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利用内含子微小RNA在体外和体内进行基因沉默

Gene silencing in vitro and in vivo using intronic microRNAs.

作者信息

Deng Jia Han, Deng Peter, Lin Shi-Lung, Ying Shao-Yao

机构信息

Department of Cell and Neurobiology, Keck School of Medicine, University of Southern California, Bishop Medical Teaching and Research Building 401, MCH51A, 1333 San Pablo Street, BMT-301, Los Angeles, CA, 90033, USA.

出版信息

Methods Mol Biol. 2015;1218:321-40. doi: 10.1007/978-1-4939-1538-5_20.

Abstract

MicroRNAs (miRNAs) are small, single-stranded noncoding RNAs important in many biological processes through posttranscriptional modification of complementary intracellular messenger RNAs (mRNAs). MiRNAs have been reported to induce RNA interference (RNAi), by utilizing the miRNA-induced silencing complex (miRISC) to target mRNAs. They were first discovered in Caenorhabditis elegans as native RNA fragments that modulate a wide range of genetic regulatory pathways during embryonic development, and are now recognized as small gene silencers transcribed from the noncoding regions of a genome. In humans, nearly 97 % of the genome is noncoding DNA and changes in these sequences are frequently noted to manifest in clinical and circumstantial malfunction; for example, type 2 myotonic dystrophy and fragile X syndrome were found to be associated with miRNAs derived from introns. Intronic miRNA (mirtrons) is a class of miRNAs derived from the processing of non-protein-coding regions of gene transcripts. The intronic miRNAs differ uniquely from previously described intergenic miRNAs in the requirement of RNA polymerase (Pol)-II and spliceosomal components for its biogenesis. Several kinds of intronic miRNAs have been identified in C. elegans, mouse, and human cells; however, their functions and applications have not been reported. It is notable that there are different, but still highly conserved, mirtrons in mammalian than in invertebrates, and could be an indication that mirtrons are an evolutionary precursor to existing miRNA biogenesis pathways. Here, we show that intron-derived miRNA is not only able to induce RNAi in mammalian cells but also in fish, chicken embryos, and adult mice cells, demonstrating the evolutionary preservation of this gene regulation system in vivo. These miRNA-mediated animal models provide artificial means to reproduce the mechanisms of miRNA-induced disease in vivo and will shed further light on miRNA-related therapies.

摘要

微小RNA(miRNA)是小的单链非编码RNA,通过对互补的细胞内信使RNA(mRNA)进行转录后修饰,在许多生物学过程中发挥重要作用。据报道,miRNA通过利用miRNA诱导沉默复合体(miRISC)靶向mRNA来诱导RNA干扰(RNAi)。它们最初是在秀丽隐杆线虫中作为天然RNA片段被发现的,这些片段在胚胎发育过程中调节广泛的基因调控途径,现在被认为是从基因组非编码区域转录而来的小基因沉默子。在人类中,近97%的基因组是非编码DNA,这些序列的变化经常被发现会在临床和环境功能障碍中表现出来;例如,发现2型强直性肌营养不良和脆性X综合征与来自内含子的miRNA有关。内含子miRNA(mirtrons)是一类从基因转录本的非蛋白质编码区域加工而来的miRNA。内含子miRNA在其生物发生对RNA聚合酶(Pol)-II和剪接体成分的需求方面,与先前描述的基因间miRNA有独特的不同。在秀丽隐杆线虫、小鼠和人类细胞中已经鉴定出几种内含子miRNA;然而,它们的功能和应用尚未见报道。值得注意的是,哺乳动物中的mirtrons与无脊椎动物中的不同,但仍然高度保守,这可能表明mirtrons是现有miRNA生物发生途径的进化前体。在这里,我们表明内含子衍生的miRNA不仅能够在哺乳动物细胞中诱导RNAi,而且在鱼类、鸡胚和成年小鼠细胞中也能诱导RNAi,这证明了这种基因调控系统在体内的进化保守性。这些miRNA介导的动物模型为在体内重现miRNA诱导疾病的机制提供了人工手段,并将进一步阐明与miRNA相关的治疗方法。

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