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  4. Comprehensive molecular portraits of human breast tumours.
 
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Titre

Comprehensive molecular portraits of human breast tumours.

Type
article
Institution
Externe
Périodique
Nature  
Contributrices/contributeurs
Koboldt, D.C.
Fulton, R.S.
McLellan, M.D.
Schmidt, H.
Kalicki-Veizer, J.
McMichael, J.F.
Fulton, L.L.
Dooling, D.J.
Ding, L.
Mardis, E.R.
Wilson, R.K.
Ally, A.
Balasundaram, M.
Butterfield, Y.S.
Carlsen, R.
Carter, C.
Chu, A.
Chuah, E.
Chun, H.J.
Coope, R.J.
Dhalla, N.
Guin, R.
Hirst, C.
Hirst, M.
Holt, R.A.
Lee, D.
Li, H.I.
Mayo, M.
Moore, R.A.
Mungall, A.J.
Pleasance, E.
Robertson, A.
Schein, J.E.
Shafiei, A.
Sipahimalani, P.
Slobodan, J.R.
Stoll, D.
Tam, A.
Thiessen, N.
Varhol, R.J.
Wye, N.
Zeng, T.
Zhao, Y.
Birol, I.
Jones, S.J.
Marra, M.A.
Cherniack, A.D.
Saksena, G.
Onofrio, R.C.
Pho, N.H.
Carter, S.L.
Schumacher, S.E.
Tabak, B.
Hernandez, B.
Gentry, J.
Nguyen, H.
Crenshaw, A.
Ardlie, K.
Beroukhim, R.
Winckler, W.
Getz, G.
Gabriel, S.B.
Meyerson, M.
Chin, L.
Park, P.J.
Kucherlapati, R.
Hoadley, K.A.
Auman, J.
Fan, C.
Turman, Y.J.
Shi, Y.
Li, L.
Topal, M.D.
He, X.
Chao, H.H.
Prat, A.
Silva, G.O.
Iglesia, M.D.
Zhao, W.
Usary, J.
Berg, J.S.
Adams, M.
Booker, J.
Wu, J.
Gulabani, A.
Bodenheimer, T.
Hoyle, A.P.
Simons, J.V.
Soloway, M.G.
Mose, L.E.
Jefferys, S.R.
Balu, S.
Parker, J.S.
Hayes, D.
Perou, C.M.
Malik, S.
Mahurkar, S.
Shen, H.
Weisenberger, D.J.
Triche, T.
Lai, P.H.
Bootwalla, M.S.
Maglinte, D.T.
Berman, B.P.
Van Den Berg, D.J.
Baylin, S.B.
Laird, P.W.
Creighton, C.J.
Donehower, L.A.
Getz, G.
Noble, M.
Voet, D.
Saksena, G.
Gehlenborg, N.
DiCara, D.
Zhang, J.
Zhang, H.
Wu, C.J.
Liu, S.Y.
Lawrence, M.S.
Zou, L.
Sivachenko, A.
Lin, P.
Stojanov, P.
Jing, R.
Cho, J.
Sinha, R.
Park, R.W.
Nazaire, M.D.
Robinson, J.
Thorvaldsdottir, H.
Mesirov, J.
Park, P.J.
Chin, L.
Reynolds, S.
Kreisberg, R.B.
Bernard, B.
Bressler, R.
Erkkila, T.
Lin, J.
Thorsson, V.
Zhang, W.
Shmulevich, I.
Ciriello, G.
Weinhold, N.
Schultz, N.
Gao, J.
Cerami, E.
Gross, B.
Jacobsen, A.
Sinha, R.
Aksoy, B.
Antipin, Y.
Reva, B.
Shen, R.
Taylor, B.S.
Ladanyi, M.
Sander, C.
Anur, P.
Spellman, P.T.
Lu, Y.
Liu, W.
Verhaak, R.R.
Mills, G.B.
Akbani, R.
Zhang, N.
Broom, B.M.
Casasent, T.D.
Wakefield, C.
Unruh, A.K.
Baggerly, K.
Coombes, K.
Weinstein, J.N.
Haussler, D.
Benz, C.C.
Stuart, J.M.
Benz, S.C.
Zhu, J.
Szeto, C.C.
Scott, G.K.
Yau, C.
Paull, E.O.
Carlin, D.
Wong, C.
Sokolov, A.
Thusberg, J.
Mooney, S.
Ng, S.
Goldstein, T.C.
Ellrott, K.
Grifford, M.
Wilks, C.
Ma, S.
Craft, B.
Yan, C.
Hu, Y.
Meerzaman, D.
Gastier-Foster, J.M.
Bowen, J.
Ramirez, N.C.
Black, A.D.
Pyatt, R.E.
White, P.
Zmuda, E.J.
Frick, J.
Lichtenberg, T.M.
Brookens, R.
George, M.M.
Gerken, M.A.
Harper, H.A.
Leraas, K.M.
Wise, L.J.
Tabler, T.R.
McAllister, C.
Barr, T.
Hart-Kothari, M.
Tarvin, K.
Saller, C.
Sandusky, G.
Mitchell, C.
Iacocca, M.V.
Brown, J.
Rabeno, B.
Czerwinski, C.
Petrelli, N.
Dolzhansky, O.
Abramov, M.
Voronina, O.
Potapova, O.
Marks, J.R.
Suchorska, W.M.
Murawa, D.
Kycler, W.
Ibbs, M.
Korski, K.
Spychała, A.
Murawa, P.
Brzeziński, J.J.
Perz, H.
Łaźniak, R.
Teresiak, M.
Tatka, H.
Leporowska, E.
Bogusz-Czerniewicz, M.
Malicki, J.
Mackiewicz, A.
Wiznerowicz, M.
Le, X.V.
Kohl, B.
Nguyen, V.T.
Thorp, R.
Nguyen, V.B.
Sussman, H.
Bui, D.P.
Hajek, R.
Nguyen, P.H.
Tran, V.T.
Huynh, Q.T.
Khan, K.Z.
Penny, R.
Mallery, D.
Curley, E.
Shelton, C.
Yena, P.
Ingle, J.N.
Couch, F.J.
Lingle, W.L.
King, T.A.
Gonzalez-Angulo, A.M.
Mills, G.B.
Dyer, M.D.
Liu, S.
Meng, X.
Patangan, M.
Waldman, F.
Stöppler, H.
Rathmell, W.
Thorne, L.
Huang, M.
Boice, L.
Hill, A.
Morrison, C.
Gaudioso, C.
Bshara, W.
Daily, K.
Egea, S.C.
Pegram, M.
Gomez-Fernandez, C.
Dhir, R.
Bhargava, R.
Brufsky, A.
Shriver, C.D.
Hooke, J.A.
Campbell, J.L.
Mural, R.J.
Hu, H.
Somiari, S.
Larson, C.
Deyarmin, B.
Kvecher, L.
Kovatich, A.J.
Ellis, M.J.
King, T.A.
Hu, H.
Couch, F.J.
Mural, R.J.
Stricker, T.
White, K.
Olopade, O.
Ingle, J.N.
Luo, C.
Chen, Y.
Marks, J.R.
Waldman, F.
Wiznerowicz, M.
Bose, R.
Chang, L.W.
Beck, A.H.
Gonzalez-Angulo, A.M.
Pihl, T.
Jensen, M.
Sfeir, R.
Kahn, A.
Chu, A.
Kothiyal, P.
Wang, Z.
Snyder, E.
Pontius, J.
Ayala, B.
Backus, M.
Walton, J.
Baboud, J.
Berton, D.
Nicholls, M.
Srinivasan, D.
Raman, R.
Girshik, S.
Kigonya, P.
Alonso, S.
Sanbhadti, R.
Barletta, S.
Pot, D.
Sheth, M.
Demchok, J.A.
Shaw, K.R.
Yang, L.
Eley, G.
Ferguson, M.L.
Tarnuzzer, R.W.
Zhang, J.
Dillon, L.A.
Buetow, K.
Fielding, P.
Ozenberger, B.A.
Guyer, M.S.
Sofia, H.J.
Palchik, J.D.
Groupes de travail
Cancer Genome Atlas Network
Liens vers les personnes
Ciriello, Giovanni  
ISSN
1476-4687
Statut éditorial
Publié
Date de publication
2012-10-04
Volume
490
Numéro
7418
Première page
61
Dernière page/numéro d’article
70
Peer-reviewed
Oui
Langue
anglais
Notes
Publication types: Journal Article ; Research Support, N.I.H., Extramural ; Research Support, Non-U.S. Gov't ; Research Support, U.S. Gov't, Non-P.H.S.
Publication Status: ppublish
Résumé
We analysed primary breast cancers by genomic DNA copy number arrays, DNA methylation, exome sequencing, messenger RNA arrays, microRNA sequencing and reverse-phase protein arrays. Our ability to integrate information across platforms provided key insights into previously defined gene expression subtypes and demonstrated the existence of four main breast cancer classes when combining data from five platforms, each of which shows significant molecular heterogeneity. Somatic mutations in only three genes (TP53, PIK3CA and GATA3) occurred at >10% incidence across all breast cancers; however, there were numerous subtype-associated and novel gene mutations including the enrichment of specific mutations in GATA3, PIK3CA and MAP3K1 with the luminal A subtype. We identified two novel protein-expression-defined subgroups, possibly produced by stromal/microenvironmental elements, and integrated analyses identified specific signalling pathways dominant in each molecular subtype including a HER2/phosphorylated HER2/EGFR/phosphorylated EGFR signature within the HER2-enriched expression subtype. Comparison of basal-like breast tumours with high-grade serous ovarian tumours showed many molecular commonalities, indicating a related aetiology and similar therapeutic opportunities. The biological finding of the four main breast cancer subtypes caused by different subsets of genetic and epigenetic abnormalities raises the hypothesis that much of the clinically observable plasticity and heterogeneity occurs within, and not across, these major biological subtypes of breast cancer.
Sujets

