首页> 外文期刊>Human Genetics >Fine mapping of familial prostate cancer families narrows the interval for a susceptibility locus on chromosome 22q12.3 to 1.36 Mb.
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Fine mapping of familial prostate cancer families narrows the interval for a susceptibility locus on chromosome 22q12.3 to 1.36 Mb.

机译:家族性前列腺癌家族的精细定位将染色体22q12.3上易感基因座的间隔缩短到1.36 Mb。

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Genetic studies suggest that hereditary prostate cancer is a genetically heterogeneous disease with multiple contributing loci. Studies of high-risk prostate cancer families selected for aggressive disease, analysis of large multigenerational families, and a meta-analysis from the International Consortium for Prostate Cancer Genetics (ICPCG), all highlight chromosome 22q12.3 as a susceptibility locus with strong statistical significance. Recently, two publications have narrowed the 22q12.3 locus to a 2.18 Mb interval using 54 high-risk families from the ICPCG collaboration, as defined by three recombination events on either side of the locus. In this paper, we present the results from fine mapping studies at 22q12.3 using both haplotype and recombination data from 42 high-risk families contributed from the Mayo Clinic and the Prostate Cancer Genetic Research Study (PROGRESS) mapping studies. No clear consensus interval is present when all families are used. However, in the subset of 14 families with >/=5 affected men per family, a 2.53-Mb shared consensus segment that overlaps with the previously published interval is identified. Combining these results with data from the earlier ICPCG study reduces the three-recombination interval at 22q12.3 to approximately 1.36 Mb.
机译:遗传研究表明,遗传性前列腺癌是一种遗传异质性疾病,具有多个基因位点。针对侵略性疾病选择的高风险前列腺癌家族的研究,大型多代家族的分析以及国际前列腺癌遗传学协会(ICPCG)的荟萃分析均突出了22q12.3号染色体作为具有重要统计学意义的易感性基因座。最近,有两个出版物使用ICPCG合作的54个高风险家族将22q12.3基因座的范围缩小到2.18 Mb间隔,这是由基因座两侧的三个重组事件定义的。在本文中,我们使用Mayo诊所和前列腺癌基因研究(PROGRESS)作图研究贡献的42个高危家庭的单倍型和重组数据,提供了22q12.3精细作图研究的结果。当使用所有家庭时,没有明确的共识间隔。但是,在14个家庭的子集中,每个家庭受其影响的男性> / = 5,发现一个2.53 Mb的共有共识片段与之前公布的间隔重叠。将这些结果与早期ICPCG研究中的数据相结合,可将22q12.3处的三个重组间隔降低至约1.36 Mb。

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