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双顺反子基因转移工具,用于递送 miRNA 和蛋白质编码序列。

Bicistronic gene transfer tools for delivery of miRNAs and protein coding sequences.

机构信息

Department of Biological Sciences, Purdue University, 915 W State St, West Lafayette, IN 47907-1392, USA.

出版信息

Int J Mol Sci. 2013 Sep 5;14(9):18239-55. doi: 10.3390/ijms140918239.

Abstract

MicroRNAs (miRNAs) are a category of small RNAs that modulate levels of proteins via post-transcriptional inhibition. Currently, a standard strategy to overexpress miRNAs is as mature miRNA duplexes, although this method is cumbersome if multiple miRNAs need to be delivered. Many of these miRNAs are found within introns and processed through the RNA polymerase II pathway. We have designed a vector to exploit this naturally-occurring intronic pathway to deliver the three members of the sensory-specific miR-183 family from an artificial intron. In one version of the vector, the downstream exon encodes the reporter (GFP) while another version encodes a fusion protein created between the transcription factor Atoh1 and the hemaglutinin epitope, to distinguish it from endogenous Atoh1. In vitro analysis shows that the miRNAs contained within the artificial intron are processed and bind to their targets with specificity. The genes downstream are successfully translated into protein and identifiable through immunofluorescence. More importantly, Atoh1 is proven functional through in vitro assays. These results suggest that this cassette allows expression of miRNAs and proteins simultaneously, which provides the opportunity for joint delivery of specific translational repressors (miRNA) and possibly transcriptional activators (transcription factors). This ability is attractive for future gene therapy use.

摘要

微小 RNA(miRNAs)是一类通过转录后抑制来调节蛋白质水平的小 RNA。目前,过表达 miRNAs 的标准策略是作为成熟 miRNA 双链体,但如果需要递送多个 miRNAs,则这种方法很繁琐。这些 miRNAs 中的许多存在于内含子中,并通过 RNA 聚合酶 II 途径进行加工。我们设计了一种载体,利用这种天然存在的内含子途径,从人工内含子中传递感觉特异性 miR-183 家族的三个成员。在该载体的一个版本中,下游外显子编码报告基因(GFP),而另一个版本则编码转录因子 Atoh1 和血凝素表位之间的融合蛋白,以将其与内源性 Atoh1 区分开来。体外分析表明,人工内含子中包含的 miRNAs 被加工并特异性结合其靶标。下游基因成功地翻译成蛋白质,并可通过免疫荧光进行鉴定。更重要的是,通过体外测定证实了 Atoh1 的功能。这些结果表明,该盒允许同时表达 miRNAs 和蛋白质,这为联合递送特定的翻译抑制剂(miRNA)和可能的转录激活剂(转录因子)提供了机会。这种能力对于未来的基因治疗应用很有吸引力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8119/3794778/ca5f2cebc068/ijms-14-18239f1.jpg

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