학술논문
HER2 mRNA Levels, Estrogen Receptor Activity and Susceptibility to Trastuzumab in Primary Breast Cancer.
Document Type
Article
Author
Source
Subject
*BREAST cancer prognosis
*IN vitro studies
*TRASTUZUMAB
*ONCOGENES
*ESTRADIOL
*CANCER relapse
*ESTROGEN receptors
*GENE expression
*RISK assessment
*MESSENGER RNA
*DISEASE susceptibility
*SURVIVAL analysis (Biometry)
*PROGRESSION-free survival
*TUMOR markers
*CELL lines
*BREAST tumors
*PHARMACODYNAMICS
*DISEASE risk factors
*EVALUATION
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Language
ISSN
2072-6694
Abstract
Simple Summary: HER2 mRNA expression is emerging as a powerful predictive biomarker of anti-HER2 drug activity in the treatment of HER2-positive breast cancer patients. Here, we found a positive association between HER2 mRNA levels and disease-free survival in patients treated with adjuvant trastuzumab. Moreover, we found that while HER2 mRNA expression was correlated with the amount of HER2 protein available on the cell membrane in ER-negative tumors, it was correlated with the low ligand-dependent activity of the estrogen receptor (i.e., addiction to HER2) in ER-positive tumors. While the results thus far demonstrate the clinical benefit of trastuzumab in breast cancer (BC), some patients do not respond to this drug. HER2 mRNA, alone or combined with other genes/biomarkers, has been proven to be a powerful predictive marker in several studies. Here, we provide evidence of the association between HER2 mRNA levels and the response to anti-HER2 treatment in HER2-positive BC patients treated with adjuvant trastuzumab and show that this association is independent of estrogen receptor (ER) tumor positivity. While HER2 mRNA expression was significantly correlated with HER2 protein levels in ER-negative tumors, no correlation was found in ER-positive tumors, and HER2 protein expression was not associated with relapse risk. Correlation analyses in the ER-positive subset identified ER activity as the pathway inversely associated with HER2 mRNA. Associations between HER2 levels and oncogene addiction, as well as between HER2 activation and trastuzumab sensitivity, were also observed in vitro in HER2-positive BC cell lines. In ER-positive but not ER-negative BC cells, HER2 transcription was increased by reducing ligand-dependent ER activity or inducing ER degradation. Accordingly, HER2 mRNA levels in patients were found to be inversely correlated with blood levels of estradiol, the natural ligand of ER that induces ER activation. Moreover, low estradiol levels were associated with a lower risk of relapse in HER2-positive BC patients treated with adjuvant trastuzumab. Overall, we found that HER2 mRNA levels, but not protein levels, indicate the HER2 dependency of tumor cells and low estrogen-dependent ER activity in HER2-positive tumors. [ABSTRACT FROM AUTHOR]