Epigenetic scores derived in saliva are associated with gestational age at birth.

IF 4.8 2区 医学 Q1 GENETICS & HEREDITY
Katie Mckinnon, Eleanor L S Conole, Kadi Vaher, Robert F Hillary, Danni A Gadd, Justyna Binkowska, Gemma Sullivan, Anna J Stevenson, Amy Corrigan, Lee Murphy, Heather C Whalley, Hilary Richardson, Riccardo E Marioni, Simon R Cox, James P Boardman
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引用次数: 0

Abstract

Background: Epigenetic scores (EpiScores), reflecting DNA methylation (DNAm)-based surrogates for complex traits, have been developed for multiple circulating proteins. EpiScores for pro-inflammatory proteins, such as C-reactive protein (DNAm CRP), are associated with brain health and cognition in adults and with inflammatory comorbidities of preterm birth in neonates. Social disadvantage can become embedded in child development through inflammation, and deprivation is overrepresented in preterm infants. We tested the hypotheses that preterm birth and socioeconomic status (SES) are associated with alterations in a set of EpiScores enriched for inflammation-associated proteins.

Results: In total, 104 protein EpiScores were derived from saliva samples of 332 neonates born at gestational age (GA) 22.14 to 42.14 weeks. Saliva sampling was between 36.57 and 47.14 weeks. Forty-three (41%) EpiScores were associated with low GA at birth (standardised estimates |0.14 to 0.88|, Bonferroni-adjusted p-value < 8.3 × 10-3). These included EpiScores for chemokines, growth factors, proteins involved in neurogenesis and vascular development, cell membrane proteins and receptors, and other immune proteins. Three EpiScores were associated with SES, or the interaction between birth GA and SES: afamin, intercellular adhesion molecule 5, and hepatocyte growth factor-like protein (standardised estimates |0.06 to 0.13|, Bonferroni-adjusted p-value < 8.3 × 10-3). In a preterm subgroup (n = 217, median [range] GA 29.29 weeks [22.14 to 33.0 weeks]), SES-EpiScore associations did not remain statistically significant after adjustment for sepsis, bronchopulmonary dysplasia, necrotising enterocolitis, and histological chorioamnionitis.

Conclusions: Low birth GA is substantially associated with a set of EpiScores. The set was enriched for inflammatory proteins, providing new insights into immune dysregulation in preterm infants. SES had fewer associations with EpiScores; these tended to have small effect sizes and were not statistically significant after adjusting for inflammatory comorbidities. This suggests that inflammation is unlikely to be the primary axis through which SES becomes embedded in the development of preterm infants in the neonatal period.

唾液中的表观遗传评分与出生时的胎龄有关。
背景:针对多种循环蛋白开发了表观遗传评分(EpiScores),反映基于 DNA 甲基化(DNAm)的复杂性状替代物。C反应蛋白(DNAm CRP)等促炎症蛋白的表观遗传评分与成人的大脑健康和认知能力有关,也与新生儿早产的炎症并发症有关。社会劣势可通过炎症嵌入儿童发育中,而早产儿中被剥夺的比例过高。我们检验了早产和社会经济地位(SES)与一组富含炎症相关蛋白的 EpiScores 变化相关的假设:从胎龄(GA)22.14 周至 42.14 周的 332 名新生儿的唾液样本中得出了 104 个蛋白质 EpiScores。唾液采样时间为 36.57 周至 47.14 周。43个(41%)EpiScores与出生时低胎龄相关(标准化估计值|0.14至0.88|,Bonferroni调整后的P值-3)。其中包括趋化因子、生长因子、参与神经发生和血管发育的蛋白质、细胞膜蛋白质和受体以及其他免疫蛋白质的 EpiScores。有三种 EpiScores 与 SES 或出生性别差异与 SES 之间的交互作用相关:阿法明、细胞间粘附分子 5 和肝细胞生长因子样蛋白(标准化估计值为 0.06 至 0.13,经 Bonferroni-adjusted p 值为 -3)。在早产儿亚组(n = 217,中位数[范围]GA 29.29周[22.14至33.0周])中,在对败血症、支气管肺发育不良、坏死性小肠结肠炎和组织学绒毛膜羊膜炎进行调整后,SES-EpiScore相关性在统计学上并不显著:结论:低出生体重与一组 EpiScores 有很大关系。结论:低出生体重儿与一组 EpiScores 有很大关系,这组 EpiScores 富含炎症蛋白,为早产儿免疫失调提供了新的视角。SES与EpiScores的相关性较小;这些相关性的效应大小往往较小,而且在调整炎症合并症后并无统计学意义。这表明,炎症不太可能是社会经济地位嵌入早产儿新生儿期发育的主要轴心。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
自引率
5.30%
发文量
150
期刊介绍: Clinical Epigenetics, the official journal of the Clinical Epigenetics Society, is an open access, peer-reviewed journal that encompasses all aspects of epigenetic principles and mechanisms in relation to human disease, diagnosis and therapy. Clinical trials and research in disease model organisms are particularly welcome.
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