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首页> 外文期刊>Methods: A Companion to Methods in Enzymology >Small RNAs derived from structural non-coding RNAs
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Small RNAs derived from structural non-coding RNAs

机译:来自结构非编码RNA的小RNA

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摘要

It has been shown in small RNA sequencing-based studies that some small RNA fragments are specifically processed from known structural non-coding RNAs, either through Dicer-dependent or Dicer-independent pathways. Although these small RNAs are often less abundant compared to microRNAs in normal mammalian tissues, they are always present in all sequenced libraries. In this paper, we use the ncPRO-seq pipeline, to describe different profiles of these small RNA fragments, and to discuss their potential processing pathways and functions. To assess whether more small RNA fragments can be detected in small RNA sequencing datasets, we decided to focus on small nuclear RNAs, abbreviated as snRNAs, which are associated with Sm ribonucleoproteins to form functional RNA-protein complexes. Here, we describe a group of small RNA fragments derived from snRNAs, which are typically highly enriched in regions bound by Sm proteins. Based on this, we propose the existence of a potential novel small RNA family associated with Sm proteins.
机译:在基于小型RNA测序的研究中已经显示,某些小RNA片段是通过已知的非切丁酶依赖性或不依赖于切丁酶的途径从已知结构非编码RNA中特异性加工而成的。尽管与正常哺乳动物组织中的microRNA相比,这些小RNA常常不那么丰富,但它们始终存在于所有测序文库中。在本文中,我们使用ncPRO-seq管道来描述这些小RNA片段的不同概况,并讨论它们的潜在加工途径和功能。为了评估是否可以在小型RNA测序数据集中检测到更多的小型RNA片段,我们决定专注于小核RNA(缩写为snRNA),其与Sm核糖核蛋白结合形成功能性RNA-蛋白质复合物。在这里,我们描述了一组源自snRNA的小RNA片段,这些片段通常高度富含Sm蛋白结合的区域。基于此,我们提出了与Sm蛋白相关的潜在新型小RNA家族的存在。

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