Meir; Maryam Fouladi; Hideo Nakamura; Giuseppe Cinalli; Miklós Garami; Péter Hauser; Ali G. Saad; Achille Iolascon; Shin Jung; Carlos Gilberto Carlotti; Rajeev Vibhakar; Young Seob Shin; Shenandoah Robinson; Massimo Zollo; Cláudia C. Faria; Jennifer A. Chan; Michael L. Levy; Poul H. Sorensen; Matthew Meyerson; Scott L. Pomeroy; Yoon‐Jae Cho; Gary D. Bader; Uri Tabori; Cynthia Hawkins; Éric Bouffet; Stephen W. Scherer; James T. Rutka; David Malkin; Steven C. Clifford; Steven J.M. Jones; Jan O. Korbel; Stefan M. Pfister; Marco A. Marra; Michael D. Taylor

doi:10.1038/nature11327

Subgroup-specific structural variation across 1,000 medulloblastoma genomes

Paul A. Northcott(Hospital for Sick Children), David Shih(University of Toronto), John Peacock(University of Toronto), Livia Garzia(Hospital for Sick Children), A. Sorana Morrissy(Hospital for Sick Children), Thomas Zichner(European Molecular Biology Laboratory), Adrian M. Stütz(European Molecular Biology Laboratory), Andrey Korshunov(German Cancer Research Center), Jüri Reimand(University of Toronto), Steven E. Schumacher(Dana-Farber Cancer Institute), Rameen Beroukhim(Broad Institute), David W. Ellison(St. Jude Children's Research Hospital), Christian R. Marshall(University of Toronto), Anath C. Lionel(Hospital for Sick Children), Stephen C. Mack(University of Toronto), Adrian M. Dubuc(University of Toronto), Yuan Yao(University of Toronto), Vijay Ramaswamy(University of Toronto), Betty Luu(Hospital for Sick Children), Adi Rolider(Hospital for Sick Children), Florence M.G. Cavalli(Hospital for Sick Children), Xin Wang(University of Toronto), Marc Remke(Hospital for Sick Children), Xiaochong Wu(Hospital for Sick Children), Readman Chiu(BC Cancer Agency), Andy Chu(BC Cancer Agency), Eric Chuah(BC Cancer Agency), Richard Corbett(BC Cancer Agency), Gemma R Hoad(BC Cancer Agency), Shaun D. Jackman(BC Cancer Agency), Yisu Li(BC Cancer Agency), Allan Lo(BC Cancer Agency), Karen Mungall(BC Cancer Agency), Ka Ming Nip(BC Cancer Agency), Jenny Q. Qian(BC Cancer Agency), Anthony Raymond(BC Cancer Agency), Nina Thiessen(BC Cancer Agency), Richard Varhol(BC Cancer Agency), İnanç Birol(BC Cancer Agency), Richard A. Moore(BC Cancer Agency), Andrew J. Mungall(BC Cancer Agency), Robert A. Holt(BC Cancer Agency), Daisuke Kawauchi(St. Jude Children's Research Hospital), Martine F. Roussel(St. Jude Children's Research Hospital), Marcel Kool(German Cancer Research Center), David Jones(German Cancer Research Center), Hendrick Witt(Heidelberg University), Africa Fernández-L(Memorial Sloan Kettering Cancer Center), Anna Marie Kenney(Neurological Surgery), Robert J. Wechsler‐Reya(Sanford Burnham Prebys Medical Discovery Institute), Peter B. Dirks(Hospital for Sick Children), Tzvi Aviv(Hospital for Sick Children), Wiesława Grajkowska(Children's Memorial Health Institute), Marta Perek‐Polnik(Children's Memorial Health Institute), Christine Haberler(Medical University of Vienna), Olivier Delattre(Inserm), Stéphanie Reynaud(Institut Curie), François Doz(Institut Curie), Sarah S. Pernet-Fattet(University Hospital of Lausanne), Byung-Kyu Cho(Seoul National University Children's Hospital), Seung‐Ki Kim(Seoul National University Children's Hospital), Kyu‐Chang Wang(Seoul National University Children's Hospital), Wolfram Scheurlen(Cnopf´sche Kinderklinik), Charles G. Eberhart(Johns Hopkins University), Michelle Fèvre‐Montange(Université Claude Bernard Lyon 1), Anne Jouvet(Université Claude Bernard Lyon 1), Ian F. Pollack(University of Pittsburgh), Xing Fan(University of Michigan), Karin M. Muraszko(University of Michigan), G. Yancey Gillespie(University of Alabama at Birmingham), Concezio Di Rocco(Università Cattolica del Sacro Cuore), Luca Massimi(Università Cattolica del Sacro Cuore), Erna Michiels(Erasmus University Rotterdam), Nanne K. Kloosterhof(Erasmus MC), Pim J. French(Erasmus MC), Johan M. Kros, James M. Olson(Fred Hutch Cancer Center), Richard G. Ellenbogen(University of Washington), Karel Zitterbart(Masaryk University), Leoš Křen(University Hospital Brno), Reid C. Thompson(Neurological Surgery), Michael K. Cooper(Vanderbilt University Medical Center), Bolesław Lach(Hamilton General Hospital), Roger E. McLendon(Duke University), Darell D. Bigner(Duke University), Adam M. Fontebasso(McGill University), Steffen Albrecht(Montreal Children's Hospital), Nada Jabado(McGill University), Janet C. Lindsey(Newcastle University), Simon Bailey(Newcastle University), Nalin Gupta(University of California, San Francisco), William A. Weiss(University of California, San Francisco), László Bognár(University of Debrecen), Álmos Klekner(University of Debrecen), Timothy Van Meter(Virginia Commonwealth University), Toshihiro Kumabe(Tohoku University), Teiji Tominaga(Tohoku University), Samer K. Elbabaa(Saint Louis University), Jeffrey R. Leonard(St. Louis Children's Hospital), Joshua B. Rubin(St. Louis Children's Hospital), Linda M. Liau(University of California, Los Angeles), Erwin G. Van Meir(Emory University), Maryam Fouladi(Cincinnati Children's Hospital Medical Center), Hideo Nakamura(Kumamoto University), Giuseppe Cinalli(Santobono Children's Hospital), Miklós Garami(Semmelweis University), Péter Hauser(Semmelweis University), Ali G. Saad(University of Arkansas for Medical Sciences), Achille Iolascon(Ceinge Biotecnologie Avanzate (Italy)), Shin Jung(Chonnam National University Hwasun Hospital), Carlos Gilberto Carlotti(Universidade de São Paulo), Rajeev Vibhakar(University of Colorado Denver), Young Seob Shin(Asan Medical Center), Shenandoah Robinson(Rainbow Babies & Children's Hospital), Massimo Zollo(Ceinge Biotecnologie Avanzate (Italy)), Cláudia C. Faria(Hospital for Sick Children), Jennifer A. Chan(University of Calgary), Michael L. Levy(Rady Children's Hospital-San Diego), Poul H. Sorensen, Matthew Meyerson(Dana-Farber Cancer Institute), Scott L. Pomeroy(Boston Children's Hospital), Yoon‐Jae Cho(Stanford University), Gary D. Bader(Mount Sinai Hospital), Uri Tabori(Hospital for Sick Children), Cynthia Hawkins(Hospital for Sick Children), Éric Bouffet(Hospital for Sick Children), Stephen W. Scherer(University of Toronto), James T. Rutka(Hospital for Sick Children), David Malkin(University of Toronto), Steven C. Clifford(Newcastle University), Steven J.M. Jones(BC Cancer Agency), Jan O. Korbel(European Molecular Biology Laboratory), Stefan M. Pfister(German Cancer Research Center), Marco A. Marra(BC Cancer Agency), Michael D. Taylor(University of Toronto)

