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Mutations in BRIP1 confer high risk of ovarian cancer
Authors:Rafnar Thorunn  Gudbjartsson Daniel F  Sulem Patrick  Jonasdottir Aslaug  Sigurdsson Asgeir  Jonasdottir Adalbjorg  Besenbacher Soren  Lundin Pär  Stacey Simon N  Gudmundsson Julius  Magnusson Olafur T  le Roux Louise  Orlygsdottir Gudbjorg  Helgadottir Hafdis T  Johannsdottir Hrefna  Gylfason Arnaldur  Tryggvadottir Laufey  Jonasson Jon G  de Juan Ana  Ortega Eugenia  Ramon-Cajal Jose M  García-Prats Maria D  Mayordomo Carlos  Panadero Angeles  Rivera Fernando  Aben Katja K H  van Altena Anne M  Massuger Leon F A G  Aavikko Mervi  Kujala Paula M  Staff Synnöve  Aaltonen Lauri A  Olafsdottir Kristrun  Bjornsson Johannes
Institution:deCODE genetics, Reykjavik, Iceland. thorunn.rafnar@decode.is
Abstract:Ovarian cancer causes more deaths than any other gynecologic malignancy in developed countries. Sixteen million sequence variants, identified through whole-genome sequencing of 457 Icelanders, were imputed to 41,675 Icelanders genotyped using SNP chips, as well as to their relatives. Sequence variants were tested for association with ovarian cancer (N of affected individuals = 656). We discovered a rare (0.41% allelic frequency) frameshift mutation, c.2040_2041insTT, in the BRIP1 (FANCJ) gene that confers an increase in ovarian cancer risk (odds ratio (OR) = 8.13, P = 2.8 × 10(-14)). The mutation was also associated with increased risk of cancer in general and reduced lifespan by 3.6 years. In a Spanish population, another frameshift mutation in BRIP1, c.1702_1703del, was seen in 2 out of 144 subjects with ovarian cancer and 1 out of 1,780 control subjects (P = 0.016). This allele was also associated with breast cancer (seen in 6/927 cases; P = 0.0079). Ovarian tumors from heterozygous carriers of the Icelandic mutation show loss of the wild-type allele, indicating that BRIP1 behaves like a classical tumor suppressor gene in ovarian cancer.
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