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The Genetic and Molecular Analyses of RAD51C and RAD51D Identifies Rare Variants Implicated in Hereditary Ovarian Cancer from a Genetically Unique Population.

Authors :
Alenezi WM
Milano L
Fierheller CT
Serruya C
Revil T
Oros KK
Behl S
Arcand SL
Nayar P
Spiegelman D
Gravel S
Mes-Masson AM
Provencher D
Foulkes WD
El Haffaf Z
Rouleau G
Bouchard L
Greenwood CMT
Masson JY
Ragoussis J
Tonin PN
Source :
Cancers [Cancers (Basel)] 2022 Apr 30; Vol. 14 (9). Date of Electronic Publication: 2022 Apr 30.
Publication Year :
2022

Abstract

To identify candidate variants in RAD51C and RAD51D ovarian cancer (OC) predisposing genes by investigating French Canadians (FC) exhibiting unique genetic architecture. Candidates were identified by whole exome sequencing analysis of 17 OC families and 53 early-onset OC cases. Carrier frequencies were determined by the genetic analysis of 100 OC or HBOC families, 438 sporadic OC cases and 1025 controls. Variants of unknown function were assayed for their biological impact and/or cellular sensitivity to olaparib. RAD51C c.414G>C;p.Leu138Phe and c.705G>T;p.Lys235Asn and RAD51D c.137C>G;p.Ser46Cys, c.620C>T;p.Ser207Leu and c.694C>T;p.Arg232Ter were identified in 17.6% of families and 11.3% of early-onset cases. The highest carrier frequency was observed in OC families (1/44, 2.3%) and sporadic cases (15/438, 3.4%) harbouring RAD51D c.620C>T versus controls (1/1025, 0.1%). Carriers of c.620C>T (n = 7), c.705G>T (n = 2) and c.137C>G (n = 1) were identified in another 538 FC OC cases. RAD51C c.705G>T affected splicing by skipping exon four, while RAD51D p.Ser46Cys affected protein stability and conferred olaparib sensitivity. Genetic and functional assays implicate RAD51C c.705G>T and RAD51D c.137C>G as likely pathogenic variants in OC. The high carrier frequency of RAD51D c.620C>T in FC OC cases validates previous findings. Our findings further support the role of RAD51C and RAD51D in hereditary OC.

Details

Language :
English
ISSN :
2072-6694
Volume :
14
Issue :
9
Database :
MEDLINE
Journal :
Cancers
Publication Type :
Academic Journal
Accession number :
35565380
Full Text :
https://doi.org/10.3390/cancers14092251