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Combining Homologous Recombination and Phosphopeptide-binding Data to Predict the Impact of BRCA1 BRCT Variants on Cancer Risk

Author: Aude Jean-Christophe
Beaudoux Olivia
Bezieau Stephan
Bignon Yves Jean
Bonnet Francoise
Bonte Dorine
Bouazzaoui Isslam
Bourdon Violaine
Boutry-Kryza Nadia
Bressac-de Paillerets Brigitte
Bronner Myriam
Bubien Virginie
Caputo Sandrine M.
Casters Laurent
Caux-Moncoutier Virginie
Coulet Florence
Dardillac Elodie
Delnatte Capucine
Delvincoun Chantal
Dumont Aurelie
Feunteun Jean
Garrec Celine
Golmard Lisa
Guibert Virginie
Guillaud-Bataille Marine
Guillerm Erell
Guirouilh-Barbat Josee
Harmand Pierre-Olivier
Houdayer Claude
Jacquet Eric
Jones Natalie
Jonveaux Philippe
Julien Patrick
Krieger Sophie
Lafitte Philippe
Lefol Cedrick
Leone Melanie
Lidereau Rosette
Lizard Sarab
Longy Michel
Lopez Bernard S.
Muller Daniele
Nhiri Naima
Noguchi Tetsuro
Nogues Catherine
Petitalot Ambre
Pujol Pascal
Remenieras Audrey
Revillion Francoise
Rouleau Etienne
Schnell Jeff A.
Sevenet Nicolas
Sinilnikova Olga
Sobol Hagay
Sokolowska Joanna
Soubrier Florent
Stoppa-Lyonnet Dominique
Toulas Christine
Uhrhammer Nancy
Vaur Dominique
Vilquin Paul
Zinn-Justin Sophie
Publication venue: 'American Association for Cancer Research (AACR)'
Publication date: 01/01/2019
Field of study

WOS:000454834200006International audienceBRCA1 mutations have been identified that increase the risk of developing hereditary breast and ovarian cancers. Genetic screening is now offered to patients with a family history of cancer, to adapt their treatment and the management of their relatives. However, a large number of BRCA1 variants of uncertain significance (VUS) are detected. To better understand the significance of these variants, a high-throughput structural and functional analysis was performed on a large set of BRCA1 VUS. Information on both cellular localization and homology-directed DNA repair (HR) capacity was obtained for 78 BRCT missense variants in the UMD-BRCA1 database and measurement of the structural stability and phosphopeptide-binding capacities was performed for 42 mutated BRCT domains. This extensive and systematic analysis revealed that most characterized causal variants affect BRCT-domain solubility in bacteria and all impair BRCA1 HR activity in cells. Furthermore, binding to a set of 5 different phosphopeptides was tested: all causal variants showed phosphopeptide-binding defects and no neutral variant showed such defects. A classification is presented on the basis of mutated BRCT domain solubility, phosphopeptide-binding properties, and VUS HR capacity. These data suggest that HR-defective variants, which present, in addition, BRCT domains either insoluble in bacteria or defective for phosphopeptide binding, lead to an increased cancer risk. Furthermore, the data suggest that variants with a WT HR activity and whose BRCT domains bind with a WT affinity to the 5 phosphopeptides are neutral. The case of variants with WT HR activity and defective phosphopeptide binding should be further characterized, as this last functional defect might be sufficient per se to lead to tumorigenesis. Implications: The analysis of the current study on BRCA1 structural and functional defects on cancer risk and classification presented may improve clinical interpretation and therapeutic selection

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