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区分人类群体中的直接、间接和源自亲代的遗传效应。

Separating direct, indirect and parent-of-origin genetic effects in the human population.

作者信息

Krätschmer Ilse, Hegemann Laura, Hofmeister Robin, Corfield Elizabeth C, Mahmoudi Mahdi, Delaneau Olivier, Andreassen Ole A, Campbell Archie, Hayward Caroline, Marioni Riccardo E, Ystrom Eivind, Havdahl Alexandra, Robinson Matthew R

机构信息

Institute Of Science and Technology Austria, Klosterneuburg, Austria.

PsychGen Center for Genetic Epidemiology and Mental Health, Norwegian Institute of Public Health, Oslo Norway.

出版信息

bioRxiv. 2025 Aug 27:2025.04.28.650988. doi: 10.1101/2025.04.28.650988.

Abstract

Here, we present a novel approach to estimate the degree to which the phenotypic effect of a DNA locus is attributable to four components: alleles in the child (direct genetic effects), alleles in the mother and the father (indirect genetic effects), or is dependent upon the parent from which it is inherited (parent-of-origin, PofO effects). Applying our model, JODIE, to 30,000 child-mother-father trios with phased DNA information from the Estonian Biobank (EstBB) and the Norwegian Mother, Father, Child Cohort (MoBa), we jointly estimate the phenotypic variance attributable to these four effects unbiased of assortative mating (AM) for height, body mass index (BMI) and childhood educational test score (EA). For all three traits, direct effects make the largest contribution to the genetic effect variance. But we find that parental indirect genetic effects make an equivalent combined contribution, and that there is a non-zero PofO effect variance for all traits. We calculate the heritability that would be obtained at the population-level in the absence of AM for common DNA loci, and show that the proportional contribution of direct effects to these heritability values can be calculated as 64.0% for EA in MoBa, 77.1% and 63.4% for height in MoBa and EstBB, and 81.2% and 88.0% for BMI in MoBa and EstBB. Additionally, using within-family genome-wide association testing, we identify 276 independently associated DNA regions that replicate across two additional biobanks, which all show a genotype-phenotype relationship that reflects an interplay of direct, indirect and PofO effects. Determining how direct, parental and PofO genetic effects combine across loci genome-wide to influence human phenotypic variation requires joint modeling of parental and child genotypes alongside the parental origin of loci and here, we make the first attempt to do this in the human population.

摘要

在此,我们提出一种新方法,以估计DNA位点的表型效应可归因于四个组成部分的程度:孩子的等位基因(直接遗传效应)、母亲和父亲的等位基因(间接遗传效应),或取决于其遗传自的亲本(亲本来源,PofO效应)。将我们的模型JODIE应用于来自爱沙尼亚生物银行(EstBB)和挪威母亲、父亲、儿童队列(MoBa)的30000个具有分阶段DNA信息的孩子 - 母亲 - 父亲三联体,我们联合估计了身高、体重指数(BMI)和儿童教育测试分数(EA)的表型方差,这些方差可归因于这四种效应,且不受选型交配(AM)的影响。对于所有这三个性状,直接效应在遗传效应方差中贡献最大。但我们发现,父母的间接遗传效应的综合贡献相当,并且所有性状都存在非零的PofO效应方差。我们计算了在不存在AM的情况下常见DNA位点在群体水平上可获得的遗传力,并表明直接效应在这些遗传力值中的比例贡献在MoBa中对于EA为64.0%,在MoBa和EstBB中对于身高分别为77.1%和63.4%,在MoBa和EstBB中对于BMI分别为81.2%和88.0%。此外,使用家庭内部全基因组关联测试,我们确定了276个在另外两个生物银行中重复的独立关联DNA区域,所有这些区域都显示出反映直接、间接和PofO效应相互作用的基因型 - 表型关系。确定直接、亲本和PofO遗传效应如何在全基因组范围内跨位点组合以影响人类表型变异需要对亲本和孩子的基因型以及位点的亲本来源进行联合建模,在此,我们首次尝试在人类群体中进行此操作。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c016/12407748/af468eda92fe/nihpp-2025.04.28.650988v3-f0001.jpg

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