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Expression of estrogen receptor beta in the breast carcinoma of BRCA1 mutation carriers

Author: AM Martin
B Górski
BJ Lynch
C Adem
D Stoppa-Lyonnet
Dariusz D Godlewski
DE Porter
DK Gaffney
E Honrado
EM Rosen
F Eisinger
GG Kuiper
Jan Bręborowicz
JM Hall
JN Marcus
JP Struewing
Krzysztof Rożnowski
LC Murphy
LC Verhoog
M de la Hoya
M Esslimani-Sahla
M Krainer
Maria M Litwiniuk
Małgorzata Stawicka
ME Robson
MG Daidone
P O'Neill
P van der Groep
R Wooster
Remigiusz Kaleta
S Fan
S Mosselman
SA Narod
SK Gruvberger-Saal
SR Lakhani
T Barkhem
T Hopp
T Sørlie
T Sørlie
V Speirs
Violetta Filas
WD Faulkes
WD Foulkes
Y Miki
Y Omoto
Publication venue: BioMed Central
Publication date: 01/01/2008
Field of study

Abstract Background Breast cancers (BC) in women carrying mutations in BRCA1 gene are more frequently estrogen receptor negative than the nonhereditary BC. Nevertheless, tamoxifen has been found to have a protective effect in preventing contralateral tumors in BRCA1 mutation carriers. The identification of the second human estrogen receptor, ERβ, raised a question of its role in hereditary breast cancer. The aim of this study was to assess the frequency of ERα, ERβ, PgR (progesterone receptor) and HER-2 expression in breast cancer patients with mutated <it>BRCA1 </it>gene and in the control group. Methods The study group consisted of 48 women with <it>BRCA1 </it>gene mutations confirmed by multiplex PCR assay. The patients were tested for three most common mutations of BRCA1 affecting the Polish population (5382insC, C61G, 4153delA). Immunostaining for ERα, ERβ and PgR (progesterone receptor) was performed using monoclonal antibodies against ERα, PgR (DakoCytomation), and polyclonal antibody against ERβ (Chemicon). The EnVision detection system was applied. The study population comprised a control group of 120 BC operated successively during the years 1998–99. Results The results of our investigation showed that <it>BRCA1 </it>mutation carriers were more likely to have ERα-negative breast cancer than those in the control group. Only 14.5% of <it>BRCA1</it>-related cancers were ERα-positive compared with 57.5% in the control group (<it>P </it>< 0.0001). On the contrary, the expression of ERβ protein was observed in 42% of <it>BRCA1</it>-related tumors and in 55% of the control group. An interesting finding was that most hereditary cancers (75% of the whole group) were triple-negative: ERα(-)/PgR(-)/HER-2(-) but almost half of this group (44.4%) showed the expression of ERβ. Conclusion In the case of <it>BRCA1</it>-associated tumors the expression of ERβ was significantly higher than the expression of ERα. This may explain the effectiveness of tamoxifen in preventing contralateral breast cancer development in <it>BRCA1 </it>mutation carriers.</p

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