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Report of Endometrial Cancer in Australian BRCA1 and BRCA2 Mutation-Positive Families

Published online by Cambridge University Press:  21 February 2012

David L. Duffy*
Affiliation:
Genetics and Population Health Division, Queensland Institute of Medical Research, Herston, Queensland, Australia. [email protected]
Yoland C. Antill
Affiliation:
Peter MacCallum Cancer Centre, Melbourne, Australia.
Colin J. Stewart
Affiliation:
PathWest, King Edward Memorial Hospital, Perth, Australia.
Joanne P. Young
Affiliation:
Genetics and Population Health Division, Queensland Institute of Medical Research, Herston, Queensland, Australia.
Amanda B. Spurdle*
Affiliation:
Genetics and Population Health Division, Queensland Institute of Medical Research, Herston, Queensland, Australia. [email protected]
*
*ADDRESS FOR CORRESPONDENCE: Amanda B. Spurdle, Molecular Cancer Epidemiology Laboratory, Genetics and Population Health Division, Queensland Institute of Medical Research, 300 Herston Rd, Herston QLD 4006, Australia.
*ADDRESS FOR CORRESPONDENCE: Amanda B. Spurdle, Molecular Cancer Epidemiology Laboratory, Genetics and Population Health Division, Queensland Institute of Medical Research, 300 Herston Rd, Herston QLD 4006, Australia.

Abstract

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There is evidence that tamoxifen treatment of BRCA1 and BRCA2 carriers for prior breast cancer increases risk of endometrioid subtype endometrial cancer (EC), and suggestive evidence that BRCA1 and BRCA2 mutation carriers may be predisposed to EC in the absence of tamoxifen exposure. We assessed the association of EC with BRCA1 or BRCA2 mutation status in Australasian breast-ovarian families. Report of at least one case of EC was significantly greater in BRCA1-positive families (35/218 (16%); p = .03) and non-significantly greater in BRCA2-positive families (23/189 (12%); p = .6), compared to high-risk breast cancer families without a BRCA1/2 mutation (86/796 (11%)). EC was the first/concurrent cancer for 41% of EC cases with multiple cancer diagnoses from BRCA1/2 families, and early onset for most of these diagnoses. Mutation status was imputed for ungeno-typed individuals from 57 BRCA1/2 pedigrees reporting EC using BRCAPRO. Effects of genotype on EC diagnosis age, and interaction with tamoxifen therapy, were assessed using Cox proportional hazards regression analysis. EC risk was non-significantly marginally greater for BRCA1 carriers (hazard ratio = 1.25, 95%CI = 0.65–2.41), and BRCA2 carriers (HR = 1.12, 95%CI = 0.51–2.45), compared to non-carrier family members. Tamoxifen therapy was highly significantly associated with EC (HR = 6.68, 95%CI = 3.12–15.15; p = 1.7 x 10-6) in BRCA1/2 families, with no evidence for interaction between tamoxifen therapy and BRCA1/2 genotype. Our family-based study supports a 7-fold increase in EC risk with tamoxifen exposure for female family members from BRCA1/2 families. Early onset EC in carriers without tamoxifen use suggests that further study is required to assess association of modest EC risk with BRCA1/2 mutation status alone.

Type
Articles
Copyright
Copyright © Cambridge University Press 2011