Expression of insulin receptor substrate 1 in primary breast cancer and lymph node metastases

被引:40
|
作者
Koda, M [1 ]
Sulkowska, M [1 ]
Kanczuga-Koda, L [1 ]
Sulkowski, S [1 ]
机构
[1] Med Univ Bialystok, Dept Clin Pathol, PL-15269 Bialystok, Poland
关键词
D O I
10.1136/jcp.2004.022590
中图分类号
R36 [病理学];
学科分类号
100104 ;
摘要
Background: Insulin receptor substrate 1 (IRS-1) transmits signals from the insulin-like growth factor I receptor ( IGF-IR) and insulin receptor (IR) and has been associated with the pathogenesis of cancer. IRS-1 downregulation has been suggested to play a role in breast cancer progression, but no simultaneous assessments of IRS-1 expression in primary breast cancer and metastases have been performed. Aims: To assess IRS-1 expression in primary and metastatic breast cancer. Methods: IRS-1 expression was analysed by means of immunohistochemistry in 109 samples of primary breast cancer and in 42 matched primary and metastatic tumours. In addition, IRS-1 expression was correlated with selected clinicopathological features, including oestrogen receptor alpha (ER alpha) and proliferation marker Ki-67 status. Results: Positive cytoplasmic IRS-1 immunostaining was found in 69.7% ( 76 of 109) and 76.2% ( 32 of 42) of the primary and metastatic tumours, respectively. Both IRS-1 positive and IRS-1 negative primary tumours produced IRS-1 positive and IRS-1 negative metastases. IRS-1 expression in primary tumours correlated with poorly differentiated (G3) breast cancer ( p< 0.005) and with lymph node involvement ( p< 0.05). In the subgroup of ER alpha positive primary tumours, IRS-1 expression positively correlated with Ki-67 ( p< 0.02, r = 0.351), but in the subgroup of ER alpha negative primary tumours there was a negative correlation ( p< 0.03, r = 20.509). IRS-1 expression in lymph node metastases correlated with neither ER alpha nor Ki-67. Conclusions: IRS-1 might be involved in breast cancer progression. Knowledge about differences between primary and metastatic tumours might help to understand mechanisms of breast cancer progression and lead to the development of more effective anticancer drugs.
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页码:645 / 649
页数:5
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