Title: Chromosomal instability determines taxane sensitivity - supplementary materials
Authors: Swanton, Charles
Nicke, Barbara
Schuett, Marion
Eklund, Aron C
Ng, Charlotte
Li, Qiyuan
Hardcastle, Thomas
Lee, Alvin
Roy, Rajat
East, Philip
Kschischo, Maik
Endesfelder, David
Wylie, Paul
Kim, Se Nyun
Chen, Jie-Guang
Howell, Michael
Ried, Thomas
Habermann, Jens K
Auer, Gert
Brenton, James D
Szallasi, Zoltan
Downward, Julian
Keywords: chemotherapy
chromosomal instability
drug resistance
taxane
cancer
Issue Date: 24-Apr-2009
Abstract: Microtubule-stabilizing (MTS) agents, such as taxanes, are important chemotherapeutics with a poorly understood mechanism of action. We identified a set of genes repressed in multiple cell lines in response to MTS agents and observed that these genes are overexpressed in tumors exhibiting chromosomal instability (CIN). Silencing 22/50 of these genes, many of which are involved in DNA repair, caused cancer cell death, suggesting that these genes are involved in the survival of aneuploid cells. Overexpression of these ‘‘CIN-survival’’ genes is associated with poor outcome in estrogen receptor–positive breast cancer and occurs frequently in basal-like and Her2-positive cases. In diploid cells, but not in chromosomally unstable cells, paclitaxel causes repression of CIN-survival genes, followed by cell death. In the OV01 ovarian cancer clinical trial, a high level of CIN was associated with taxane resistance but carboplatin sensitivity, indicating that CIN may determine MTS response in vivo. Thus, pretherapeutic assessment of CIN may optimize treatment stratification and clinical trial design using these agents.
URI: http://www.dspace.cam.ac.uk/handle/1810/217842
Appears in Collections:Scholarly works - Oncology

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