Abstract

We will conduct a nested case-control study of women who participated in the Breast Cancer Detection Demonstration Project (BCDDP). All women who underwent breast biopsy revealing benign breast parenchyma during the screening phase of the BCDDP will be eligible for inclusion in the study if they did not have a previous history of breast cancer. All such women who develop breast cancer during subsequent follow-up will be included in the case group for the study. Each case patient will be matched with two control patients. Control patients will be matched to case patients by project center, age, and date of entry biopsy (within 6 months). The entry biopsy of all case and control patients will be assessed using Page's histologic classification scheme. This review will be done independently without knowledge of the patient's subsequent cancer outcome. Dr. Page will discuss the nuances of his classification scheme with the pathologists prior to, but not after, the start of review of study material. Dr. Winfield will classify the mammograms from study subjects at the time of their entry biopsy. These mammograms will be assessed with respect to parenchymal pattern (Wolf's criteria), calcifications, asymmetry, mass density, architectural distortion, and focal duct dilatation. This review will also be conducted without knowledge of the patient's subsequent cancer outcome. 17,012 women underwent benign breast biopsy during the screening phase of the BCDDP. A median follow-up time of 8.75 years is available on these women; 490 developed breast cancer during follow-up. The BCDDP data base includes the patient's date of birth, family history of breast cancer, menstrual history and status, reproductive history, and exogenous female hormone history. We will use conditional logistic regression analysis to assess the individual and combined effects of the histologic, mammographic and non-anatomic risk factors in the study. Our previous research has indicated that 70% of women who undergo benign breast biopsy are not at increased breast cancer risk while 4% of these women have a fivefold increase in the risk of this disease. In this study we will determine whether our previous results can be confirmed in a different population of subjects using different pathologists. If our previous results are corroborated, it will be possible to reassure the majority of patients with benign breast disease that they are not at enhanced cancer risk while identifying a small minority of these patients who need to be followed with great care.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA046492-01
Application #
3189760
Study Section
(SRC)
Project Start
1988-04-01
Project End
1991-03-31
Budget Start
1988-04-01
Budget End
1989-03-31
Support Year
1
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Type
Schools of Medicine
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37203

  Publications

Abbott, Robert G; Forrest, Stephanie; Pienta, Kenneth J (2006) Simulating the hallmarks of cancer. Artif Life 12:617-34
Merajver, S D; Weber, B L; Cody, R et al. (1997) Breast conservation and prolonged chemotherapy for locally advanced breast cancer: the University of Michigan experience. J Clin Oncol 15:2873-81
Dupont, W D; Parl, F F; Hartmann, W H et al. (1993) Breast cancer risk associated with proliferative breast disease and atypical hyperplasia. Cancer 71:1258-65
Page, D L; Kidd Jr, T E; Dupont, W D et al. (1991) Lobular neoplasia of the breast: higher risk for subsequent invasive cancer predicted by more extensive disease. Hum Pathol 22:1232-9
Dupont, W D; Page, D L (1991) Menopausal estrogen replacement therapy and breast cancer. Arch Intern Med 151:67-72
Jensen, R A; Page, D L; Dupont, W D et al. (1989) Invasive breast cancer risk in women with sclerosing adenosis. Cancer 64:1977-83
Dupont, W D (1989) Converting relative risks to absolute risks: a graphical approach. Stat Med 8:641-51