Nature

July 24, 2012

10.1038/nature11327

Cited by 919Open Access

Full Text

Abstract

Medulloblastoma, the most common malignant paediatric brain tumour, is currently treated with nonspecific cytotoxic therapies including surgery, whole-brain radiation, and aggressive chemotherapy. As medulloblastoma exhibits marked intertumoural heterogeneity, with at least four distinct molecular variants, previous attempts to identify targets for therapy have been underpowered because of small samples sizes. Here we report somatic copy number aberrations (SCNAs) in 1,087 unique medulloblastomas. SCNAs are common in medulloblastoma, and are predominantly subgroup-enriched. The most common region of focal copy number gain is a tandem duplication of SNCAIP, a gene associated with Parkinson’s disease, which is exquisitely restricted to Group 4α. Recurrent translocations of PVT1, including PVT1-MYC and PVT1-NDRG1, that arise through chromothripsis are restricted to Group 3. Numerous targetable SCNAs, including recurrent events targeting TGF-β signalling in Group 3, and NF-κB signalling in Group 4, suggest future avenues for rational, targeted therapy. Medulloblastoma is the most common malignant brain tumour in children; having assembled over 1,000 samples the authors report that somatic copy number aberrations are common in medulloblastoma, in particular a tandem duplication of SNCAIP, a gene associated with Parkinson’s disease, which is restricted to subgroup 4α, and translocations of PVT1, which are restricted to Group 3. Medulloblastoma is the most common malignant brain tumour in children. Four papers published in the 2 August 2012 issue of Nature use whole-genome and other sequencing techniques to produce a detailed picture of the genetics and genomics of this condition. Notable findings include the identification of recurrent mutations in genes not previously implicated in medulloblastoma, with significant genetic differences associated with the four biologically distinct subgroups and clinical outcomes in each. Potential avenues for therapy are suggested by the identification of targetable somatic copy-number alterations, including recurrent events targeting TGFβ signalling in Group 3, and NF-κB signalling in Group 4 medulloblastomas.

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