Proliferation marker securin identifies favourable outcome in invasive ductal breast cancer

被引:0
作者
K Talvinen
J Tuikkala
O Nevalainen
A Rantanen
P Hirsimäki
J Sundström
P Kronqvist
机构
[1] Turku University Hospital,Department of Pathology
[2] University of Turku,Department of Information Technology
[3] University of Turku,Department of Surgical Hospital
[4] Turku University Hospital,undefined
来源
British Journal of Cancer | 2008年 / 99卷
关键词
securin; breast cancer; cDNA microarray; immunohistochemistry; proliferation; prognosis;
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学科分类号
摘要
We introduce a new proliferation marker, securin (pituitary tumour-transforming 1 (PTTG1)), analysed in invasive ductal breast carcinomas by cDNA microarrays and immunohistochemistry. In cDNA microarray of a total of 4000 probes of genes, securin was revealed with a significant change in expression among the several proliferation-related genes studied. The value of securin as a proliferation marker was verified immunohistochemically (n=44) in invasive ductal breast cancer. In follow-up analyses of the sample of patients, the prognostic value of securin was compared with the established markers of breast cancer proliferation, Ki-67 and mitotic activity index (MAI). Our results of a small sample of patients suggest that low securin expression identifies a distinct subgroup of more favourable outcome among patients with high Ki-67 immunoexpression or high MAI. In univariate analysis of Cox's regression, 10-unit increment of securin immunopositivity was associated with a 2.3-fold overall risk of death due to breast cancer and a 7.1-fold risk of death due to breast cancer in the sample of patients stratified according to the cutoff points of 10 and 20% of securin immunopositivity. We suggest that securin immunostaining is a promising and clinically applicable proliferation marker. The finding urges further prognostic studies with a large sample of patients.
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页码:335 / 340
页数:5
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