Frequency of p53 Mutations in Breast Carcinomas From Ashkenazi Jewish Carriers of BRCA1 Mutations

doi:10.1093/jnci/91.5.469

JNCI Journal of the National Cancer Institute 1999 91(5):469-473; doi:10.1093/jnci/91.5.469
© 1999 by Oxford University Press

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Journal of the National Cancer Institute, Vol. 91, No. 5, 469-473, March 3, 1999
© 1999 Oxford University Press

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Frequency of p53 Mutations in Breast Carcinomas From Ashkenazi Jewish Carriers of BRCA1 Mutations

Kelly-Anne Phillips, Kerrie Nichol, Hilmi Ozcelik, Julia Knight, Susan J. Done, Pamela J. Goodwin, Irene L. Andrulis

Affiliations of authors: K.-A. Phillips, Center for Cancer Genetics and Samuel Lunenfeld Research Institute of Mt. Sinai Hospital, and Department of Medical Oncology and Hematology, Princess Margaret Hospital, Toronto, ON, Canada; K. Nichol, Center for Cancer Genetics and Samuel Lunenfeld Research Institute of Mt. Sinai Hospital; H. Ozcelik, Center for Cancer Genetics and Samuel Lunenfeld Research Institute of Mt. Sinai Hospital, and Department of Laboratory Medicine and Pathobiology, University of Toronto; J. Knight, Division of Preventive Oncology, Cancer Care Ontario; S. J. Done, Samuel Lunenfeld Institute of Mt. Sinai Hospital, and Department of Laboratory Medicine and Pathobiology, University of Toronto; P. J. Goodwin, Samuel Lunenfeld Research Institute of Mt. Sinai Hospital and Marvelle Koffler Breast Center of Mt. Sinai Hospital; I. L. Andrulis, Center for Cancer Genetics and Samuel Lunenfeld Research Institute of Mt. Sinai Hospital, Department of Laboratory Medicine and Pathobiology and Department of Medical and Molecular Genetics, University of Toronto, and Division of Preventive Oncology, Cancer Care Ontario.

Correspondence to: Irene L. Andrulis, Ph.D., Center for Cancer Genetics, Samuel Lunenfeld Research Institute, Mt. Sinai Hospital, 600 University Ave., Toronto, ON M5G 1X5, Canada (e-mail: andrulis{at}mshri.on.ca).

BACKGROUND: Breast carcinomas occurring in carriers of BRCA1gene mutations may have a distinctly different pathway of molecularpathogenesis from those occurring in noncarriers. Data frommurine models implicate loss of p53 (also known as TP53) genefunction as a critical early event in the malignant transformationof cells with a BRCA1 mutation. Therefore, breast tumors fromBRCA1 mutation carriers might be expected to exhibit a high frequencyof p53 mutations. This study examined the frequency of p53 mutationsin the breast tumors of Ashkenazi Jewish carriers and noncarriersof BRCA1 mutations. METHODS: Tumor DNA from carriers and noncarriersof BRCA1 mutations was screened for mutations in exons 4 through10 of the p53 gene by use of the polymerase chain reaction andsingle-strand conformation polymorphism (SSCP) analysis of theamplified DNA. Direct sequencing was performed on gene fragmentsthat showed altered mobility in SSCP analysis. RESULTS: Mutationsin the p53 gene were detected in 10 of 13 tumors from BRCA1mutation carriers versus 10 of 33 tumors from noncarriers (two-sidedP = .007). The p53 mutations were distributed throughout exons4 through 10 and included both protein-truncating and missensemutations in both groups. CONCLUSIONS: A statistically significantly higherfrequency of p53 mutations was found in breast tumors from carriersof BRCA1 mutations than from noncarriers, which adds to theaccumulating evidence that loss of p53 function is an importantstep in the molecular pathogenesis of BRCA1 mutation-associatedbreast tumors. This finding may have implications for understandingphenotypic differences and potential prognostic differencesbetween BRCA1 mutation-associated hereditary breast cancers andsporadic cancers.

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				R. E. Buller, T. A. Lallas, M. S. Shahin, A. K. Sood, M. Hatterman-Zogg, B. Anderson, J. I. Sorosky, and P. A. Kirby The p53 Mutational Spectrum Associated with BRCA1 Mutant Ovarian Cancer Clin. Cancer Res., April 1, 2001; 7(4): 831 - 838. [Abstract] [Full Text]

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				M. Esteller, J. M. Silva, G. Dominguez, F. Bonilla, X. Matias-Guiu, E. Lerma, E. Bussaglia, J. Prat, I. C. Harkes, E. A. Repasky, et al. Promoter Hypermethylation and BRCA1 Inactivation in Sporadic Breast and Ovarian Tumors J Natl Cancer Inst, April 5, 2000; 92(7): 564 - 569. [Abstract] [Full Text] [PDF]

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