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Comprehensive Molecular Portraits of Invasive Lobular Breast Cancer.

Title: Comprehensive Molecular Portraits of Invasive Lobular Breast Cancer.
Authors: Ciriello, G.; Gatza, M.L.; Beck, A.H.; Wilkerson, M.D.; Rhie, S.K.; Pastore, A.; Zhang, H.; McLellan, M.; Yau, C.; Kandoth, C.; Bowlby, R.; Shen, H.; Hayat, S.; Fieldhouse, R.; Lester, S.C.; Tse, G.M.; Factor, R.E.; Collins, L.C.; Allison, K.H.; Chen, Y.Y.; Jensen, K.; Johnson, N.B.; Oesterreich, S.; Mills, G.B.; Cherniack, A.D.; Robertson, G.; Benz, C.; Sander, C.; Laird, P.W.; Hoadley, K.A.; King, T.A.; TCGA Research, Network; Perou, C.M.
Contributors: TCGA Research, Network; Akbani, R.; Auman, JT.; Balasundaram, M.; Balu, S.; Barr, T.; Beck, A.; Benz, C.; Benz, S.; Berrios, M.; Beroukhim, R.; Bodenheimer, T.; Boice, L.; Bootwalla, MS.; Bowen, J.; Bowlby, R.; Brooks, D.; Cherniack, AD.; Chin, L.; Cho, J.; Chudamani, S.; Ciriello, G.; Davidsen, T.; Demchok, JA.; Dennison, JB.; Ding, L.; Felau, I.; Ferguson, ML.; Frazer, S.; Gabriel, SB.; Gao, J.; Gastier-Foster, JM.; Gatza, ML.; Gehlenborg, N.; Gerken, M.; Getz, G.; Gibson, WJ.; Hayes, DN.; Heiman, DI.; Hoadley, KA.; Holbrook, A.; Holt, RA.; Hoyle, AP.; Hu, H.; Huang, M.; Hutter, CM.; Hwang, ES.; Jefferys, SR.; Jones, SJ.; Ju, Z.; Kim, J.; Lai, PH.; Laird, PW.; Lawrence, MS.; Leraas, KM.; Lichtenberg, TM.; Lin, P.; Ling, S.; Liu, J.; Liu, W.; Lolla, L.; Lu, Y.; Ma, Y.; Maglinte, DT.; Mardis, E.; Marks, J.; Marra, MA.; McAllister, C.; McLellan, M.; Meng, S.; Meyerson, M.; Mills, GB.; Moore, RA.; Mose, LE.; Mungall, AJ.; Murray, BA.; Naresh, R.; Noble, MS.; Oesterreich, S.; Olopade, O.; Parker, JS.; Perou, CM.; Pihl, T.; Saksena, G.; Schumacher, SE.; Shaw, KR.; Ramirez, NC.; Rathmell, WK.; Rhie, SK.; Roach, J.; Robertson, AG.; Sander, C.; Schein, JE.; Schultz, N.; Shen, H.; Sheth, M.; Shi, Y.; Shih, J.; Shelley, CS.
Publication Year: 2015
Collection: Université de Lausanne (UNIL): Serval - Serveur académique lausannois
Description: Invasive lobular carcinoma (ILC) is the second most prevalent histologic subtype of invasive breast cancer. Here, we comprehensively profiled 817 breast tumors, including 127 ILC, 490 ductal (IDC), and 88 mixed IDC/ILC. Besides E-cadherin loss, the best known ILC genetic hallmark, we identified mutations targeting PTEN, TBX3, and FOXA1 as ILC enriched features. PTEN loss associated with increased AKT phosphorylation, which was highest in ILC among all breast cancer subtypes. Spatially clustered FOXA1 mutations correlated with increased FOXA1 expression and activity. Conversely, GATA3 mutations and high expression characterized luminal A IDC, suggesting differential modulation of ER activity in ILC and IDC. Proliferation and immune-related signatures determined three ILC transcriptional subtypes associated with survival differences. Mixed IDC/ILC cases were molecularly classified as ILC-like and IDC-like revealing no true hybrid features. This multidimensional molecular atlas sheds new light on the genetic bases of ILC and provides potential clinical options.
Document Type: article in journal/newspaper
Language: English
ISSN: 1097-4172
Relation: Cell; https://iris.unil.ch/handle/iris/235211; serval:BIB_E5BACAE80B12; 000362952700023
DOI: 10.1016/j.cell.2015.09.033
Availability: https://iris.unil.ch/handle/iris/235211; https://doi.org/10.1016/j.cell.2015.09.033
Accession Number: edsbas.9854CBA5
Database: BASE