前沿:长基因间非编码 RNA Tmevpg1 对 Th1 细胞 Ifng 表达的影响。
Cutting edge: influence of Tmevpg1, a long intergenic noncoding RNA, on the expression of Ifng by Th1 cells.
机构信息
Department of Pathology, Microbiology, and Immunology, Vanderbilt University School of Medicine, Nashville, TN 37232, USA.
出版信息
J Immunol. 2012 Sep 1;189(5):2084-8. doi: 10.4049/jimmunol.1200774. Epub 2012 Jul 30.
Abstract
The majority of the genome is noncoding and was thought to be nonfunctional. However, it is now appreciated that transcriptional control of protein coding genes resides within these noncoding regions. Thousands of genes encoding long intergenic noncoding RNAs (lincRNAs) have been recently identified throughout the genome, which positively or negatively regulate transcription of neighboring target genes. Both TMEVPG1 and its mouse ortholog encode lincRNAs and are positioned near the IFN-γ gene (IFNG). In this study, we show that transcription of both mouse and human TMEVPG1 genes is Th1 selective and dependent on Stat4 and T-bet, transcription factors that drive the Th1 differentiation program. Ifng expression is partially restored in Stat4-/-Tbx21-/- cells through coexpression of T-bet and Tmevpg1, and Tmevpg1 expression contributes to, but alone is not sufficient to, drive Th1-dependent Ifng expression. Our results suggest that TMEVPG1 belongs to the general class of lincRNAs that positively regulate gene transcription.
摘要
大部分基因组是非编码的,曾被认为是无功能的。然而,现在人们已经意识到,蛋白质编码基因的转录调控存在于这些非编码区域中。最近在整个基因组中已经鉴定出了数千个编码长基因间非编码 RNA(lincRNA)的基因,它们正向或负向调节邻近靶基因的转录。TMEVPG1 及其小鼠同源物都编码 lincRNA,并且位于 IFN-γ 基因(IFNG)附近。在这项研究中,我们表明,两种小鼠和人类 TMEVPG1 基因的转录均具有 Th1 选择性,并且依赖于 Stat4 和 T-bet,这两种转录因子驱动 Th1 分化程序。在 Stat4-/-Tbx21-/-细胞中,通过共表达 T-bet 和 Tmevpg1,部分恢复了 Ifng 的表达,并且 Tmevpg1 的表达有助于,但不能单独驱动 Th1 依赖性 Ifng 的表达。我们的结果表明,TMEVPG1 属于一类正向调节基因转录的 lincRNA。
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