Department of Urology, Norris Comprehensive Cancer Center, Keck School of Medicine, University of Southern California, NOR7346, 1441 Eastlake Ave., Los Angeles, CA 90089, USA.
Biochem Biophys Res Commun. 2011 Jul 29;411(2):276-80. doi: 10.1016/j.bbrc.2011.06.123. Epub 2011 Jun 24.
MicroRNAs (miRNAs) are ∼22nt non-coding RNA molecules that usually function as endogenous repressors of target genes. Many biological processes depend on faithful miRNA expression and miRNA profiling has revealed dysregulation of many miRNAs in neurological, and cardiovascular diseases, and in cancer. Despite this finding, most studies have focused on the function of single miRNAs or miRNA clusters. To better address physiologically relevant collaborative miRNA interactions, we developed a simple and flexible platform which expresses several miRNAs that have different genomic locations from a single transcript using endogenous pre-miRNA sequences. As a proof of principle we cloned the miR-34 tumor suppressor family and showed that the miR-34a/34b/34c vector expresses each miRNA at similar levels to individual miRNA containing vectors. Moreover, the miR-34a/34b/34c vector suppressed cell growth more than the individual miRNA vectors. We expect that this platform will be invaluable as a tool to study the complex and synergistic interactions of aberrantly expressed miRNAs in human diseases and may have applications for use in gene therapy.
微小 RNA(miRNAs)是约 22nt 的非编码 RNA 分子,通常作为靶基因的内源性抑制剂发挥作用。许多生物过程依赖于 miRNA 的忠实表达,miRNA 谱分析显示,许多 miRNA 在神经、心血管疾病和癌症中失调。尽管有了这一发现,但大多数研究仍集中在单个 miRNA 或 miRNA 簇的功能上。为了更好地解决与生理相关的协同 miRNA 相互作用,我们开发了一种简单灵活的平台,该平台使用内源性 pre-miRNA 序列从单个转录本中表达具有不同基因组位置的多个 miRNA。作为原理验证,我们克隆了 miR-34 肿瘤抑制因子家族,并表明 miR-34a/34b/34c 载体以与单个 miRNA 载体相似的水平表达每种 miRNA。此外,miR-34a/34b/34c 载体比单个 miRNA 载体更能抑制细胞生长。我们预计,该平台将成为研究人类疾病中异常表达 miRNA 的复杂协同相互作用的宝贵工具,并可能在基因治疗中有应用。
