COsegregation of VARiants in the BRCA1/2 and PALB2 Genes

  • STATUS
    Recruiting
  • End date
    Dec 26, 2027
  • participants needed
    2000
  • sponsor
    Institut Curie
Updated on 26 January 2021
Investigator
Sandrine CAPUTO, PhD
Primary Contact
Centre Eug ne Marquis (0.0 mi away) Contact
+76 other location
cancer
breast cancer
KIT
BRCA1/2
BRCA1
BRCA2
palb2
cancer of the ovary

Summary

The aim of the COVAR project is to classify reliably a maximum of VUS of the French database in order to use them for the genetic counseling. The results obtained through this study will have a major impact on clinical management of the patients and their families conducting in some cases to propose a prophylactic surgery.

Description

The BRCA1 and BRCA2 genes are the two major high-risk breast and/or ovarian cancer susceptibility genes. Monoallelic germline mutations that disrupt their normal gene function significantly increase the risk of developing cancer in carriers. The identification of a causal mutation in a proband allows proposing pre-symptomatic testing for the causal mutation to all at-risk relatives. Currently, a causal mutation, used for genetic counseling, is presented in approximatively 13% of families tested. Variants of unknown biological significance (VUS) are detected in more than 20% of proband tested. For the families of these probands, genetic testing could not be proposed to relatives and the genetic counseling is guided by family history and epidemiological knowledges exclusively.

The French UMD-BRCA1/2 database, accredited by the French National Cancer Institute, collects anonymous results of genetic tests performed by authorized French laboratories since 1995, giving a real-time vision of families carrying the same VUS. In september 2011, the French UMD-BRCA1/2 database comprised 706 different variants in 1,300 BRCA1 families and 1,089 different variants in 2,101 BRCA2 families. One of the key measurable parameters for classification of VUS as causal mutations is their co-segregation with the disease. As the average size of French families is relatively small, the information of variant co-segregation limited to one family would not be significant. However, the compilation of co-segregation results obtained from several families will allow to obtain more precise and complete estimations of the probability of causality of a given variant.

For PALB2, the gene was discovered in 2006. This PALB2 gene has been identified as a predisposition factor to breast cancer by a candidate gene approach. In a first step, the protein encoded by this PALB2 gene (PArtner and Localizer of BRCA2) was identified by a co-immunoprecipitation approach of BRCA2 and its different partners (Foulkes et al., 2007; Rahman et al., 2007). Xia et al., 2006). The association studies showed that monoallelic inactivating variants were more common in women with breast cancer group compared to the control group. A large study of 362 cases in eight countries confirmed the position of PALB2 (Antoniou et al., 2014). The risk of ovarian cancer is likely but not yet proven. This gene has been used for diagnosis in France since July 2015. The data collection is ongoing and the database under construction.

The objective of the COVAR study (COsegregation VARiants) is to organize co-segregation studies of the VUS of the database UMD-BRCA1/2, in order to determine the causal or non-causal nature of these variants. To organize the variants by their clinical relevance, a grid with 5 classes has been used: 1=neutral, 2=likely neutral, 3=VUS, 4=likely causal, 5=causal. The VUS of classes 3 and 4 will be candidates to co-segregation studies because they cannot be used for the genetic counseling.

In the selected families the index case will invite the family members (affected and unaffected) to provide a sample of salivary fluid to test the presence of the VUS. The probability that a VUS is causal will be calculated from the cosegregation data using a Bayesian model. The results will be integrated in the multifactorial model described by D. Goldgar, model integrating different parameters as amino acid conservation, structural impact of the variant, co-occurrence with a pathogenic mutation, family history and tumor characteristics.

Details
Condition Ovarian disorder, Breast Cancer, BRCA1 gene, Ovarian Cancer, BRCA2 gene, Ovarian Function, Genes, PALB2, Recurrent Ovarian Cancer, Genes, PALB2, Genes, PALB2, breast tumors, tumor of the breast, breast tumor, ovarian tumors, Genes, PALB2, Genes, PALB2, Genes, PALB2
Treatment salivary kit
Clinical Study IdentifierNCT01689584
SponsorInstitut Curie
Last Modified on26 January 2021

Eligibility

Yes No Not Sure

Inclusion Criteria

Index cases
A person carrying a BRCA1 or BRCA2 or PALB2 variant class 3 or 4, present and selected in the families of UMD-BRCA1/2 or PALB2 national database of genetic group and cancer (GGC Unicancer) which identifies changes in BRCA1, BRCA2 and PALB2 genes of all French laboratories
Age 18 years
Signed written inform consent "index case
Related parties
Everything related to an index case, diagnosed with breast cancer or ovarian cancer
Any related case of a free index, selected by the investigators, according to family structure and the degree of related compared to the index case
Age 18 years
Signed written inform consent "Related selected

Exclusion Criteria

Minors
Persons deprived of liberty or under guardianship (including curators)
Absence of signed written inform consent
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