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Title: Consistent metagenes from cancer expression profiles yield agent specific predictors of chemotherapy response
Type: Journal articleJournal article
Participant(s):
Author:  Li, Qiyuan (Cwisno: 38074)
Technical University of Denmark

Author:  Eklund, Aron Charles (Cwisno: 40738)
Technical University of Denmark
Email:

Author:  Birkbak, Nicolai Juul (Cwisno: 43582)
Technical University of Denmark
Email:

Forfatter:  Desmedt, Christine
Jules Bordet Institute, Medical Oncology Department

Forfatter:  Haibe-Kains, Benjamin
Dana-Farber Cancer Institute, Boston, Department of Biostatistics

Forfatter:  Sotiriou, Christos
Jules Bordet Institute, Medical Oncology Department

Forfatter:  Symmans, W. Fraser
University of Texas, Department of Pathology

Forfatter:  Pusztai, Lajos
University of Texas, Department of Breast Medical Oncology

Author:  Brunak, Søren (Cwisno: 4734)
Technical University of Denmark
Email:

Forfatter:  Richardson, Andrea L
Brigham and Women’s Hospital, Department of Pathology

Author:  Szallasi, Zoltan Imre (Cwisno: 35725)
Technical University of Denmark
Email:

Abstract: BACKGROUND: Genome scale expression profiling of human tumor samples is likely to yield improved cancer treatment decisions. However, identification of clinically predictive or prognostic classifiers can be challenging when a large number of genes are measured in a small number of tumors. RESULTS: We describe an unsupervised method to extract robust, consistent metagenes from multiple analogous data sets. We applied this method to expression profiles from five "double negative breast cancer" (DNBC) (not expressing ESR1 or HER2) cohorts and derived four metagenes. We assessed these metagenes in four similar but independent cohorts and found strong associations between three of the metagenes and agent-specific response to neoadjuvant therapy. Furthermore, we applied the method to ovarian and early stage lung cancer, two tumor types that lack reliable predictors of outcome, and found that the metagenes yield predictors of survival for both. CONCLUSIONS: These results suggest that the use of multiple data sets to derive potential biomarkers can filter out data set-specific noise and can increase the efficiency in identifying clinically accurate biomarkers.
Published: in journal: B M C Bioinformatics (ISSN: 1471-2105) (DOI: http://dx.doi.org/10.1186/1471-2105-12-310), vol: 12, issue: 1, pages: 310, 2011
DOI:
File(s):
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