Prediction of Docetaxel Response in Human Breast Cancer by Gene Expression Profiling

Author:

Iwao-Koizumi Kyoko1,Matoba Ryo1,Ueno Noriko1,Kim Seung Jin1,Ando Akiko1,Miyoshi Yasuo1,Maeda Eisaku1,Noguchi Shinzaburo1,Kato Kikuya1

Affiliation:

1. From the Taisho Laboratory of Functional Genomics, Nara Institute of Science and Technology, Nara; Department of Surgical Oncology, Osaka University Medical School, Osaka; and NTT Communication Science Laboratories, Kyoto, Japan

Abstract

Purpose Docetaxel is one of the most effective anticancer drugs available in the treatment of breast cancer. Nearly half of the treated patients, however, do not respond to chemotherapy and suffer from side effects. The ability to reliably predict a patient's response based on tumor gene expression will improve therapeutic decision making and save patients from unnecessary side effects. Patients and Methods A total of 44 breast tumor tissues were sampled by biopsy before treatment with docetaxel, and the response to therapy was clinically evaluated by the degree of reduction in tumor size. Gene expression profiling of the biopsy samples was performed with 2,453 genes using a high-throughput reverse transcriptase polymerase chain reaction technique. Using genes differentially expressed between responders and nonresponders, a diagnostic system based on the weighted-voting algorithm was constructed. Results This system predicted the clinical response of 26 previously unanalyzed samples with over 80% accuracy, a level promising for clinical applications. Diagnostic profiles in nonresponders were characterized by elevated expression of genes controlling the cellular redox environment (ie, redox genes, such as thioredoxin, glutathione-S-transferase, and peroxiredoxin). Overexpression of these genes protected cultured mammary tumor cells from docetaxel-induced cell death, suggesting that enhancement of the redox system plays a major role in docetaxel resistance. Conclusion These results suggest that the clinical response to docetaxel can be predicted by gene expression patterns in biopsy samples. The results also suggest that one of the molecular mechanisms of the resistance is activation of a group of redox genes.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

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