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miR-222 异构体受 I 型干扰素的差异调控。

miR-222 isoforms are differentially regulated by type-I interferon.

机构信息

Centre for Innate Immunity and Infectious Diseases, Monash Institute of Medical Research, Monash University, Clayton, Victoria 3168, Australia.

Department of Molecular and Translational Science, Monash University, Clayton, Victoria 3168, Australia.

出版信息

RNA. 2018 Mar;24(3):332-341. doi: 10.1261/rna.064550.117. Epub 2017 Dec 20.

DOI:10.1261/rna.064550.117
PMID:29263133
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5824353/
Abstract

Endogenous microRNAs (miRNAs) often exist as multiple isoforms (known as "isomiRs") with predominant variation around their 3'-end. Increasing evidence suggests that different isomiRs of the same family can have diverse functional roles, as recently demonstrated with the example of miR-222-3p 3'-end variants. While isomiR levels from a same miRNA family can vary between tissues and cell types, change of templated isomiR stoichiometry to stimulation has not been reported to date. Relying on small RNA-sequencing analyses, we demonstrate here that miR-222-3p 3'-end variants >23 nt are specifically decreased upon interferon (IFN) β stimulation of human fibroblasts, while shorter isoforms are spared. This length-dependent dynamic regulation of long miR-222-3p 3'-isoforms and >40 other miRNA families was confirmed in human monocyte-derived dendritic cells following infection with Typhimurium, underlining the breadth of 3'-length regulation by infection, beyond the example of miR-222-3p. We further show that stem-loop miRNA Taqman RT-qPCR exhibits selectivity between 3'-isoforms, according to their length, and that this can lead to misinterpretation of results when these isoforms are differentially regulated. Collectively, and to our knowledge, this work constitutes the first demonstration that the stoichiometry of highly abundant templated 3'-isoforms of a same miRNA family can be dynamically regulated by a stimulus. Given that such 3'-isomiRs can have different functions, our study underlines the need to consider isomiRs when investigating miRNA-based regulation.

摘要

内源性 microRNAs(miRNAs)通常存在多种异构体(称为“isomiRs”),其 3'-端主要存在变异。越来越多的证据表明,同一家族的不同 isomiRs 可能具有不同的功能作用,最近就 miR-222-3p 3'-端变体的例子证明了这一点。虽然同一 miRNA 家族的 isomiR 水平在组织和细胞类型之间可能有所不同,但迄今为止尚未报道模板化 isomiR 化学计量比变化的刺激作用。在这里,我们依赖于小 RNA-seq 分析,证明干扰素(IFN)β刺激人成纤维细胞时,miR-222-3p 3'-端变体 >23 nt 特异性减少,而较短的异构体则幸免。这种长 miR-222-3p 3'-异构体和 >40 其他 miRNA 家族的长度依赖性动态调节在感染 Typhimurium 后在人单核细胞衍生的树突状细胞中得到了证实,强调了感染对 3'-长度调节的广泛程度,超出了 miR-222-3p 的例子。我们进一步表明,茎环 miRNA Taqman RT-qPCR 根据其长度在 3'-异构体之间具有选择性,并且当这些异构体存在差异调节时,这可能导致结果的误解。总之,据我们所知,这项工作首次证明了同一 miRNA 家族的高度丰富的模板化 3'-异构体的化学计量比可以被刺激动态调节。鉴于这种 3'-isomiRs 可能具有不同的功能,我们的研究强调了在研究 miRNA 为基础的调节时需要考虑 isomiRs。

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