Comprehensive molecular portraits of human breast tumours

被引：9403

作者：

Koboldt, Daniel C. ^{[2
]}

Fulton, Robert S. ^{[2
]}

McLellan, Michael D. ^{[2
]}

Schmidt, Heather ^{[2
]}

Kalicki-Veizer, Joelle ^{[2
]}

McMichael, Joshua F. ^{[2
]}

Fulton, Lucinda L. ^{[2
]}

Dooling, David J. ^{[2
]}

Ding, Li ^{[2
,3
]}

Mardis, Elaine R. ^{[2
,3
,4
]}

Wilson, Richard K. ^{[2
,3
,4
]}

Ally, Adrian ^{[5
]}

Balasundaram, Miruna ^{[5
]}

Butterfield, Yaron S. N. ^{[5
]}

Carlsen, Rebecca ^{[5
]}

Carter, Candace ^{[5
]}

Chu, Andy ^{[5
]}

Chuah, Eric ^{[5
]}

Chun, Hye-Jung E. ^{[5
]}

Coope, Robin J. N. ^{[5
]}

Dhalla, Noreen ^{[5
]}

Guin, Ranabir ^{[5
]}

Hirst, Carrie ^{[5
]}

Hirst, Martin ^{[5
]}

Holt, Robert A. ^{[5
]}

Lee, Darlene ^{[5
]}

Li, Haiyan I. ^{[5
]}

Mayo, Michael ^{[5
]}

Moore, Richard A. ^{[5
]}

Mungall, Andrew J. ^{[5
]}

Pleasance, Erin ^{[5
]}

Robertson, A. Gordon ^{[5
]}

Schein, Jacqueline E. ^{[5
]}

Shafiei, Arash ^{[5
]}

Sipahimalani, Payal ^{[5
]}

Slobodan, Jared R. ^{[5
]}

Stoll, Dominik ^{[5
]}

Tam, Angela ^{[5
]}

Thiessen, Nina ^{[5
]}

Varhol, Richard J. ^{[5
]}

Wye, Natasja ^{[5
]}

Zeng, Thomas ^{[5
]}

Zhao, Yongjun ^{[5
]}

Birol, Inanc ^{[5
]}

Jones, Steven J. M. ^{[5
]}

Marra, Marco A. ^{[5
]}

Cherniack, Andrew D. ^{[6
]}

Saksena, Gordon ^{[6
,27
]}

Onofrio, Robert C. ^{[6
]}

Pho, Nam H. ^{[6
]}

机构：

[1] Univ N Carolina, Dept Genet, Chapel Hill, NC 27599 USA

[2] Washington Univ, Genome Inst, St Louis, MO 63108 USA

[3] Washington Univ, Dept Genet, St Louis, MO 63110 USA

[4] Washington Univ, Siteman Canc Ctr, St Louis, MO 63110 USA

[5] BC Canc Agcy, Canadas Michael Smith Genome Sci Ctr, Vancouver, BC V5Z, Canada

[6] Broad Inst MIT & Harvard, Cambridge, MA 02142 USA

[7] Dana Farber Canc Inst, Dept Canc Biol, Boston, MA 02115 USA

[8] Harvard Univ, Sch Med, Dept Med, Boston, MA 02115 USA

[9] Dana Farber Canc Inst, Dept Med Oncol, Boston, MA 02115 USA

[10] Dana Farber Canc Inst, Ctr Canc Genome Discovery, Boston, MA 02115 USA

[11] Harvard Univ, Sch Med, Dept Pathol, Boston, MA 02115 USA

[12] Dana Farber Canc Inst, Belfer Inst Appl Canc Sci, Boston, MA 02115 USA

[13] Harvard Univ, Sch Med, Ctr Biomed Informat, Boston, MA 02115 USA

[14] Harvard Univ, Sch Med, Dept Genet, Boston, MA 02115 USA

[15] Brigham & Womens Hosp, Div Genet, Boston, MA 02115 USA

[16] Univ N Carolina, Lineberger Comprehens Canc Ctr, Chapel Hill, NC 27599 USA

[17] Univ N Carolina, Eshelman Sch Pharm, Chapel Hill, NC 27599 USA

[18] Univ N Carolina, Inst Pharmacogenet & Individualized Therapy, Chapel Hill, NC 27599 USA

