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首页> 外文期刊>International Journal of Legal Medicine >A real-time PCR-based amelogenin Y allele dropout assessment model in gender typing of degraded DNA samples
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A real-time PCR-based amelogenin Y allele dropout assessment model in gender typing of degraded DNA samples

机译:基于实时PCR的降解原DNA性别分型的牙釉蛋白Y等位基因缺失评估模型

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摘要

Allelic dropout due to stochastic variation in degraded small quantity DNA appears to be one of the most serious genotyping errors. Most methods require PCR replication to address this problem. The small amounts of valuable samples are often a limitation for such replications. We report a real-time PCR-based amelogonin Y (AMELY) allele dropout estimation model in an AMEL-based gender typing. We examined 915 replicates of AMELY-positive modern male DNA with varying amounts of DNA and humic acid. A male-specific AMEL fragment (AMELy) dropped out in 143 genuine male replicates, leading to gender typing errors. By graphing a scatter plot of the crossing point versus the end cycle fluorescence of the male replicates, a standard graph model for the estimation of the AMELy allele dropout was constructed with the dropout-prone and dropout-free zones. This model was then applied to ancient DNA (aDNA) samples. Nine samples identified as female were found in the dropout-prone zone; with higher DNA concentrations, six were shifted to the dropout-free zone. Among them, two female identifications were converted to male. All the aDNA gender was confirmed by sex-determination region Y marker amplification. Our data suggest that this model could be a basic approach for securing AMELy allele dropout-safe data from the stochastic variation of degraded inhibitory DNA samples.
机译:由于降解的少量DNA随机变化而导致的等位基因缺失似乎是最严重的基因分型错误之一。大多数方法都需要PCR复制来解决此问题。少量有价值的样品通常是此类复制的限制。我们报告了基于AMEL的性别类型中基于实时PCR的amelogonin Y(AMELY)等位基因缺失估计模型。我们检查了915个AMELY阳性现代雄性DNA的复制品,其中包含不同数量的DNA和腐殖酸。一个男性专用的AMEL片段(AMELy)在143个真正的男性复制品中丢失,导致性别分类错误。通过绘制交点相对于雄性复制品的末端循环荧光的散点图,构建了一个具有掉落倾向区和无掉落区的用于估计AMELy等位基因落差的标准图模型。然后将此模型应用于古代DNA(aDNA)样本。在容易辍学的地区发现了九个被确定为雌性的样品。 DNA浓度较高时,有六个转移到无辍学区。其中,两名女性身份被转换为男性。通过性别决定区域Y标记扩增证实了所有aDNA性别。我们的数据表明,该模型可能是从降解的抑制性DNA样品的随机变异中获取AMELy等位基因脱落安全数据的基本方法。

著录项

  • 来源
    《International Journal of Legal Medicine》 |2013年第1期|55-61|共7页
  • 作者单位

    Institute for Medical Sciences Chung-Ang University">(1);

    Department of Anatomy College of Medicine and Medical School Chung-Ang University">(3);

    Department of Microbiology College of Medicine and Medical School Chung-Ang University">(2);

    Department of Microbiology College of Medicine and Medical School Chung-Ang University">(2);

    Institute for Medical Sciences Chung-Ang University">(1);

    Department of Laboratory Medicine College of Medicine and Medical School Chung-Ang University">(4);

    Institute for Medical Sciences Chung-Ang University">(1);

    Department of Physiology College of Medicine and Medical School Chung-Ang University">(5);

    Department of Anatomy College of Medicine and Medical School Chung-Ang University">(3);

    The Hun School of Princeton">(7);

    Department of Life Science College of Natural Science Chung-Ang University">(6);

    Department of Microbiology College of Medicine Seoul National University">(8);

    Department of Microbiology College of Medicine and Medical School Chung-Ang University">(10);

    Institute for Medical Sciences College of Medicine and Medical School Chung-Ang University">(9);

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    AMELY allele dropout; Ancient bone; Real-time PCR; Melting curve analysis; Amelogenin;

    机译:等位基因缺失;古骨实时PCR;熔解曲线分析;褪黑激素;

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