Hierarchical lncRNA regulatory network in early-onset severe preeclampsia.

IF 4.4 1区 生物学 Q1 BIOLOGY BMC Biology Pub Date : 2024-07-29 DOI:10.1186/s12915-024-01959-1
Haihua Liu, Zhijian Wang, Yanjun Li, Qian Chen, Sijia Jiang, Yue Gao, Jing Wang, Yali Chi, Jie Liu, Xiaoli Wu, Qiong Chen, Chaoqun Xiao, Mei Zhong, Chunlin Chen, Xinping Yang
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Abstract

Background: Recent studies have shown that several long non-coding RNAs (lncRNAs) in the placenta are associated with preeclampsia (PE). However, the extent to which lncRNAs may contribute to the pathological progression of PE is unclear.

Results: Here, we report a hierarchical regulatory network involved in early-onset severe PE (EOSPE). We have carried out transcriptome sequencing on the placentae from patients and normal subjects to identify the differentially expressed genes (DEGs), including some lncRNAs (DElncRNAs). We then constructed a high-quality hierarchical regulatory network of lncRNAs, transcription factors (TFs), and target DEGs, containing 1851 lncRNA-TF interactions and 6901 TF-promoter interactions. The lncRNA-to-target regulatory interactions were further validated by the triplex structures between the DElncRNAs and the promoters of the target DEGs. The DElncRNAs in the regulatory network were clustered into 3 clusters, one containing DElncRNAs correlated with the blood pressure, including FLNB-AS1 with targeting 27.89% (869/3116) DEGs in EOSPE. We further demonstrated that FLNB-AS1 could bind the transcription factor JUNB to regulate a series members of the HIF-1 signaling pathway in trophoblast cells.

Conclusions: Our results suggest that the differential expression of lncRNAs may perturb the lncRNA-TF-DEG hierarchical regulatory network, leading to the dysregulation of many genes involved in EOSPE. Our study provides a new strategy and a valuable resource for studying the mechanism underlying gene dysregulation in EOSPE patients.

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早发重度子痫前期的分层lncRNA调控网络
背景:最近的研究表明,胎盘中的几种长非编码RNA(lncRNA)与子痫前期(PE)有关。然而,lncRNA 对子痫前期病理进展的影响程度尚不清楚:结果:在此,我们报告了参与早发重度子痫前期(EOSPE)的分层调控网络。我们对患者和正常人的胎盘进行了转录组测序,以确定差异表达基因(DEGs),包括一些lncRNAs(DElncRNAs)。然后,我们构建了一个由lncRNAs、转录因子(TFs)和目标DEGs组成的高质量分层调控网络,其中包含1851个lncRNA-TF相互作用和6901个TF-启动子相互作用。DElncRNA与目标DEG启动子之间的三重结构进一步验证了lncRNA与目标之间的调控相互作用。调控网络中的DElncRNA被聚类为3个簇,其中一个簇包含了与血压相关的DElncRNA,其中FLNB-AS1靶向了EOSPE中27.89%(869/3116)的DEGs。我们进一步证实,FLNB-AS1可与转录因子JUNB结合,调控滋养层细胞中HIF-1信号通路的一系列成员:我们的研究结果表明,lncRNA的差异表达可能会扰乱lncRNA-TF-DEG的分级调控网络,导致许多参与EOSPE的基因失调。我们的研究为研究 EOSPE 患者基因失调的机制提供了一种新策略和宝贵资源。
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来源期刊
BMC Biology
BMC Biology 生物-生物学
CiteScore
7.80
自引率
1.90%
发文量
260
审稿时长
3 months
期刊介绍: BMC Biology is a broad scope journal covering all areas of biology. Our content includes research articles, new methods and tools. BMC Biology also publishes reviews, Q&A, and commentaries.
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