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Haplotype sharing correlation of alcohol dependence on chromosomes 1–6 in 93 nuclear families

机译:93个核心家庭酒精依赖于1-6号染色体的单体型共享相关性

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摘要

Haplotype data contain signatures of ancestral alleles and increased information for mapping genes associated with complex traits. The motivation of this paper is to test the feasibility of a recently developed haplotype reconstruction algorithm and to perform haplotype-sharing correlation (HSC) analysis in nuclear families using data provided by the Genetic Analysis Workshop 14 and the Collaborative Study of the Genetics of Alcoholism. As an exemplary analysis, haplotype data on chromosomes 1–6 were reconstructed from genotype data in 93 nuclear families by minimizing both the recombinants in within-family haplotypes and the tree distance in between-family haplotypes. HSC analysis was performed using the best set of reconstructed haplotypes, and chromosome-wide significance was evaluated using a permutation procedure. Three markers were found to have significant haplotype associations with DSM-IV alcohol dependence that exceeded the 0.05 level of chromosome-wide significance: marker rs895941 at 36.7 cM on chromosome 3 (p = 0.03), marker rs1631833 at 109.1 cM on chromosome 4 (p = 0.008), and marker rs953887 at 74.2 cM on chromosome 6 (p = 0.02). These results indicated the usefulness of HSC analysis and provided further evidence on chromosome regions associated with alcohol dependence.
机译:单倍型数据包含祖先等位基因的特征和用于绘制与复杂性状相关的基因的更多信息。本文的目的是测试遗传算法研讨会14和酒精中毒遗传学合作研究提供的数据,以测试最近开发的单倍型重建算法的可行性,并在核科中进行单倍型共享相关(HSC)分析。作为示例分析,通过最小化家庭内单倍型的重组体和家庭间单倍型的树距,从93个核科的基因型数据重建了1-6号染色体上的单倍型数据。使用最佳的一组重组单倍型进行HSC分析,并使用置换程序评估整个染色体的重要性。发现三个标记物与DSM-IV酒精依赖具有显着的单倍型关联,超过了整个染色体显着性水平的0.05水平:标记rs895941在3号染色体上为36.7 cM(p = 0.03),标记rs1631833在4号染色体上为109.1 cM(p = 0.008),以及在6号染色体上74.2 cM处的标记rs953887(p = 0.02)。这些结果表明HSC分析的有用性,并提供了与酒精依赖相关的染色体区域的进一步证据。

著录项

  • 期刊名称 BMC Genetics
  • 作者

    Dajun Qian;

  • 作者单位
  • 年(卷),期 2005(6),Suppl 1
  • 年度 2005
  • 页码 S79
  • 总页数 4
  • 原文格式 PDF
  • 正文语种
  • 中图分类 遗传学;
  • 关键词

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