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Exome Sequencing Identifies Rare Deleterious Mutations in DNA Repair Genes FANCC and BLM as Potential Breast Cancer Susceptibility Alleles
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نویسنده
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thompson e.r. ,doyle m.a. ,ryland g.l. ,rowley s.m. ,choong d.y.h. ,tothill r.w. ,thorne h. ,barnes d.r. ,li j. ,ellul j. ,philip g.k. ,antill y.c. ,james p.a. ,trainer a.h. ,mitchell g. ,campbell i.g.
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منبع
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plos genetics - 2012 - دوره : 8 - شماره : 9
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چکیده
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Despite intensive efforts using linkage and candidate gene approaches,the genetic etiology for the majority of families with a multi-generational breast cancer predisposition is unknown. in this study,we used whole-exome sequencing of thirty-three individuals from 15 breast cancer families to identify potential predisposing genes. our analysis identified families with heterozygous,deleterious mutations in the dna repair genes fancc and blm,which are responsible for the autosomal recessive disorders fanconi anemia and bloom syndrome. in total,screening of all exons in these genes in 438 breast cancer families identified three with truncating mutations in fancc and two with truncating mutations in blm. additional screening of fancc mutation hotspot exons identified one pathogenic mutation among an additional 957 breast cancer families. importantly,none of the deleterious mutations were identified among 464 healthy controls and are not reported in the 1,000 genomes data. given the rarity of fanconi anemia and bloom syndrome disorders among caucasian populations,the finding of multiple deleterious mutations in these critical dna repair genes among high-risk breast cancer families is intriguing and suggestive of a predisposing role. our data demonstrate the utility of intra-family exome-sequencing approaches to uncover cancer predisposition genes,but highlight the major challenge of definitively validating candidates where the incidence of sporadic disease is high,germline mutations are not fully penetrant,and individual predisposition genes may only account for a tiny proportion of breast cancer families. © 2012 thompson et al.
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آدرس
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victorian breast cancer research consortium cancer genetics laboratory,peter maccallum cancer centre,east melbourne,vic, Australia, bioinformatics core facility,peter maccallum cancer centre,east melbourne,vic, Australia, victorian breast cancer research consortium cancer genetics laboratory,peter maccallum cancer centre,east melbourne,vic,australia,centre for cancer research,monash institute of medical research,monash university,clayton,vic, Australia, victorian breast cancer research consortium cancer genetics laboratory,peter maccallum cancer centre,east melbourne,vic, Australia, victorian breast cancer research consortium cancer genetics laboratory,peter maccallum cancer centre,east melbourne,vic, Australia, molecular genomics core facility,peter maccallum cancer centre,east melbourne,vic, Australia, kathleen cunningham foundation consortium for research into familial breast cancer (kconfab),peter maccallum cancer centre,east melbourne,vic, Australia, centre for cancer genetic epidemiology,department of public health and primary care,university of cambridge,cambridge, United Kingdom, bioinformatics core facility,peter maccallum cancer centre,east melbourne,vic, Australia, bioinformatics core facility,peter maccallum cancer centre,east melbourne,vic, Australia, life sciences computation centre,victorian life sciences computation initiative,carlton,vic, Australia, victorian breast cancer research consortium cancer genetics laboratory,peter maccallum cancer centre,east melbourne,vic, Australia, familial cancer centre,peter maccallum cancer centre,east melbourne,vic,australia,sir peter maccallum department of oncology,university of melbourne,parkville,vic, Australia, victorian breast cancer research consortium cancer genetics laboratory,peter maccallum cancer centre,east melbourne,vic,australia,familial cancer centre,peter maccallum cancer centre,east melbourne,vic, Australia, familial cancer centre,peter maccallum cancer centre,east melbourne,vic,australia,sir peter maccallum department of oncology,university of melbourne,parkville,vic, Australia, victorian breast cancer research consortium cancer genetics laboratory,peter maccallum cancer centre,east melbourne,vic,australia,sir peter maccallum department of oncology,university of melbourne,parkville,vic,australia,department of pathology,university of melbourne,parkville,vic, Australia
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Authors
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