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首页> 外文期刊>Human Heredity >Detection of intergenerational genetic effects with application to HLA-B matching as a risk factor for schizophrenia.
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Detection of intergenerational genetic effects with application to HLA-B matching as a risk factor for schizophrenia.

机译:检测代际遗传效应并将其应用于HLA-B匹配作为精神分裂症的危险因素。

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摘要

BACKGROUND AND METHODS: Association studies using unrelated individuals cannot detect intergenerational genetic effects contributing to disease. To detect these effects, we improve the extended maternal-fetal genotype (EMFG) incompatibility test to estimate any combination of maternal effects, offspring effects, and their interactions at polymorphic loci or multiple SNPs, using any size pedigrees. We explore the advantages of using extended pedigrees rather than nuclear families. We apply our methods to schizophrenia pedigrees to investigate whether the previously associated mother-daughter HLA-B matching is a genuine risk or the result of bias. RESULTS: Simulations demonstrate that using the EMFG test with extended pedigrees increases power and precision, while partitioning extended pedigrees into nuclear families can underestimate intergenerational effects. Application to actual data demonstrates that mother-daughter HLA-B matching remains a schizophrenia risk factor. Furthermore, ascertainment and mate selection biases cannot by themselves explain the observed HLA-B matching and schizophrenia association. CONCLUSIONS: Our results demonstrate the power of the EMFG test to examine intergenerational genetic effects, highlight the importance of pedigree rather than case/control or case-mother/control-mother designs, illustrate that pedigrees provide a means to examine alternative, non-causal mechanisms, and they strongly support the hypothesis that HLA-B matching is causally involved in the etiology of schizophrenia in females.
机译:背景与方法:使用无关个体进行的关联研究无法检测出导致疾病的代际遗传效应。为了检测这些影响,我们改进了扩展的母胎基因型(EMFG)不相容性测试,以使用任何大小的谱系估计母体效应,后代效应及其在多态位点或多个SNP处的相互作用的任何组合。我们探索使用扩展谱系而不是核心家庭的优势。我们将我们的方法应用于精神分裂症家系,以调查先前相关的母女HLA-B匹配是否是真正的风险或偏见的结果。结果:仿真表明,使用带有扩展谱系的EMFG测试可提高功能和精度,而将扩展谱系划分为核家族可低估世代效应。应用于实际数据表明,母女HLA-B匹配仍然是精神分裂症的危险因素。此外,确定性和伴侣选择偏倚本身不能解释观察到的HLA-B匹配和精神分裂症的关联。结论:我们的结果证明了EMFG测试具有检验代际遗传效应的能力,突出了血统而不是病例/对照或病例-母亲/对照-母亲设计的重要性,说明了血统书提供了一种检验替代性非因果关系的方法这种机制,并强烈支持HLA-B匹配是女性精神分裂症病因的因果关系这一假说。

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