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胎盘-脑轴的证据:多组学核聚合预测极早产儿的智力和社交障碍。

Evidence for the placenta-brain axis: multi-omic kernel aggregation predicts intellectual and social impairment in children born extremely preterm.

机构信息

Biobehavioral Laboratory, School of Nursing, University of North Carolina, 544 Carrington Hall, Campus Box 7460, Chapel Hill, NC, 27599-7460, USA.

Institute for Environmental Health Solutions, Gillings School of Global Public Health, University of North Carolina, Chapel Hill, NC, USA.

出版信息

Mol Autism. 2020 Dec 11;11(1):97. doi: 10.1186/s13229-020-00402-w.

Abstract

BACKGROUND

Children born extremely preterm are at heightened risk for intellectual and social impairment, including Autism Spectrum Disorder (ASD). There is increasing evidence for a key role of the placenta in prenatal developmental programming, suggesting that the placenta may, in part, contribute to origins of neurodevelopmental outcomes.

METHODS

We examined associations between placental transcriptomic and epigenomic profiles and assessed their ability to predict intellectual and social impairment at age 10 years in 379 children from the Extremely Low Gestational Age Newborn (ELGAN) cohort. Assessment of intellectual ability (IQ) and social function was completed with the Differential Ability Scales-II and Social Responsiveness Scale (SRS), respectively. Examining IQ and SRS allows for studying ASD risk beyond the diagnostic criteria, as IQ and SRS are continuous measures strongly correlated with ASD. Genome-wide mRNA, CpG methylation and miRNA were assayeds with the Illumina Hiseq 2500, HTG EdgeSeq miRNA Whole Transcriptome Assay, and Illumina EPIC/850 K array, respectively. We conducted genome-wide differential analyses of placental mRNA, miRNA, and CpG methylation data. These molecular features were then integrated for a predictive analysis of IQ and SRS outcomes using kernel aggregation regression. We lastly examined associations between ASD and the multi-omic-predicted component of IQ and SRS.

RESULTS

Genes with important roles in neurodevelopment and placental tissue organization were associated with intellectual and social impairment. Kernel aggregations of placental multi-omics strongly predicted intellectual and social function, explaining approximately 8% and 12% of variance in SRS and IQ scores via cross-validation, respectively. Predicted in-sample SRS and IQ showed significant positive and negative associations with ASD case-control status.

LIMITATIONS

The ELGAN cohort comprises children born pre-term, and generalization may be affected by unmeasured confounders associated with low gestational age. We conducted external validation of predictive models, though the sample size (N = 49) and the scope of the available out-sample placental dataset are limited. Further validation of the models is merited.

CONCLUSIONS

Aggregating information from biomarkers within and among molecular data types improves prediction of complex traits like social and intellectual ability in children born extremely preterm, suggesting that traits within the placenta-brain axis may be omnigenic.

摘要

背景

极早产儿出生时存在智力和社交障碍的风险增加,包括自闭症谱系障碍(ASD)。越来越多的证据表明胎盘在产前发育编程中起着关键作用,这表明胎盘可能在一定程度上导致神经发育结局的起源。

方法

我们研究了 379 名来自超低 gestational age newborn(ELGAN)队列的儿童的胎盘转录组和表观基因组谱之间的关联,并评估了它们预测 10 岁时智力和社交障碍的能力。使用差异能力量表-II(DAS-II)和社交反应量表(SRS)分别评估智力能力(IQ)和社会功能。研究 IQ 和 SRS 可以研究自闭症风险超出诊断标准,因为 IQ 和 SRS 是与自闭症密切相关的连续测量指标。使用 Illumina Hiseq 2500、HTG EdgeSeq miRNA 全转录组分析和 Illumina EPIC/850K 微阵列分别检测全基因组 mRNA、CpG 甲基化和 miRNA。我们对胎盘 mRNA、miRNA 和 CpG 甲基化数据进行了全基因组差异分析。然后,使用核聚集回归对这些分子特征进行集成,以进行 IQ 和 SRS 结果的预测分析。最后,我们研究了 ASD 与 IQ 和 SRS 的多组学预测成分之间的关联。

结果

在神经发育和胎盘组织组织中具有重要作用的基因与智力和社交障碍有关。胎盘多组学的核聚集强烈预测了智力和社交功能,通过交叉验证分别解释了 SRS 和 IQ 得分的约 8%和 12%的方差。预测的样本内 SRS 和 IQ 与 ASD 病例对照状态呈显著正相关和负相关。

局限性

ELGAN 队列由早产儿出生的儿童组成,概括可能受到与低胎龄相关的未测量混杂因素的影响。我们对预测模型进行了外部验证,尽管样本量(N = 49)和可用的外样本胎盘数据集的范围有限。值得进一步验证这些模型。

结论

在分子数据类型内和之间聚合信息可提高对极早产儿出生的儿童复杂特征(如社交和智力能力)的预测,这表明胎盘-大脑轴内的特征可能是全基因组的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7ad8/7730750/a91fcfb7a22f/13229_2020_402_Fig1_HTML.jpg

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