2015
DOI: 10.1007/s10549-015-3459-3
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DNA repair capacity is impaired in healthy BRCA1 heterozygous mutation carriers

Abstract: BRCA1 germline mutations increase the lifetime risk of developing breast and ovarian cancers. However, taking into account the differences in disease manifestation among mutation carriers, it is probable that different BRCA1 mutations have distinct haploinsufficiency effects and lead to the formation of different phenotypes. Using lymphoblastoid cell lines derived from heterozygous BRCA1 mutation carriers and non-carriers, we investigated the haploinsufficiency effects of various mutation types using qPCR, imm… Show more

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Cited by 25 publications
(35 citation statements)
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References 34 publications
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“…Hence, the prevalence of BRCA1‐deficient individuals is currently unknown, but likely greater than that estimated by mutational screening. The reported collective 65% BRCA1 deficiency (Baldeyron et al, ; Vaclova et al, ) likely varies considerably in any given human, but may be greater than the 28–40% decrease in BRCA1 protein in our cKO and KO Brca1 models, suggesting that conceptal variations in BRCA1 levels could be an important determinant of risk for FASD.…”
Section: Dna Repairmentioning
confidence: 71%
See 1 more Smart Citation
“…Hence, the prevalence of BRCA1‐deficient individuals is currently unknown, but likely greater than that estimated by mutational screening. The reported collective 65% BRCA1 deficiency (Baldeyron et al, ; Vaclova et al, ) likely varies considerably in any given human, but may be greater than the 28–40% decrease in BRCA1 protein in our cKO and KO Brca1 models, suggesting that conceptal variations in BRCA1 levels could be an important determinant of risk for FASD.…”
Section: Dna Repairmentioning
confidence: 71%
“…Though limited information is available, a variety of missense and truncating mutations exhibit a collective 65% deficiency in BRCA1 protein levels in human peripheral blood lymphocytes (Baldeyron et al, ; Vaclova et al, ). However, the degree of deficiency depends on the mutation (Baldeyron et al, ; Vaclova et al, ), where some individuals could have biallelic mutations with minimal BRCA1 expression/activity (Domchek et al, ). Most of the missense and truncating mutations in BRCA1 identified to date are commonly associated with breast and ovarian cancers.…”
Section: Dna Repairmentioning
confidence: 99%
“…In the long run, accumulated knowledge about segregation of the genotype and an individual's cancer susceptibility within families may eventually clarify the significance of VUS. At the moment, careful evaluation of DNA repair capacity in lymphocytes from cases with VUS might be useful (Pathania et al 2014, Vaclová et al 2015. It would be particularly useful to construct a collection of isogenic knock-in cells with candidate variants using the CRISPR-CAS9 system (Paquet et al 2016).…”
Section: Discussionmentioning
confidence: 99%
“…However, this reported prevalence only considers BRCA1 mutations related to cancer, and the actual incidence may be higher when considering BRCA1 mutations yet to be identified. Though limited information is available, in humans, a variety of missense and truncating mutations suggest up to a 65% deficiency in BRCA1 protein levels from peripheral blood lymphocytes (Baldeyron et al, ; Vaclova et al, ). This human level of BRCA1 deficiency is considerably greater than the 28‐40% deficiencies in our cKO and KO Brca1 models, suggesting that conceptal variations in BRCA1 levels could be an important determinant of risk for ASD and FASD.…”
Section: Dna Repair and Genetic Predisposition To Asd And Fasdmentioning
confidence: 99%