Juodakis Julius, Ytterberg Karin, Flatley Christopher, Sole-Navais Pol, Jacobsson Bo
Department of Obstetrics and Gynecology, Institute of Clinical Sciences, University of Gothenburg, Gothenburg, Sweden.
Department of Genetics and Bioinformatics, Division of Health Data and Digitalisation, Norwegian Institute of Public Health, Oslo, Norway.
medRxiv. 2023 Feb 10:2023.02.07.23285609. doi: 10.1101/2023.02.07.23285609.
Preterm birth is a major burden to neonatal health worldwide, determined in part by genetics. Recently, studies discovered several genes associated with this trait or its continuous equivalent - gestational duration. However, their effect timing, and thus clinical importance, is still unclear. Here, we use genotyping data of 31,000 births from the Norwegian Mother, Father and Child cohort (MoBa) to investigate different models of the genetic pregnancy "clock". We conduct genome-wide association studies using gestational duration or preterm birth, replicating known maternal associations and finding one new foetal variant. We illustrate how the interpretation of these results is complicated by the loss of power when dichotomizing. Using flexible survival models, we resolve this complexity and find that many of the known loci have time-varying effects, often stronger early in pregnancy. The overall polygenic control of birth timing appears to be shared in the term and preterm, but not very preterm periods, and exploratory results suggest involvement of the major histocompatibility complex genes in the latter. These findings show that the known gestational duration loci are clinically relevant, and should help design further experimental studies.
早产是全球新生儿健康的主要负担,部分由基因决定。最近,研究发现了几个与该性状或其连续等效物——孕周相关的基因。然而,它们的作用时间以及临床重要性仍不清楚。在此,我们使用来自挪威母亲、父亲和儿童队列研究(MoBa)的31000例出生的基因分型数据,来研究遗传妊娠“时钟”的不同模型。我们使用孕周或早产进行全基因组关联研究,重复已知的母体关联并发现一个新的胎儿变异。我们说明了二分法时由于效能损失如何使这些结果的解释变得复杂。使用灵活的生存模型,我们解决了这种复杂性,发现许多已知位点具有随时间变化的效应,通常在妊娠早期更强。出生时间的总体多基因控制似乎在足月和早产期是共享的,但在极早产期并非如此,探索性结果表明主要组织相容性复合体基因参与了极早产期。这些发现表明,已知的孕周位点具有临床相关性,并应有助于设计进一步的实验研究。
