Local recurrence after Breast-Conserving therapy in relation to gene expression patterns in a large series of patients

B. Kreike; H. Halfwerk; N. Armstrong; P. Bult; J.A. Foekens; S.C. Veltkamp; D.S.A. Nuyten; H. Bartelink; M.J. van de Vijver

doi:10.1158/1078-0432.CCR-08-2644

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Local recurrence after Breast-Conserving therapy in relation to gene expression patterns in a large series of patients

Journal article

Peer reviewed

Local recurrence after Breast-Conserving therapy in relation to gene expression patterns in a large series of patients

B. Kreike, H. Halfwerk, N. Armstrong, P. Bult, J.A. Foekens, S.C. Veltkamp, D.S.A. Nuyten, H. Bartelink and M.J. van de Vijver

Clinical Cancer Research, Vol.15(12), pp.4181-4190

2009

DOI: https://doi.org/10.1158/1078-0432.CCR-08-2644

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Abstract

Purpose: The majority of patients with early-stage breast cancer are treated with breast-conserving therapy (BCT). Several clinical risk factors are associated with local recurrence (LR) after BCT but are unable to explain all instances of LR after BCT. Here, gene expression microarrays are used to identify novel risk factors for LR after BCT. Experimental Design: Gene expression profiles of 56 primary invasive breast carcinomas from patients who developed a LR after BCT were compared with profiles of 109 tumors from patients who did not develop a LR after BCT. Both unsupervised and supervised methods of classification were used to separate patients into groups corresponding to disease outcome. In addition, for 15 patients, the gene expression profile in the recurrence was compared with that of the primary tumor. Results: The two main clusters found by hierarchical cluster analysis of all 165 primary invasive breast carcinomas revealed no association with LR. Predefined gene sets (molecular subtypes and “chromosomal instability” signature) are associated with LR (P = 0.0002 and 0.003, respectively). Significant analysis of microarrays revealed an association between LR and cell proliferation, not captured by histologic grading. Class prediction analysis constructed a gene classifier, which was successfully validated, cross-platform, on an independent data set of 161 patients (log-rank P = 0.041). In multivariate analysis, young age was the only independent predictor of LR. Conclusions: We have constructed and cross-platform validated a gene expression profile predictive for LR after BCT, which is characterized by genes involved in cell proliferation but not a surrogate for high histologic grade.

Details

Title: Local recurrence after Breast-Conserving therapy in relation to gene expression patterns in a large series of patients
Authors/Creators: B. Kreike (Author/Creator) - The Netherlands Cancer Institute
H. Halfwerk (Author/Creator)
N. Armstrong (Author/Creator)
P. Bult (Author/Creator)
J.A. Foekens (Author/Creator)
S.C. Veltkamp (Author/Creator)
D.S.A. Nuyten (Author/Creator)
H. Bartelink (Author/Creator)
M.J. van de Vijver (Author/Creator)
Publication Details: Clinical Cancer Research, Vol.15(12), pp.4181-4190
Publisher: American Association for Cancer research
Identifiers: 991005541072907891
Copyright: © 2016 American Association for Cancer Research
Murdoch Affiliation: Murdoch University
Language: English
Resource Type: Journal article

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Collaboration types: Domestic collaboration
Citation topics: 1 Clinical & Life Sciences; 1.119 Breast Cancer Scanning; 1.119.574 Lymphedema
Web Of Science research areas: Oncology
ESI research areas: Clinical Medicine