微小RNA miR-27通过抑制SNAP25和TXN2的表达来抑制腺病毒感染。
MicroRNA miR-27 Inhibits Adenovirus Infection by Suppressing the Expression of SNAP25 and TXN2.
作者信息
Machitani Mitsuhiro, Sakurai Fuminori, Wakabayashi Keisaku, Nakatani Kosuke, Tachibana Masashi, Mizuguchi Hiroyuki
机构信息
Laboratory of Biochemistry and Molecular Biology, Graduate School of Pharmaceutical Sciences, Osaka University, Suita, Osaka, Japan.
Institute for Frontier Life and Medical Sciences, Kyoto University, Sakyo-ku, Kyoto, Japan.
出版信息
J Virol. 2017 May 26;91(12). doi: 10.1128/JVI.00159-17. Print 2017 Jun 15.
Recent studies have reported that host microRNAs (miRNAs) regulate infections by several types of viruses via various mechanisms and that inhibition of the miRNA processing factors enhances or prevents viral infection. However, it has not been clarified whether these effects of miRNAs extend to adenovirus (Ad) infection. Here we show that miR-27a and -b efficiently inhibit infection with an Ad via the downregulation of SNAP25 and TXN2, which are members of the SNARE proteins and the thioredoxin family, respectively. Approximately 80% reductions in Ad genomic copy number were found in cells transfected with miR-27a/b mimics, whereas there were approximately 2.5- to 5-fold larger copy numbers of the Ad genome following transfection with miR-27a/b inhibitors. Microarray gene expression analysis and analysis demonstrated that SNAP25 and TXN2 are target genes of miR-27a/b. A reporter assay using plasmids containing the 3' untranslated regions of the SNAP25 and TXN2 genes showed that miR-27a/b directly suppressed SNAP25 and TXN2 expression through posttranscriptional gene silencing. Knockdown of SNAP25 led to a significant inhibition of Ad entry into cells. Knockdown of TXN2 induced cell cycle arrest at G phase, leading to a reduction in Ad replication. In addition, overexpression of Ad-encoded small noncoding RNAs (VA-RNAs) restored the miR-27a/b-mediated reduction in infection level with a VA-RNA-lacking Ad mutant due to the VA-RNA-mediated inhibition of miR-27a/b expression. These results indicate that miR-27a and -b suppress SNAP25 and TXN2 expression via posttranscriptional gene silencing, leading to efficient suppression of Ad infection. Adenovirus (Ad) is widely used as a platform for replication-incompetent Ad vectors (Adv) and replication-competent oncolytic Ad (OAd) in gene therapy and virotherapy. Regulation of Ad infection is highly important for efficient gene therapies using both Adv and OAd. In this study, we demonstrate that miR-27a and -b, which are widely expressed in host cells, suppress SNAP25 and TXN2 expression through posttranscriptional gene silencing. Suppression of SNAP25 and TXN2 expression leads to inhibition of Ad entry into cells and to cell cycle arrest, respectively, leading to efficient suppression of Ad infection. Our findings provide important clues to the improvement of gene therapies using both Adv and OAd.
最近的研究报道,宿主微小RNA(miRNA)通过多种机制调节几种病毒的感染,并且抑制miRNA加工因子可增强或阻止病毒感染。然而,miRNA的这些作用是否扩展到腺病毒(Ad)感染尚未明确。在此,我们表明miR-27a和 -b通过下调SNAP25和TXN2有效抑制Ad感染,SNAP25和TXN2分别是可溶性N-乙基马来酰胺敏感因子附着蛋白受体(SNARE)蛋白家族和硫氧还蛋白家族的成员。在用miR-27a/b模拟物转染的细胞中,发现Ad基因组拷贝数减少了约80%,而在用miR-27a/b抑制剂转染后,Ad基因组的拷贝数增加了约2.5至5倍。基因芯片基因表达分析表明,SNAP25和TXN2是miR-27a/b的靶基因。使用含有SNAP25和TXN2基因3'非翻译区的质粒进行的报告基因检测表明,miR-27a/b通过转录后基因沉默直接抑制SNAP25和TXN2的表达。敲低SNAP25导致Ad进入细胞受到显著抑制。敲低TXN2诱导细胞周期在G期停滞,导致Ad复制减少。此外,Ad编码的小非编码RNA(VA-RNA)的过表达恢复了miR-27a/b介导的缺乏VA-RNA的Ad突变体感染水平的降低,这是由于VA-RNA介导的对miR-27a/b表达的抑制。这些结果表明,miR-27a和 -b通过转录后基因沉默抑制SNAP25和TXN2的表达,从而有效抑制Ad感染。腺病毒(Ad)在基因治疗和病毒治疗中被广泛用作无复制能力的Ad载体(Adv)和有复制能力的溶瘤Ad(OAd)的平台。Ad感染的调控对于使用Adv和OAd的高效基因治疗非常重要。在本研究中,我们证明在宿主细胞中广泛表达的miR-27a和 -b通过转录后基因沉默抑制SNAP25和TXN2的表达。SNAP25和TXN2表达的抑制分别导致Ad进入细胞受到抑制和细胞周期停滞,从而有效抑制Ad感染。我们的发现为改进使用Adv和OAd的基因治疗提供了重要线索。
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