首页> 美国卫生研究院文献>American Journal of Human Genetics >A Unified Stepwise Regression Procedure for Evaluating the Relative Effects of Polymorphisms within a Gene Using Case/Control or Family Data: Application to HLA in Type 1 Diabetes
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A Unified Stepwise Regression Procedure for Evaluating the Relative Effects of Polymorphisms within a Gene Using Case/Control or Family Data: Application to HLA in Type 1 Diabetes

机译:使用病例/对照或家族数据评估基因内多态性相对影响的统一逐步回归程序:在1型糖尿病HLA中的应用

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摘要

A stepwise logistic-regression procedure is proposed for evaluation of the relative importance of variants at different sites within a small genetic region. By fitting statistical models with main effects, rather than modeling the full haplotype effects, we generate tests, with few degrees of freedom, that are likely to be powerful for detecting primary etiological determinants. The approach is applicable to either case/control or nuclear-family data, with case/control data modeled via unconditional and family data via conditional logistic regression. Four different conditioning strategies are proposed for evaluation of effects at multiple, closely linked loci when family data are used. The first strategy results in a likelihood that is equivalent to analysis of a matched case/control study with each affected offspring matched to three pseudocontrols, whereas the second strategy is equivalent to matching each affected offspring with between one and three pseudocontrols. Both of these strategies require parental phase (i.e., those haplotypes present in the parents) to be inferable. Families in which phase cannot be determined must be discarded, which can considerably reduce the effective size of a data set, particularly when large numbers of loci that are not very polymorphic are being considered. Therefore, a third strategy is proposed in which knowledge of parental phase is not required, which allows those families with ambiguous phase to be included in the analysis. The fourth and final strategy is to use conditioning method 2 when parental phase can be inferred and to use conditioning method 3 otherwise. The methods are illustrated using nuclear-family data to evaluate the contribution of loci in the HLA region to the development of type 1 diabetes.
机译:提出了逐步的逻辑回归程序,用于评估小遗传区域内不同位点的变体的相对重要性。通过将统计模型与主要效应进行拟合,而不是对整个单倍型效应进行建模,我们生成了自由度较小的测试,这些测试可能对于检测主要病因是有力的。该方法适用于病例/对照或核家庭数据,病例/对照数据通过无条件建模,而家庭数据通过条件逻辑回归建模。当使用家庭数据时,提出了四种不同的调节策略来评估在多个紧密联系的基因座上的作用。第一种策略产生的可能性等同于对匹配的案例/对照研究的分析,其中每个受影响的后代均与三个假对照匹配,而第二个策略等效于将每个受影响的后代与一个至三个伪对照进行匹配。这两种策略都要求父母阶段(即父母中存在的单倍型)是可推断的。必须丢弃无法确定相位的族,这可能会大大减少数据集的有效大小,尤其是在考虑大量不是非常多态的基因座时。因此,提出了第三种策略,其中不需要父母阶段的知识,这使得那些具有模糊阶段的家庭可以被包括在分析中。第四个也是最后一个策略是在可以推断出父母阶段时使用调节方法2,否则使用调节方法3。使用核心家庭数据说明了这些方法,以评估HLA区域中基因座对1型糖尿病发展的贡献。

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