Distinct genes related to drug response identified in ER positive and ER negative breast cancer cell lines

A Hershko; A Tabchy; AS Knoop; B Gyorffy; B Wermuth; BM Bolstad; C Liedtke; C Pollard; Chunqiao Tian; CM Perou; Dakun Wang; David A. Gingrich; Elad Katz; F Andre; F Andre; G Rustici; GD Girnun; George Tseng; H Pelicano; H Zembutsu; JG Park; JJ Pink; JK Lee; JS Parker; Kui Shen; M Tanner; Michael J. Gabrin; Nan Song; NR Council; Paul R. Ervin; R Rouzier; R Takata; RM Neve; S Dan; S Paik; SA Marchitti; Shara D. Rice; Stacey L. Brower; T Iwamoto; T Iwamoto; T Sorlie; T Sorlie; TA Jarvinen; U Scherf; V Spataro; VG Tusher; Y Wang; Z Hu; Z Mi; Zhenyu Ding; Zhibao Mi

research

Distinct genes related to drug response identified in ER positive and ER negative breast cancer cell lines

Authors: A Hershko
A Tabchy
AS Knoop
B Gyorffy
B Wermuth
BM Bolstad
C Liedtke
C Pollard
Chunqiao Tian
CM Perou
Dakun Wang
David A. Gingrich
Elad Katz
F Andre
F Andre
G Rustici
GD Girnun
George Tseng
H Pelicano
H Zembutsu
JG Park
JJ Pink
JK Lee
JS Parker
Kui Shen
M Tanner
Michael J. Gabrin
Nan Song
NR Council
Paul R. Ervin
R Rouzier
R Takata
RM Neve
S Dan
S Paik
SA Marchitti
Shara D. Rice
Stacey L. Brower
T Iwamoto
T Iwamoto
T Sorlie
T Sorlie
TA Jarvinen
U Scherf
V Spataro
VG Tusher
Y Wang
Z Hu
Z Mi
Zhenyu Ding
Zhibao Mi
Publication date: 1 January 2012
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

Breast cancer patients have different responses to chemotherapeutic treatments. Genes associated with drug response can provide insight to understand the mechanisms of drug resistance, identify promising therapeutic opportunities, and facilitate personalized treatment. Estrogen receptor (ER) positive and ER negative breast cancer have distinct clinical behavior and molecular properties. However, to date, few studies have rigorously assessed drug response genes in them. In this study, our goal was to systematically identify genes associated with multidrug response in ER positive and ER negative breast cancer cell lines. We tested 27 human breast cell lines for response to seven chemotherapeutic agents (cyclophosphamide, docetaxel, doxorubicin, epirubicin, fluorouracil, gemcitabine, and paclitaxel). We integrated publicly available gene expression profiles of these cell lines with their in vitro drug response patterns, then applied meta-analysis to identify genes related to multidrug response in ER positive and ER negative cells separately. One hundred eighty-eight genes were identified as related to multidrug response in ER positive and 32 genes in ER negative breast cell lines. Of these, only three genes (DBI, TOP2A, and PMVK) were common to both cell types. TOP2A was positively associated with drug response, and DBI was negatively associated with drug response. Interestingly, PMVK was positively associated with drug response in ER positive cells and negatively in ER negative cells. Functional analysis showed that while cell cycle affects drug response in both ER positive and negative cells, most biological processes that are involved in drug response are distinct. A number of signaling pathways that are uniquely enriched in ER positive cells have complex cross talk with ER signaling, while in ER negative cells, enriched pathways are related to metabolic functions. Taken together, our analysis indicates that distinct mechanisms are involved in multidrug response in ER positive and ER negative breast cells. © 2012 Shen et al