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在妊娠人子宫肌层中的体内全基因组 PGR 结合鉴定了分娩的潜在调控因子。

In Vivo Genome-Wide PGR Binding in Pregnant Human Myometrium Identifies Potential Regulators of Labor.

机构信息

Department of Obstetrics & Gynecology, Feinberg School of Medicine, Northwestern University, Chicago, IL, 60611, USA.

Department of Bioengineering, University of Illinois at Chicago, Chicago, IL, 60612, USA.

出版信息

Reprod Sci. 2023 Feb;30(2):544-559. doi: 10.1007/s43032-022-01002-0. Epub 2022 Jun 22.

Abstract

The alterations in myometrial biology during labor are not well understood. The myometrium is the contractile portion of the uterus and contributes to labor, a process that may be regulated by the steroid hormone progesterone. Thus, human myometrial tissues from term pregnant in-active-labor (TIL) and term pregnant not-in-labor (TNIL) subjects were used for genome-wide analyses to elucidate potential future preventive or therapeutic targets involved in the regulation of labor. Using myometrial tissues directly subjected to RNA sequencing (RNA-seq), progesterone receptor (PGR) chromatin immunoprecipitation sequencing (ChIP-seq), and histone modification ChIP-seq, we profiled genome-wide changes associated with gene expression in myometrial smooth muscle tissue in vivo. In TIL myometrium, PGR predominantly occupied promoter regions, including the classical progesterone response element, whereas it bound mainly to intergenic regions in TNIL myometrial tissue. Differential binding analysis uncovered over 1700 differential PGR-bound sites between TIL and TNIL, with 1361 sites gained and 428 lost in labor. Functional analysis identified multiple pathways involved in cAMP-mediated signaling enriched in labor. A three-way integration of the data for ChIP-seq, RNA-seq, and active histone marks uncovered the following genes associated with PGR binding, transcriptional activation, and altered mRNA levels: ATP11A, CBX7, and TNS1. In vitro studies showed that ATP11A, CBX7, and TNS1 are progesterone responsive. We speculate that these genes may contribute to the contractile phenotype of the myometrium during various stages of labor. In conclusion, we provide novel labor-associated genome-wide events and PGR-target genes that can serve as targets for future mechanistic studies.

摘要

分娩过程中子宫生物学的改变尚不清楚。子宫肌层是子宫的收缩部分,有助于分娩,这一过程可能受甾体激素孕酮的调节。因此,使用来自足月未临产(TIL)和足月已临产(TNIL)孕妇的人子宫肌组织进行全基因组分析,以阐明参与分娩调节的潜在未来预防或治疗靶点。使用直接进行 RNA 测序(RNA-seq)、孕酮受体(PGR)染色质免疫沉淀测序(ChIP-seq)和组蛋白修饰 ChIP-seq 的子宫肌组织,我们对与子宫平滑肌组织体内基因表达相关的全基因组变化进行了分析。在 TIL 子宫肌中,PGR 主要占据启动子区域,包括经典孕酮反应元件,而在 TNIL 子宫肌组织中主要结合于基因间区域。差异结合分析发现 TIL 和 TNIL 之间存在 1700 多个差异 PGR 结合位点,其中 1361 个在分娩时获得,428 个在分娩时丢失。功能分析确定了参与 cAMP 介导信号转导的多个途径在分娩中富集。ChIP-seq、RNA-seq 和活性组蛋白标记的三向整合揭示了与 PGR 结合、转录激活和 mRNA 水平改变相关的以下基因:ATP11A、CBX7 和 TNS1。体外研究表明,ATP11A、CBX7 和 TNS1 对孕酮有反应。我们推测这些基因可能有助于子宫肌在分娩各个阶段的收缩表型。总之,我们提供了与分娩相关的全基因组新事件和 PGR 靶基因,可作为未来机制研究的靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bbc3/9988762/5b8cc4824a20/43032_2022_1002_Fig1_HTML.jpg

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