[19] Univ N Carolina, Dept Pathol & Lab Med, Chapel Hill, NC 27599 USA

[20] Univ N Carolina, Div Med Oncol, Dept Internal Med, Chapel Hill, NC 27599 USA

[21] Univ So Calif, USC Epigenome Ctr, Los Angeles, CA 90033 USA

[22] Johns Hopkins Univ, Div Canc Biol, Sidney Kimmel Comprehens Canc Ctr, Baltimore, MD 21231 USA

[23] Baylor Coll Med, Dan L Duncan Canc Ctr, Houston, TX 77030 USA

[24] Baylor Coll Med, Human Genome Sequencing Ctr, Houston, TX 77030 USA

[25] Baylor Coll Med, Dept Mol & Cellular Biol, Houston, TX 77030 USA

[26] Baylor Coll Med, Dept Mol Virol & Microbiol, Houston, TX 77030 USA

[27] Eli & Edythe L Broad Inst Massachusetts Inst Tech, Cambridge, MA 02142 USA

[28] Univ Texas MD Anderson Canc Ctr, Dept Genom Med, Inst Appl Canc Sci, Houston, TX 77054 USA

[29] Univ Texas MD Anderson Canc Ctr, Dept Genom Med, Houston, TX 77054 USA

[30] Brigham & Womens Hosp, Div Genet, Boston, MA 02115 USA

[31] Childrens Hosp, Informat Program, Boston, MA 02115 USA

[32] Inst Syst Biol, Seattle, WA 98109 USA

[33] Tampere Univ Technol, FIN-33101 Tampere, Finland

[34] Univ Texas MD Anderson Canc Ctr, Canc Genom Core Lab, Houston, TX 77030 USA

[35] Mem Sloan Kettering Canc Ctr, Computat Biol Ctr, New York, NY 10065 USA

[36] Mem Sloan Kettering Canc Ctr, Dept Epidemiol & Biostat, New York, NY 10065 USA

[37] Mem Sloan Kettering Canc Ctr, Human Oncol & Pathogenesis Program, New York, NY 10065 USA

[38] Oregon Hlth & Sci Univ, Portland, OR 97239 USA

[39] Univ Texas MD Anderson Canc Ctr, Dept Syst Biol, Houston, TX 77030 USA

[40] Univ Texas MD Anderson Canc Ctr, Kleberg Ctr Mol Markers, Houston, TX 77030 USA

[41] Univ Texas MD Anderson Canc Ctr, Dept Bioinformat & Computat Biol, Houston, TX 77030 USA

[42] Univ Calif Santa Cruz, Dept Biomol Engn, Santa Cruz, CA 95064 USA

[43] Univ Calif Santa Cruz, Ctr Biomol Sci & Engn, Santa Cruz, CA 95064 USA

[44] Univ Calif Santa Cruz, Howard Hughes Med Inst, Santa Cruz, CA 95064 USA

[45] Buck Inst Res Aging, Novato, CA 94945 USA

[46] NCI, Ctr Bioinformat & Informat Technol, Rockville, MD 20852 USA

[47] Ohio State Univ, Coll Med, Dept Pathol, Columbus, OH 43205 USA

[48] Ohio State Univ, Coll Med, Dept Pediat, Columbus, OH 43205 USA

[49] Nationwide Childrens Hosp, Res Inst, Columbus, OH 43205 USA

[50] ABS Inc, Indianapolis, IN 46204 USA

来源：

NATURE | 2012年 / 490卷 / 7418期

基金：

美国国家卫生研究院;

关键词：

BASAL-LIKE; MUTATIONAL EVOLUTION; HIGH-FREQUENCY; PIK3CA GENE; LUMINAL-B; CANCER; SUPPRESSOR; SUBTYPES; PATHWAYS; TARGET;

D O I：

10.1038/nature11412

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

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.

引用

页码：61 / 70

页数：10

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