Localization of human BRCA1 and its loss in high-grade, non-inherited breast carcinomas

被引:0
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作者
Cindy A. Wilson
Lillian Ramos
Maria R. Villaseñor
Karl H. Anders
Michael F. Press
Kathy Clarke
Beth Karlan
Jun-Jie Chen
Ralph Scully
David Livingston
Robert H. Zuch
Michael H. Kanter
Sylvan Cohen
Frank J. Calzone
Dennis J. Slamon
机构
[1] UCLA School of Medicine,Department of Medicine, Division of Hematology–Oncology
[2] Southern California Permanente Medical Group,Department of Pathology
[3] Norris Comprehensive Cancer Center,Department of Pathology
[4] University of Southern California,Charles A. Dana Division of Human Cancer Genetics
[5] Dana–Farber Cancer Institute,undefined
[6] Molecular Biology,undefined
[7] Amgen Inc.,undefined
[8] Amgen Center,undefined
来源
Nature Genetics | 1999年 / 21卷
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摘要
Although the link between the BRCA1 tumour–suppressor gene and hereditary breast and ovarian cancer is established1,2,3,4,5, the role, if any, of BRCA1 in non–familial cancers is unclear. BRCA1 mutations are rare in sporadic cancers6,7,8, but loss of BRCA1 resulting from reduced expression or incorrect subcellular localization9,10 is postulated to be important in non–familial breast and ovarian cancers. Epigenetic loss, however, has not received general acceptance due to controversy regarding the subcellular localization of BRCA1 proteins, reports of which have ranged from exclusively nuclear11,12,13,14,15, to conditionally nuclear10, to the ER/golgi16, to cytoplasmic invaginations into the nucleus17. In an attempt to resolve this issue, we have comprehensively characterized 19 anti–BRCA1 antibodies. These reagents detect a 220–kD protein localized in discrete nuclear foci in all epithelial cell lines, including those derived from breast malignancies. Immunohistochemical staining of human breast specimens also revealed BRCA1 nuclear foci in benign breast, invasive lobular cancers and low–grade ductal carcinomas. Conversely, BRCA1 expression was reduced or undetectable in the majority of high–grade, ductal carcinomas, suggesting that absence of BRCA1 may contribute to the pathogenesis of a significant percentage of sporadic breast cancers.
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页码:236 / 240
页数:4
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