High thioredoxin expression is associated with resistance to docetaxel in primary breast cancer

SJ Kim, Y Miyoshi, T Taguchi, Y Tamaki… - Clinical Cancer …, 2005 - AACR
SJ Kim, Y Miyoshi, T Taguchi, Y Tamaki, H Nakamura, J Yodoi, K Kato, S Noguchi
Clinical Cancer Research, 2005AACR
Purpose: Thioredoxin overexpression is suggested to be associated with resistance to
several chemotherapeutic agents in vitro. In the present study, it has been studied whether
or not high thioredoxin expression is associated with resistance to docetaxel therapy in
breast cancer patients. Patients and Methods: Sixty-three primary breast cancer patients
were treated with docetaxel (60 mg/m2, q3w) for four cycles in the neoadjuvant setting.
Expression of thioredoxin, estrogen receptor (ER), p53, BRCA-1, and Bcl-2 in tumor tissues …
Abstract
Purpose: Thioredoxin overexpression is suggested to be associated with resistance to several chemotherapeutic agents in vitro. In the present study, it has been studied whether or not high thioredoxin expression is associated with resistance to docetaxel therapy in breast cancer patients.
Patients and Methods: Sixty-three primary breast cancer patients were treated with docetaxel (60 mg/m2, q3w) for four cycles in the neoadjuvant setting. Expression of thioredoxin, estrogen receptor (ER), p53, BRCA-1, and Bcl-2 in tumor tissues obtained before docetaxel therapy was studied by immunohistochemistry (thioredoxin, p53, BRCA-1, and Bcl-2) and enzyme immunoassay (ER), and relationship of expression of these biomarkers with a pathologic response was investigated.
Results: There was no significant correlation between the expression of p53, BRCA-1, or Bcl-2 and a response to docetaxel. However, tumors with high thioredoxin expression showed a significantly lower response rate (0%) than those with low thioredoxin expression (30.6%; P = 0.018) and ER-negative tumors showed a significantly higher response rate (32.4%) than ER-positive tumors (10.7%; P = 0.043). Thioredoxin expression significantly increased after docetaxel therapy (mean, 56.1%) as compared with that before docetaxel therapy (mean, 28.6%; P < 0.0001) but there was no significant association between the extent of increase in thioredoxin expression and response.
Conclusion: High thioredoxin expression in prechemotherapy tumor samples, but not the increase in thioredoxin expression induced by docetaxel, is associated with resistance to docetaxel in breast cancer. Thioredoxin and ER might be clinically useful in the prediction of a response to docetaxel.
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