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利用结构方程模型联合估计 UK Biobank 中母婴对出生体重的影响。

Using structural equation modelling to jointly estimate maternal and fetal effects on birthweight in the UK Biobank.

机构信息

University of Queensland Diamantina Institute, The University of Queensland, Translational Research Institute, Brisbane, QLD, Australia.

Institute of Biomedical and Clinical Science, University of Exeter Medical School, University of Exeter, Royal Devon and Exeter Hospital, Exeter, UK.

出版信息

Int J Epidemiol. 2018 Aug 1;47(4):1229-1241. doi: 10.1093/ije/dyy015.

Abstract

BACKGROUND

To date, 60 genetic variants have been robustly associated with birthweight. It is unclear whether these associations represent the effect of an individual's own genotype on their birthweight, their mother's genotype, or both.

METHODS

We demonstrate how structural equation modelling (SEM) can be used to estimate both maternal and fetal effects when phenotype information is present for individuals in two generations and genotype information is available on the older individual. We conduct an extensive simulation study to assess the bias, power and type 1 error rates of the SEM and also apply the SEM to birthweight data in the UK Biobank study.

RESULTS

Unlike simple regression models, our approach is unbiased when there is both a maternal and a fetal effect. The method can be used when either the individual's own phenotype or the phenotype of their offspring is not available, and allows the inclusion of summary statistics from additional cohorts where raw data cannot be shared. We show that the type 1 error rate of the method is appropriate, and that there is substantial statistical power to detect a genetic variant that has a moderate effect on the phenotype and reasonable power to detect whether it is a fetal and/or a maternal effect. We also identify a subset of birthweight-associated single nucleotide polymorphisms (SNPs) that have opposing maternal and fetal effects in the UK Biobank.

CONCLUSIONS

Our results show that SEM can be used to estimate parameters that would be difficult to quantify using simple statistical methods alone.

摘要

背景

迄今为止,已有 60 种遗传变异与出生体重显著相关。这些关联是否代表个体自身基因型对其出生体重的影响、其母亲的基因型,还是两者兼而有之,目前尚不清楚。

方法

我们展示了当两代个体存在表型信息且较年长个体存在基因型信息时,结构方程模型(SEM)如何用于估计母体和胎儿效应。我们进行了广泛的模拟研究,以评估 SEM 的偏差、功效和Ⅰ类错误率,并将 SEM 应用于英国生物库研究中的出生体重数据。

结果

与简单回归模型不同,当存在母体和胎儿效应时,我们的方法是无偏的。当个体自身的表型或其后代的表型不可用时,该方法可以使用,并且允许包含无法共享原始数据的其他队列的汇总统计信息。我们表明该方法的Ⅰ类错误率是适当的,并且具有很大的统计功效来检测对表型有中等影响的遗传变异,并且有合理的功效来检测它是否是胎儿和/或母体效应。我们还确定了英国生物库中一组出生体重相关的单核苷酸多态性(SNP),它们具有相反的母体和胎儿效应。

结论

我们的结果表明,SEM 可用于估计仅使用简单统计方法难以量化的参数。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/95d8/6124616/77e80d5f8a00/dyy015f1.jpg

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