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长链非编码RNA:来自基因组印记的经验教训。

Long noncoding RNAs: Lessons from genomic imprinting.

作者信息

Kanduri Chandrasekhar

机构信息

Department of Medical Genetics, Institute of Biomedicine, Sahlgrenska Academy, University of Gothenburg, 40530 Gothenburg, Sweden.

出版信息

Biochim Biophys Acta. 2016 Jan;1859(1):102-11. doi: 10.1016/j.bbagrm.2015.05.006. Epub 2015 May 22.

Abstract

Genomic imprinting has been a great resource for studying transcriptional and post-transcriptional-based gene regulation by long noncoding RNAs (lncRNAs). In this article, I overview the functional role of intergenic lncRNAs (H19, IPW, and MEG3), antisense lncRNAs (Kcnq1ot1, Airn, Nespas, Ube3a-ATS), and enhancer lncRNAs (IG-DMR eRNAs) to understand the diverse mechanisms being employed by them in cis and/or trans to regulate the parent-of-origin-specific expression of target genes. Recent evidence suggests that some of the lncRNAs regulate imprinting by promoting intra-chromosomal higher-order chromatin compartmentalization, affecting replication timing and subnuclear positioning. Whereas others act via transcriptional occlusion or transcriptional collision-based mechanisms. By establishing genomic imprinting of target genes, the lncRNAs play a critical role in important biological functions, such as placental and embryonic growth, pluripotency maintenance, cell differentiation, and neural-related functions such as synaptic development and plasticity. An emerging consensus from the recent evidence is that the imprinted lncRNAs fine-tune gene expression of the protein-coding genes to maintain their dosage in cell. Hence, lncRNAs from imprinted clusters offer insights into their mode of action, and these mechanisms have been the basis for uncovering the mode of action of lncRNAs in several other biological contexts. This article is part of a Special Issue entitled: Clues to long noncoding RNA taxonomy, edited by Dr. Tetsuro Hirose and Dr. Shinichi Nakagawa.

摘要

基因组印记一直是研究长链非编码RNA(lncRNA)介导的转录及转录后基因调控的重要资源。在本文中,我将概述基因间lncRNA(H19、IPW和MEG3)、反义lncRNA(Kcnq1ot1、Airn、Nespas、Ube3a-ATS)和增强子lncRNA(IG-DMR eRNA)的功能作用,以了解它们通过顺式和/或反式作用调控靶基因亲本来源特异性表达所采用的多种机制。最近的证据表明,一些lncRNA通过促进染色体内高阶染色质区室化、影响复制时间和亚核定位来调控印记。而其他lncRNA则通过转录阻抑或基于转录碰撞的机制发挥作用。通过建立靶基因的基因组印记,lncRNA在重要生物学功能中发挥关键作用,如胎盘和胚胎生长、多能性维持、细胞分化以及与神经相关的功能,如突触发育和可塑性。近期证据得出的一个新共识是,印记lncRNA对蛋白质编码基因的表达进行微调,以维持其在细胞中的剂量。因此,来自印记簇的lncRNA为深入了解其作用模式提供了线索,这些机制也是揭示lncRNA在其他几种生物学背景下作用模式的基础。本文是由广濑哲郎博士和中川信一博士编辑的特刊“长链非编码RNA分类线索”的一部分。

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