非裔美国妇女的早产问题:妊娠早期多血型试点研究。

Alexandra L Nowak, Nadia Saadat, Jiao Sun, Anna M Forsman, Xiaoyu Liang, Cara Joyce, Jennifer Woo, Christopher G Engeland, Dawn P Misra, Carmen Giurgescu, Wei Zhang, Cindy M Anderson
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引用次数: 0

摘要

早产(PTB;HLA-DQB2 基因在早产和过期产妇女之间存在甲基化差异(cg12296550;p = .02)和表达差异(p = .014;log2FC = 2.5)。基因表达分析表明,HLA-DQB2 和 HLA-DRB4 (p = .028; log2FC = -3.6)是表达量最高的两个基因。HLA-DQB2 在 PTB 中表达较高,而 HLA-DRB4 在足月儿中表达较高。然而,经 Bonferroni 校正后,没有基因仍具有显著性(p < .05)。在降维模型中,HLA-DRB4 和 AKR1C1 被确定为潜在的生物标记物,它们对免疫功能和异体分解也很重要。基因表达的改变可能会导致炎症失衡或异基因不耐受,从而导致 PTB。这项研究提供了概念性证据,证明了未来利用更多人群进行多组学研究的可行性和重要性,以进一步探索在此发现的基因和通路。
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Preterm Birth in African American Women: A Multi-Omic Pilot Study in Early Pregnancy.

Preterm birth (PTB; <37 weeks completed gestation) is a devastating problem affecting over 13 million live births worldwide. In the U.S., African Americans experience significantly higher rates of PTB compared to non-Hispanic Whites. PTB disparities have been linked to social determinants of health (e.g., socioeconomic status, discrimination). However, the biological underpinnings related to these associations are unclear. DNA methylation (DNAm) is subject to environmental influences, and DNAm modifications are known to affect gene expression. Using a multi-omic approach, we examined differences in combined DNA methylation (DNAm) and messenger RNA (mRNA) transcriptomic data from 20 pregnant African American women (12 PTB; 8 term birth) early in pregnancy (8-18 weeks gestation). We found that the HLA-DQB2 gene was both differentially methylated (cg12296550; p = .02) and differentially expressed (p = .014; log2FC = 2.5) between women with PTB and term birth. Gene expression analysis showed HLA-DQB2 and HLA-DRB4 (p = .028; log2FC = -3.6) were the two most highly expressed genes. HLA-DQB2 expressed higher in PTB and HLA-DRB4 expressed higher in term birth. However, no genes remained significant (p < .05) after Bonferroni correction. HLA-DRB4 and AKR1C1 were identified as a potential biomarkers in dimensionality reduction models and are also important to immune function and allogenic breakdown. Altered gene expression may lead to inflammatory imbalances or allogenic intolerance resulting in PTB. This study provides proof-of-concept evidence for the feasibility and importance of future multi-omics studies with larger populations to further explore the genes and pathways identified here.

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