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采用结构方程模型将经典人类白细胞抗原(HLA)位点对出生体重的遗传效应划分为母体和胎儿成分。

Partitioning genetic effects on birthweight at classical human leukocyte antigen loci into maternal and fetal components, using structural equation modelling.

机构信息

Frazer Institute, Faculty of Medicine, University of Queensland, Brisbane, QLD, Australia.

Institute for Molecular Bioscience, University of Queensland, Brisbane, QLD, Australia.

出版信息

Int J Epidemiol. 2024 Feb 1;53(1). doi: 10.1093/ije/dyad142.

Abstract

BACKGROUND

Single nucleotide polymorphisms in the human leukocyte antigen (HLA) region in both maternal and fetal genomes have been robustly associated with birthweight (BW) in previous genetic association studies. However, no study to date has partitioned the association between BW and classical HLA alleles into maternal and fetal components.

METHODS

We used structural equation modelling (SEM) to estimate the maternal and fetal effects of classical HLA alleles on BW. Our SEM leverages the data structure of the UK Biobank (UKB), which includes ∼270 000 participants' own BW and/or the BW of their firstborn child.

RESULTS

We show via simulation that our model yields asymptotically unbiased estimates of the maternal and fetal allelic effects on BW and appropriate type I error rates, in contrast to simple regression models. Asymptotic power calculations show that we have sufficient power to detect moderate-sized maternal or fetal allelic effects of common HLA alleles on BW in the UKB. Applying our SEM to imputed classical HLA alleles and own and offspring BW from the UKB replicated the previously reported association at the HLA-C locus and revealed strong evidence for maternal (HLA-A03:01, B35:01, B39:06, P <0.001) and fetal allelic effects (HLA-B39:06, P <0.001) of non-HLA-C alleles on BW.

CONCLUSIONS

Our model yields asymptotically unbiased estimates, appropriate type I error rates and appreciable power to estimate maternal and fetal effects on BW. These novel allelic associations between BW and classical HLA alleles provide insight into the immunogenetics of fetal growth in utero.

摘要

背景

在先前的遗传关联研究中,人类白细胞抗原(HLA)区域中的单核苷酸多态性与出生体重(BW)之间存在显著关联。然而,迄今为止尚无研究将 BW 与经典 HLA 等位基因之间的关联分解为母体和胎儿成分。

方法

我们使用结构方程模型(SEM)来估计经典 HLA 等位基因对 BW 的母体和胎儿效应。我们的 SEM 利用 UK Biobank(UKB)的数据结构,其中包括约 270000 名参与者自身 BW 或其第一胎的 BW。

结果

通过模拟,我们的模型显示出渐近无偏估计母体和胎儿等位基因对 BW 的影响,以及适当的Ⅰ型错误率,与简单回归模型形成对比。渐近功效计算表明,我们有足够的功效在 UKB 中检测到常见 HLA 等位基因对 BW 的中等大小的母体或胎儿等位基因效应。将我们的 SEM 应用于 UKB 中推断的经典 HLA 等位基因以及自身和后代 BW,复制了 HLA-C 基因座先前报道的关联,并为 BW 上非 HLA-C 等位基因的母体(HLA-A03:01、B35:01、B39:06,P<0.001)和胎儿等位基因效应(HLA-B39:06,P<0.001)提供了强有力的证据。

结论

我们的模型提供了渐近无偏估计、适当的Ⅰ型错误率和可观的估计 BW 上母体和胎儿效应的功效。这些 BW 与经典 HLA 等位基因之间的新等位基因关联为胎儿在子宫内生长的免疫遗传学提供了深入了解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f467/10859143/1447fb43d00b/dyad142f1.jpg

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