Breast Neoplasms/clas...

Breast Neoplasms/gene...

Breast Neoplasms/meta...

Breast Neoplasms/path...

Class I Phosphatidyli...

DNA Copy Number Varia...

DNA Methylation

DNA Mutational Analys...

Exome/genetics

Female

GATA3 Transcription F...

Gene Expression Profi...

Gene Expression Regul...

Genes, BRCA1

Genes, Neoplasm/genet...

Genes, erbB-2/genetic...

Genes, p53/genetics

Genetic Heterogeneity...

Genome, Human/genetic...

Genomics

Humans

MAP Kinase Kinase Kin...

MicroRNAs/genetics

Mutation/genetics

Oligonucleotide Array...

Ovarian Neoplasms/gen...

Ovarian Neoplasms/pat...

Phosphatidylinositol ...

Protein Array Analysi...

Proteomics

RNA, Messenger/geneti...

RNA, Neoplasm/genetic...

Receptors, Estrogen/m...

Retinoblastoma Protei...

Retinoblastoma Protei...

PID Serval
serval:BIB_5B5C7C13B539
DOI
10.1038/nature11412
PMID
23000897
WOS
000309446800032
Permalien
https://iris.unil.ch/handle/iris/37554
Open Access
Oui
Date de création
2018-07-06T10:02:45.107Z
Date de création dans IRIS
2025-05-20T13:42:47Z
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