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通过 5' tRNA 片段控制非编码 RNA 的产生和组蛋白水平。

Control of noncoding RNA production and histone levels by a 5' tRNA fragment.

机构信息

Department of Biochemistry and Molecular Pharmacology, University of Massachusetts Medical School, Worcester, Massachusetts 01605, USA.

出版信息

Genes Dev. 2020 Jan 1;34(1-2):118-131. doi: 10.1101/gad.332783.119. Epub 2019 Dec 12.

Abstract

Small RNAs derived from mature tRNAs, referred to as tRNA fragments or "tRFs," are an emerging class of regulatory RNAs with poorly understood functions. We recently identified a role for one specific tRF-5' tRF-Gly-GCC, or tRF-GG-as a repressor of genes associated with the endogenous retroelement MERVL, but the mechanistic basis for this regulation was unknown. Here, we show that tRF-GG plays a role in production of a wide variety of noncoding RNAs-snoRNAs, scaRNAs, and snRNAs-that are dependent on Cajal bodies for stability and activity. Among these noncoding RNAs, regulation of the U7 snRNA by tRF-GG modulates heterochromatin-mediated transcriptional repression of MERVL elements by supporting an adequate supply of histone proteins. Importantly, the effects of inhibiting tRF-GG on histone mRNA levels, on activity of a histone 3' UTR reporter, and ultimately on MERVL regulation could all be suppressed by manipulating U7 RNA levels. We additionally show that the related RNA-binding proteins hnRNPF and hnRNPH bind directly to tRF-GG, and are required for Cajal body biogenesis, positioning these proteins as strong candidates for effectors of tRF-GG function in vivo. Together, our data reveal a conserved mechanism for 5' tRNA fragment control of noncoding RNA biogenesis and, consequently, global chromatin organization.

摘要

来自成熟 tRNA 的小 RNA 被称为 tRNA 片段或“tRFs”,是一类新兴的调节 RNA,其功能尚未被充分理解。我们最近发现了一种特定的 tRF-5' tRF-Gly-GCC,即 tRF-GG,作为内源性反转录元件 MERVL 相关基因的抑制剂的作用,但这种调节的机制尚不清楚。在这里,我们表明 tRF-GG 在多种非编码 RNA 的产生中发挥作用——snoRNA、scaRNA 和 snRNA——这些非编码 RNA 的稳定性和活性依赖于 Cajal 体。在这些非编码 RNA 中,tRF-GG 对 U7 snRNA 的调节通过支持组蛋白蛋白的充足供应来调节 MERVL 元件的异染色质介导的转录抑制。重要的是,抑制 tRF-GG 对组蛋白 mRNA 水平、组蛋白 3'UTR 报告基因活性以及最终对 MERVL 调节的影响都可以通过操纵 U7 RNA 水平来抑制。我们还表明,相关的 RNA 结合蛋白 hnRNPF 和 hnRNPH 直接与 tRF-GG 结合,并且是 Cajal 体发生所必需的,这些蛋白是 tRF-GG 功能在体内的效应物的强有力候选者。总之,我们的数据揭示了 5' tRNA 片段控制非编码 RNA 生物发生的保守机制,从而影响了全局染色质组织。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/855f/6938667/5e6018609a0f/118f01.jpg

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