Molecular classification and biomarkers of clinical outcome in breast ductal carcinoma in situ: Analysis of TBCRC 038 and RAHBT cohorts

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Date
2022-12-12
Authors
Strand, Siri H.
Rivero-Gutiérrez, Belén
Houlahan, Kathleen E.
Seoane, Jose A.
King, Lorraine M.
Risom, Tyler
Simpson, Lunden A.
Vennam, Sujay
Khan, Aziz
Cisneros, Luis
Hardman, Timothy
Harmon, Bryan
Couch, Fergus
Gallagher, Kristalyn
Kilgore, Mark
Wei, Shi
DeMichele, Angela
King, Tari
McAuliffe, Priscilla F.
Nangia, Julie
Lee, Joanna
Tseng, Jennifer
Storniolo, Anna Maria
Thompson, Alastair M.
Gupta, Gaorav P.
Burns, Robyn
Veis, Deborah J.
DeSchryver, Katherine
Zhu, Chunfang
Matusiak, Magdalena
Wang, Jason
Zhu, Shirley X.
Tappenden, Jen
Ding, Daisy Yi
Zhang, Dadong
Luo, Jingqin
Jiang, Shu
Varma, Sushama
Anderson, Lauren
Straub, Cody
Srivastava, Sucheta
Curtis, Christina
Tibshirani , Rob
Angelo, Robert Michael
Hall , Allison
Owzar , Kouros
Polyak , Kornelia
Maley, Carlo
Marks, Jeffrey R.
Colditz, Graham A.
Hwang, E. Shelley
West , Robert B.
Language
American English
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Medicine, School of Medicine
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Elsevier
Abstract

Ductal carcinoma in situ (DCIS) is the most common precursor of invasive breast cancer (IBC), with variable propensity for progression. We perform multiscale, integrated molecular profiling of DCIS with clinical outcomes by analyzing 774 DCIS samples from 542 patients with 7.3 years median follow-up from the Translational Breast Cancer Research Consortium 038 study and the Resource of Archival Breast Tissue cohorts. We identify 812 genes associated with ipsilateral recurrence within 5 years from treatment and develop a classifier that predicts DCIS or IBC recurrence in both cohorts. Pathways associated with recurrence include proliferation, immune response, and metabolism. Distinct stromal expression patterns and immune cell compositions are identified. Our multiscale approach employed in situ methods to generate a spatially resolved atlas of breast precancers, where complementary modalities can be directly compared and correlated with conventional pathology findings, disease states, and clinical outcome.

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Keywords
ductal carcinoma in situ, RNA gene expression profiling, whole genome sequencing, multiplex immunohistochemistry, precancer, tumor microenvironment, classifier, prognosis, progression, breast cancer
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Cite As
Strand, S. H., Rivero-Gutiérrez, B., Houlahan, K. E., Seoane, J. A., King, L. M., Risom, T., Simpson, L. A., Vennam, S., Khan, A., Cisneros, L., Hardman, T., Harmon, B., Couch, F., Gallagher, K., Kilgore, M., Wei, S., DeMichele, A., King, T., McAuliffe, P. F., … West, R. B. (2022). Molecular classification and biomarkers of clinical outcome in breast ductal carcinoma in situ: Analysis of TBCRC 038 and RAHBT cohorts. Cancer Cell, 40(12), 1521-1536.e7. https://doi.org/10.1016/j.ccell.2022.10.021
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Cancer Cell
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https://hdl.handle.net/1805/40197
DOI
https://doi.org/10.1016/j.ccell.2022.10.021
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