Assessment of Rare BRCA1 and BRCA2 Variants of Unknown Significance Using Hierarchical Modeling

Overview

Journal Genet Epidemiol

Specialties Genetics
Public Health

Date 2011 Apr 27

PMID 21520273

Citations 14

Authors

Marinela Capanu

Patrick Concannon

Robert W Haile

Leslie Bernstein

Kathleen E Malone

Charles F Lynch

Xiaolin Liang

Sharon N Teraoka

Anh T Diep

Duncan C Thomas

Jonine L Bernstein

Colin B Begg

Affiliations

Soon will be listed here.

Abstract

Current evidence suggests that the genetic risk of breast cancer may be caused primarily by rare variants. However, while classification of protein-truncating mutations as deleterious is relatively straightforward, distinguishing as deleterious or neutral the large number of rare missense variants is a difficult on-going task. In this article, we present one approach to this problem, hierarchical statistical modeling of data observed in a case-control study of contralateral breast cancer (CBC) in which all the participants were genotyped for variants in BRCA1 and BRCA2. Hierarchical modeling permits leverage of information from observed correlations of characteristics of groups of variants with case-control status to infer with greater precision the risks of individual rare variants. A total of 181 distinct rare missense variants were identified among the 705 cases with CBC and the 1,398 controls with unilateral breast cancer. The model identified three bioinformatic hierarchical covariates, align-GV, align-GD, and SIFT scores, each of which was modestly associated with risk. Collectively, the 11 variants that were classified as adverse on the basis of all the three bioinformatic predictors demonstrated a stronger risk signal. This group included five of six missense variants that were classified as deleterious at the outset by conventional criteria. The remaining six variants can be considered as plausibly deleterious, and deserving of further investigation (BRCA1 R866C; BRCA2 G1529R, D2665G, W2626C, E2663V, and R3052W). Hierarchical modeling is a strategy that has promise for interpreting the evidence from future association studies that involve sequencing of known or suspected cancer genes.

Citing Articles

The Pathogenic R3052W BRCA2 Variant Disrupts Homology-Directed Repair by Failing to Localize to the Nucleus.

Jimenez-Sainz J, Krysztofiak A, Garbarino J, Rogers F, Jensen R Front Genet. 2022; 13:884210.

PMID: 35711920 PMC: 9197106. DOI: 10.3389/fgene.2022.884210.

Integrative analysis of functional genomic annotations and sequencing data to identify rare causal variants via hierarchical modeling.

Capanu M, Ionita-Laza I Front Genet. 2015; 6:17.

PMID: 26005447 PMC: 4424902. DOI: 10.3389/fgene.2015.00176.

New recurrent BRCA1/2 mutations in Polish patients with familial breast/ovarian cancer detected by next generation sequencing.

Kluska A, Balabas A, Paziewska A, Kulecka M, Nowakowska D, Mikula M BMC Med Genomics. 2015; 8:19.

PMID: 25948282 PMC: 4429836. DOI: 10.1186/s12920-015-0092-2.

False discovery rates for rare variants from sequenced data.

Capanu M, Seshan V Genet Epidemiol. 2015; 39(2):65-76.

PMID: 25556339 PMC: 4711769. DOI: 10.1002/gepi.21880.

A powerful and adaptive association test for rare variants.

Pan W, Kim J, Zhang Y, Shen X, Wei P Genetics. 2014; 197(4):1081-95.

PMID: 24831820 PMC: 4125385. DOI: 10.1534/genetics.114.165035.

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