Expression of a Truncated Brca1 Protein Delays Lactational Mammary Development in Transgenic Mice

被引:0
|
作者
Melissa A. Brown
Hans Nicolai
Kathy Howe
Toyomasa Katagiri
El-Nasir Lalani
Kaylene J. Simpson
Nathan W. Manning
Andrew Deans
Phil Chen
Kum Kum Khanna
Mas Rina Wati
Beatrice L. Griffiths
Chun-Fang Xu
Gordon W. H. Stamp
Ellen Solomon
机构
[1] King's College London,Cancer Genetics Laboratory, Department of Medical and Molecular Genetics
[2] Imperial Cancer Research Fund,Department of Biochemistry and Molecular Biology
[3] University of Melbourne,Department of Biochemistry and Molecular Biology
[4] University of Queensland,Department of Biochemistry and Molecular Biology
[5] University of Queensland,Department of Histopathology
[6] Imperial College School of Medicine,undefined
[7] Queensland Institute of Medical Research,undefined
来源
Transgenic Research | 2002年 / 11卷
关键词
Brca1; dominant-negative; mammary gland; transgenic mice;
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摘要
To address the hypothesis that certain disease-associated mutants of the breast-ovarian cancer susceptibility gene BRCA1 have biological activity in vivo, we have expressed a truncated Brca1 protein (trBrca1) in cell-lines and in the mammary gland of transgenic mice. Immunofluorescent analysis of transfected cell-lines indicates that trBRCA1 is a stable protein and that it is localized in the cell cytoplasm. Functional analysis of these cell-lines indicates that expression of trBRCA1 confers an increased radiosensitivity phenotype on mammary epithelial cells, consistent with abrogation of the BRCA1 pathway. MMTV-trBrca1 transgenic mice from two independent lines displayed a delay in lactational mammary gland development, as demonstrated by altered histological profiles of lobuloalveolar structures. Cellular and molecular analyses indicate that this phenotype results from a defect in differentiation, rather than altered rates of proliferation or apoptosis. The results presented in this paper are consistent with trBrca1 possessing dominant-negative activity and playing an important role in regulating normal mammary development. They may also have implications for germline carriers of BRCA1 mutations.
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页码:467 / 478
页数:11
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