δ样4mrna受邻近天然反义转录物调控。

Q4 Neuroscience
Vascular Cell Pub Date : 2015-03-24 eCollection Date: 2015-01-01 DOI:10.1186/s13221-015-0028-9
Keguo Li, Tamjid Chowdhury, Padmanabhan Vakeel, Christopher Koceja, Venkatesh Sampath, Ramani Ramchandran
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引用次数: 16

摘要

背景:最近的证据表明,基因组中的大多数rna不编码蛋白质。它们位于正义(S)或反义(AS)取向,迄今为止,人们对这些非编码rna (ncrna)的功能意义知之甚少。在这里,我们研究了S和AS转录本在关键血管生成基因Delta-like 4 (Dll4)调控中的关系。方法:采用RACE (Rapid Amplification of cDNA Ends)方法,对小鼠和人内皮细胞中Dll4基因位点的天然反义转录物进行鉴定,称为Dll4 Anti-Sense (Dll4- as)。实时荧光定量PCR检测Dll4和Dll4- as mRNA水平。通过过表达和敲低Dll4-AS来研究Dll4-AS的功能。结果:Dll4- as由三种接近Dll4启动子区域的异构体组成。Dll4- as异构体在不同内皮细胞系中的表达模式不同,但与Dll4的表达模式一致。在Dll4基因座中发现了一个双启动子元件,它控制着两个转录本的表达。Dll4- as和Dll4都对细胞密度敏感,细胞密度越高越有利于它们的表达。外源性Dll4刺激如VEGF、FGF和Notch信号抑制剂改变了Dll4 - as和Dll4的表达,表明转录物有共同调控作用。同时,敲低Dll4- as导致Dll4表达下调。结果,内皮细胞在体外增殖和迁移增加,芽形成增加。Dll4- as对Dll4的调控在体内也是保守的。结论:一种新的非编码rna介导的Dll4位点调控参与了血管发育过程,如细胞增殖、迁移和发芽。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Delta-like 4 mRNA is regulated by adjacent natural antisense transcripts.

Delta-like 4 mRNA is regulated by adjacent natural antisense transcripts.

Delta-like 4 mRNA is regulated by adjacent natural antisense transcripts.

Delta-like 4 mRNA is regulated by adjacent natural antisense transcripts.

Background: Recent evidence suggests that a majority of RNAs in the genome do not code for proteins. They are located in the sense (S) or antisense (AS) orientation and, to date, the functional significance of these non-coding RNAs (ncRNAs) is poorly understood. Here, we examined the relationship between S and AS transcripts in the regulation of a key angiogenesis gene, Delta-like 4 (Dll4).

Methods: Rapid Amplification of cDNA Ends (RACE) method was used to identify natural antisense transcripts in the Dll4 gene locus in murine and human endothelial cells, referred to as Dll4 Anti-Sense (Dll4-AS). Messenger RNA (mRNA) levels of Dll4 and Dll4-AS were quantified by real-time PCR. The function of Dll4-AS was investigated by overexpression and knocking down of Dll4-AS.

Results: Dll4-AS comprises of three isoforms that map proximal to the Dll4 promoter region. Expression patterns of Dll4-AS isoforms vary among different endothelial cell lines, but are always congruent with those of Dll4. A dual promoter element in the Dll4 locus has been identified that controls the expression of both transcripts. Both Dll4-AS and Dll4 are sensitive to cellular density in that higher cellular density favors their expression. Exogenous Dll4 stimuli such as VEGF, FGF and Notch signaling inhibitor altered both DLL4-AS and DLL4 expression suggesting co-regulation of the transcripts. Also, knocking down of Dll4-AS results in down-regulation of Dll4 expression. As a consequence, endothelial cell proliferation and migration increases in vitro, and sprout formation increases. The regulation of Dll4 by Dll4-AS was also conserved in vivo.

Conclusion: A novel form of non-coding RNA-mediated regulation at the Dll4 locus contributes to vascular developmental processes such as cell proliferation, migration and sprouting.

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来源期刊
Vascular Cell
Vascular Cell Neuroscience-Neurology
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