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人类子宫肌层中的动态转录组、可及基因组和 PGR 顺式作用元件组谱。

Dynamic transcriptome, accessible genome, and PGR cistrome profiles in the human myometrium.

机构信息

Reproductive & Developmental Biology Laboratory, National Institute of Environmental Health Sciences, Research Triangle Park, NC.

Department of Obstetrics & Gynecology, University of South Florida Morsani College of Medicine and Moffitt Cancer Center, Tampa, FL.

出版信息

FASEB J. 2020 Feb;34(2):2252-2268. doi: 10.1096/fj.201902654R. Epub 2019 Dec 12.

DOI:10.1096/fj.201902654R
PMID:31908010
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10189786/
Abstract

The myometrium undergoes structural and functional remodeling during pregnancy. We hypothesize that myometrial genomic elements alter correspondingly in preparation for parturition. Human myometrial tissues from nonpregnant (NP) and term pregnant (TP) human subjects were examined by RNAseq, ATACseq, and PGR ChIPseq assays to profile transcriptome, assessible genome, and PGR occupancy. NP and TP specimens exhibit 2890 differentially expressed genes, reflecting an increase of metabolic, inflammatory, and PDGF signaling, among others, in adaptation to pregnancy. At the epigenome level, patterns of accessible genome change between NP and TP myometrium, leading to the altered enrichment of binding motifs for hormone and muscle regulators such as the progesterone receptor (PGR), Krüppel-like factors, and MEF2A transcription factors. PGR genome occupancy exhibits a significant difference between the two stages of the myometrium, concomitant with distinct transcriptomic profiles including genes such as ENO1, LHDA, and PLCL1 in the glycolytic and calcium signaling pathways. Over-representation of SRF, MYOD, and STAT binding motifs in PGR occupying sites further suggests interactions between PGR and major muscle regulators for myometrial gene expression. In conclusion, changes in accessible genome and PGR occupancy are part of the myometrial remodeling process and may serve as mechanisms to formulate the state-specific transcriptome profiles.

摘要

子宫肌层在怀孕期间经历结构和功能重塑。我们假设,为了分娩,子宫肌层的基因组元件相应地发生改变。通过 RNAseq、ATACseq 和 PGR ChIPseq 检测,对非妊娠 (NP) 和足月妊娠 (TP) 人类受试者的人子宫肌组织进行了检测,以描绘转录组、可及基因组和 PGR 占有率。NP 和 TP 标本表现出 2890 个差异表达基因,反映了代谢、炎症和 PDGF 信号等方面的增加,以适应妊娠。在表观基因组水平上,NP 和 TP 子宫肌层之间可及基因组的模式发生变化,导致激素和肌肉调节因子(如孕激素受体 (PGR)、Krüppel 样因子和 MEF2A 转录因子)结合基序的富集发生改变。PGR 基因组占有率在子宫肌层的两个阶段存在显著差异,伴随着独特的转录组谱,包括糖酵解和钙信号通路中的 ENO1、LHDA 和 PLCL1 等基因。PGR 占据位点中 SRF、MYOD 和 STAT 结合基序的过度表达进一步表明 PGR 与主要肌肉调节因子之间的相互作用,用于子宫肌层基因表达。总之,可及基因组和 PGR 占有率的变化是子宫肌重塑过程的一部分,可能作为形成特定状态转录组谱的机制。

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