BARD1 is A Low/Moderate Breast Cancer Risk Gene: Evidence Based on An Association Study of the Central European p.Q564X Recurrent Mutation.

Malwina Suszynska,Jan Lubinski,Tadeusz Debniak,Magdalena Ratajska,Natalia Bogdanova,Dominika Wokolorczyk,Anna Jakubowska,Thilo Dörk,Steven Narod,Katarzyna Klonowska,Cezary Cybulski,Marek Szwiec,Wojciech Kluzniak,Piotr Kozlowski,Tomasz Huzarski,Jacek Gronwald

doi:10.3390/cancers11060740

Abstract

In addition to several well-established breast cancer (BC) susceptibility genes, the contribution of other candidate genes to BC risk remains mostly undefined. BARD1 is a potentially predisposing BC gene, however, the rarity of its mutations and an insufficient family/study size have hampered corroboration and estimation of the associated cancer risks. To clarify the role of BARD1 mutations in BC predisposition, a comprehensive case-control association study of a recurring nonsense mutation c.1690C>T (p.Q564X) was performed, comprising ~14,000 unselected BC patients and ~5900 controls from Polish and Belarusian populations. For comparisons, two BARD1 variants of unknown significance were also genotyped. We detected the highest number of BARD1 variants in BC cases in any individual BARD1-specific study, including 38 p.Q564X mutations. The p.Q564X was associated with a moderately increased risk of BC (OR = 2.30, p = 0.04). The estimated risk was even higher for triple-negative BC and bilateral BC. As expected, the two tested variants of unknown significance did not show significant associations with BC risk. Our study provides substantial evidence for the association of a deleterious BARD1 mutation with BC as a low/moderate risk allele. The p.Q564X was shown to be a Central European recurrent mutation with potential relevance for future genetic testing.

Highlights

IntroductionBreast cancer (BC) is the most common cancer diagnosed in women worldwide, with over
Breast cancer (BC) is the most common cancer diagnosed in women worldwide, with over1.5 million new cases diagnosed each year [1]
Our study indicated a likely contribution of BRCA1-associated RING domain 1 (BARD1) mutations to bilateral breast cancer (BC) (OR = 4.85, p = 0.02), which is another indicator of hereditary BC, in addition to triple-negative BC (TNBC)

Summary

Introduction

Breast cancer (BC) is the most common cancer diagnosed in women worldwide, with over. 1.5 million new cases diagnosed each year [1]. Most BCs occur sporadically, potentially as a result of interactions between multiple environmental, lifestyle, hormonal and genetic factors. Approximately 5–10% of BCs present with a familial aggregation due to hereditary mutations in highly penetrant genes. Familial BC frequently co-occurs and shares some genetic background with epithelial ovarian cancer (OC). Other indicators of hereditary BC are younger age of onset, bilateral disease, and triple-negative BC (TNBC). Mutations in high-risk genes, including BRCA1 [2]

Methods

Results

Discussion

Conclusion