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DA - CIMA - Oncología - Oncología molecular - Artículos de Revista >
Please use this identifier to cite or link to this item:
http://hdl.handle.net/10171/17895
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| Title: | Deletion of chromosome 11q predicts response to anthracycline-based chemotherapy in early breast cancer |
| Author(s) : | Climent, J. (J.)
Dimitrow, P. (P.)
Fridlyand, J. (J.)
Palacios, J. (José)
Siebert, R. (Reiner)
Albertson, D. (Donna G.)
Gray, J.W. (Joe W.)
Pinkel, D. (Daniel)
Lluch, A. (Ana)
Martinez-Climent, J.A. (José Angel) |
| Issue Date: | 2007 |
| Publisher: | American Association for Cancer Research |
| Citation: | Climent J, Dimitrow P, Fridlyand J, Palacios J, Siebert R, Albertson DG, et al. Deletion of chromosome 11q predicts response to anthracycline-based chemotherapy in early breast cancer. Cancer Res 2007 Jan 15;67(2):818-826. |
| Keywords: | Anthracyclines
Breast Neoplasms |
| Abstract: | Despite the recent consensus on the eligibility of adjuvant
systemic therapy in patients with lymph node–negative breast
cancer (NNBC) based on clinicopathologic criteria, specific
biological markers are needed to predict sensitivity to the
different available therapeutic options.W e examined the feasibility
of developing a genomic predictor of chemotherapy
response and recurrence risk in 185 patients with NNBC using
assembled arrays containing 2,460 bacterial artificial chromosome
clones for scanning the genome for DNA copy number
changes.Aft er surgery, 90 patients received anthracyclinebased
chemotherapy, whereas 95 did not.T amoxifen was administered
to patients with hormone receptor–positive tumors.
The association of genomic and clinicopathologic data and
outcome was computed using Cox proportional hazard models
and multiple testing adjustment procedures.Analysis of NNBC
genomes revealed a common genomic signature.Specific DNA
copy number aberrations were associated with hormonal
receptor status, but not with other clinicopathologic variables.
In patients treated with chemotherapy, none of the genomic
changes were significantly correlated with recurrence.In
patients not receiving chemotherapy, deletion of eight bacterial
artificial chromosome clones clustered to chromosome 11q
was independently associated with relapse (disease-free survival
at 10 years F SE, 40% F 14% versus 86% F 6%; P < 0.0001).
The 54 patients with deletion of 11q (29%) did not present more
aggressive clinicopathologic features than those without 11q
loss.The adverse influence of 11q deletion on clinical outcome
was confirmed in an independent validation series of 88
patients with NNBC.Our data suggests that patients with NNBC
with the 11q deletion might benefit from anthracycline-based
chemotherapy despite other clinical, pathologic, or genetic
features.However , these initial findings should be evaluated
in randomized clinical trials. |
| URI: | http://hdl.handle.net/10171/17895 |
| Publisher version (URL): | http://cancerres.aacrjournals.org/content/67/2/818 |
| Appears in Collections: | DA - CIMA - Oncología - Oncología molecular - Artículos de Revista
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