Age-specific differences in oncogenic pathway deregulation seen in human breast tumors.

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Anders, Carey K

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Acharya, Chaitanya R

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Hsu, David S

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Broadwater, Gloria

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Garman, Katherine

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Foekens, John A

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Zhang, Yi

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Wang, Yixin

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Marcom, Kelly

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Marks, Jeffrey R

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Mukherjee, Sayan

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Nevins, Joseph R

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Blackwell, Kimberly L

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Potti, Anil

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Wu, Xiaolin

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United States

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2011-06-21T17:31:22Z

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2008-01-02

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PURPOSE: To define the biology driving the aggressive nature of breast cancer arising in young women. EXPERIMENTAL DESIGN: Among 784 patients with early stage breast cancer, using prospectively-defined, age-specific cohorts (young <or=45 years; older >or=65 years), 411 eligible patients (n = 200<or=45 years; n = 211>or=65 years) with clinically-annotated Affymetrix microarray data were identified. GSEA, signatures of oncogenic pathway deregulation and predictors of chemotherapy sensitivity were evaluated within the two age-defined cohorts. RESULTS: In comparing deregulation of oncogenic pathways between age groups, a higher probability of PI3K (p = 0.006) and Myc (p = 0.03) pathway deregulation was observed in breast tumors arising in younger women. When evaluating unique patterns of pathway deregulation, a low probability of Src and E2F deregulation in tumors of younger women, concurrent with a higher probability of PI3K, Myc, and beta-catenin, conferred a worse prognosis (HR = 4.15). In contrast, a higher probability of Src and E2F pathway activation in tumors of older women, with concurrent low probability of PI3K, Myc and beta-catenin deregulation, was associated with poorer outcome (HR = 2.7). In multivariate analyses, genomic clusters of pathway deregulation illustrate prognostic value. CONCLUSION: Results demonstrate that breast cancer arising in young women represents a distinct biologic entity characterized by unique patterns of deregulated signaling pathways that are prognostic, independent of currently available clinico-pathologic variables. These results should enable refinement of targeted treatment strategies in this clinically challenging situation.

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Version of Record

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https://www.ncbi.nlm.nih.gov/pubmed/18167534

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1932-6203

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https://hdl.handle.net/10161/4481

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eng

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en_US

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Public Library of Science (PLoS)

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PLoS One

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10.1371/journal.pone.0001373

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Plos One

dc.subject

Adult

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Age Factors

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Aged

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Breast Neoplasms

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Cohort Studies

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Female

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Humans

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Middle Aged

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Oncogenes

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Age-specific differences in oncogenic pathway deregulation seen in human breast tumors.

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dc.type

Journal article

duke.contributor.orcid

Acharya, Chaitanya R|0000-0001-7149-1749

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Marcom, Kelly|0000-0001-5302-6368

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Marks, Jeffrey R|0000-0002-2054-5468

duke.date.pubdate

2008-1-2

duke.description.issue

1

duke.description.volume

3

pubs.author-url

https://www.ncbi.nlm.nih.gov/pubmed/18167534

pubs.begin-page

e1373

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1

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Clinical Science Departments

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Duke

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Duke Cancer Institute

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Faculty

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Institutes and Centers

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Medicine

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Medicine, Gastroenterology

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Medicine, Medical Oncology

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Pathology

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Radiation Oncology

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School of Medicine

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Surgery

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Surgery, Surgical Sciences

pubs.publication-status

Published online

pubs.volume

3

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