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转录组分析揭示了与人类足月分娩相关的子宫肌拓扑关联结构域。

Transcriptomic analysis reveals myometrial topologically associated domains linked to the onset of human term labour.

机构信息

Department of Infectious Diseases, Central Clinical School, Monash University and the Alfred Hospital, Melbourne, VIC, Australia.

Mothers and Babies Research Centre, HMRI University of Newcastle, NSW, Australia.

出版信息

Mol Hum Reprod. 2022 Mar 8;28(3). doi: 10.1093/molehr/gaac003.

Abstract

Changes in cell phenotype are thought to occur through the expression of groups of co-regulated genes within topologically associated domains (TADs). In this paper, we allocate genes expressed within the myometrium of the human uterus during the onset of term labour into TADs. Transformation of the myometrial cells of the uterus into a contractile phenotype during term human labour is the result of a complex interaction of different epigenomic and genomic layers. Recent work suggests that the transcription factor (TF) RELA lies at the top of this regulatory network. Using deep RNA sequencing (RNAseq) analysis of myometrial samples (n = 16) obtained at term from women undergoing caesarean section prior to or after the onset of labour, we have identified evidence for how other gene expression regulatory elements interact with TFs in the labour phenotype transition. Gene set enrichment analysis of our RNAseq data identified three modules of enriched genes (M1, M2 and M3), which in gene ontology studies are linked to matrix degradation, smooth muscle and immune gene signatures, respectively. These genes were predominantly located within chromosomal TADs suggesting co-regulation of expression. Our transcriptomic analysis also identified significant differences in the expression of long non-coding RNAs (lncRNA), microRNAs (miRNA) and TFs that were predicted to target genes within the TADs. Additionally, network analysis revealed 15 new lncRNA (MCM3AP-AS1, TUG1, MIR29B2CHG, HCG18, LINC00963, KCNQ1OT1, NEAT1, HELLPAR, SNHG16, NUTM2B-AS1, MALAT1, PSMA3-AS1, GABPB1-AS1, NORAD and NKILA) and 4 miRNA (mir-145, mir-223, mir-let-7a and mir-132) as top gene hubs with three TFs (NFKB1, RELA and ESR1) as master regulators. Together, these factors are likely to be involved in co-regulatory networks driving a myometrial transformation to generate an estrogen-sensitive phenotype. We conclude that lncRNA and miRNA targeting the estrogen receptor 1 and nuclear factor kappa B pathways play a key role in the initiation of human labour. For the first time, we perform an integrative analysis to present a multi-level genomic signature made of mRNA, non-coding RNA and TFs in the myometrium for spontaneous term labour.

摘要

细胞表型的变化被认为是通过拓扑相关结构域(TAD)内的一组共调控基因的表达来实现的。在本文中,我们将在人类子宫中表达的基因分配到子宫肌层中的 TAD 中。在足月分娩期间,子宫平滑肌细胞转化为收缩表型是不同表观遗传和基因组层相互作用的结果。最近的研究表明,转录因子(TF)RELA 位于这个调控网络的顶端。我们使用深度 RNA 测序(RNAseq)分析了 16 名在剖宫产前或分娩开始后从接受剖宫产的足月妇女中获得的子宫肌样本,鉴定了其他基因表达调控元件如何与劳动表型转换中的 TF 相互作用的证据。我们的 RNAseq 数据的基因集富集分析确定了三个富含基因的模块(M1、M2 和 M3),在基因本体论研究中,这些模块分别与基质降解、平滑肌和免疫基因特征相关。这些基因主要位于染色体 TAD 内,表明表达的共调控。我们的转录组分析还鉴定了长非编码 RNA(lncRNA)、微小 RNA(miRNA)和 TF 的表达的显著差异,这些 TF 被预测为 TAD 内基因的靶基因。此外,网络分析揭示了 15 个新的 lncRNA(MCM3AP-AS1、TUG1、MIR29B2CHG、HCG18、LINC00963、KCNQ1OT1、NEAT1、HELLPAR、SNHG16、NUTM2B-AS1、MALAT1、PSMA3-AS1、GABPB1-AS1、NORAD 和 NKILA)和 4 个 miRNA(mir-145、mir-223、mir-let-7a 和 mir-132)作为顶级基因枢纽,以及三个 TF(NFKB1、RELA 和 ESR1)作为主调控因子。这些因素可能共同参与驱动子宫平滑肌转化以产生雌激素敏感表型的共调控网络。我们得出结论,lncRNA 和 miRNA 靶向雌激素受体 1 和核因子 kappa B 途径在人类分娩的开始中发挥关键作用。这是我们第一次进行综合分析,在人类足月自发性分娩中呈现出由 mRNA、非编码 RNA 和 TF 组成的多层次基因组特征。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2fbd/8903000/c4c4d055e908/gaac003f1.jpg

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