Allele Imbalance, or Loss of Heterozygosity, in Normal Breast Epithelium of Sporadic Breast Cancer Cases and BRCA1 Gene Mutation Carriers Is Increased Compared With Reduction Mammoplasty Tissues

Author:

Larson Pamela S.1,Schlechter Benjamin L.1,de las Morenas Antonio1,Garber Judy E.1,Cupples L. Adrienne1,Rosenberg Carol L.1

Affiliation:

1. From the Departments of Pathology and Laboratory Medicine and Medicine, Boston University School of Medicine and Boston Medical Center; Department of Biostatistics, Boston University School of Public Health; and Department of Adult Oncology, Dana-Farber Cancer Institute, Boston, MA

Abstract

Purpose Normal-appearing breast epithelium can contain genetic abnormalities, including allele imbalance (AI), also referred to as loss of heterozygosity. Whether abnormalities are associated with cancer or cancer risk is unknown. Patients and Methods We performed a miniallelotype, using 20 microsatellites, on each of 460 histologically normal, microdissected breast terminal ducto-lobular units (TDLUs) from three groups of women: sporadic breast cancer patients (SP; n = 18), BRCA1 gene mutation carriers (BRCA1; n = 16), and controls undergoing reduction mammoplasty (RM; n = 18). We analyzed the results using Fisher's exact tests, logistic regression, and generalized estimating equations. Results AI was increased three-fold in SP and BRCA1 groups compared with RM. Both the number of TDLUs with AI increased (eight [5%] of 162 in the RM group compared with 24 [15%] of 162 in the SP and 22 [16%] of 136 in the BRCA1 groups; P = .0150), and the proportion of patients with AI increased (five [28%] of 18 in the RM group compared with 15 [83%] of 18 in the SP and 13 [81%] of 16 in the BRCA1 groups; P = .0007). The adjusted odds ratios (OR) for AI in TDLU increased in SP (OR = 15.5) and BRCA1 (OR = 13.7) patients compared with RM (P = .0025). This result was particularly evident on chromosome 17q (P = .0393), where more AI was seen in BRCA1 (OR = 12.4) than in SP (OR = 4.9) patients or RM controls. Conclusion Increased prevalence of AI in normal-appearing epithelium is associated with breast cancer and increased breast cancer risk. The increased prevalence may reflect dysregulation, even in normal-appearing epithelium, of genomic processes contributing to cancer development. The clinical significance of genetic alterations in the subset of controls remains to be determined.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

Reference31 articles.

1. Loss of Heterozygosity in Normal Tissue Adjacent to Breast Carcinomas

2. Loss of heterozygosity as a predictor to map tumor suppressor genes in cancer: molecular basis of its occurrence

3. Kerangueven F, Noguchi T, Coulier F, et al: Genome-wide search for loss of heterozygosity shows extensive genetic diversity of human breast carcinomas. Cancer Res 57: 5469,1997-5474,

4. Loss of Heterozygosity in Normal Tissue Adjacent to Breast Carcinomas

5. Larson PS, de las Morenas A, Cupples LA, et al: Genetically abnormal clones in histologically normal breast tissue. Am J Pathol 152: 1591,1998-1598,

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