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Novel small RNA expression libraries uncover hsa-miR-30b and hsa-miR-30c as important factors in anoikis resistance

机译:新颖的小RNA表达文库揭示了hsa-miR-30b和hsa-miR-30c是耐厌氧症的重要因素

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MicroRNAs (miRNAs) have been widely studied in order to elucidate their biological functions. MicroRNA microarrays or miRNA overexpression libraries generated by synthesis and cloning of individual miRNAs have been used to study their different roles. In this work, we have developed a novel methodology to express mature miRNAs and other small RNAs from a double convergent RNA polymerase III promoter. We show that the generated miRNAs function similarly to those processed from primary transcripts or pri-miRNAs. This system allowed us to produce a lentiviral library expressing the whole population of small RNAs present in a metastatic cell line. A functional screening using this library led to the identification of hsa-miR-30b and hsa-miR-30c as negative regulators of cell death induced by loss of attachment (anoikis). Importantly, we demonstrated that the acquisition of anoikis resistance via these miRNAs is achieved through down-regulation of caspase 3 expression. Moreover, overexpression of these miRNAs resulted in a decrease of other types of caspase 3-dependent cell death and enhanced the survival of MCF10A acinar cells in morphogenesis assays, suggesting a putative role as oncomirs. In summary, this novel methodology provides a powerful and effective way for identifying novel small RNAs involved in a particular biological process.
机译:为了阐明其生物学功能,对MicroRNA(miRNA)进行了广泛的研究。通过合成和克隆单个miRNA生成的MicroRNA微阵列或miRNA过表达文库已用于研究它们的不同作用。在这项工作中,我们开发了一种新的方法,可以从双聚合RNA聚合酶III启动子表达成熟的miRNA和其他小RNA。我们表明,生成的miRNA的功能类似于从原始转录本或pri-miRNA加工的那些。该系统使我们能够产生慢病毒文库,该文库表达转移细胞系中存在的全部小RNA。使用该文库的功能筛选导致鉴定了hsa-miR-30b和hsa-miR-30c作为由附着丧失引起的细胞死亡的负调节剂(无神经)。重要的是,我们证明了通过下调caspase 3表达可以实现通过这些miRNA的耐缺氧能力。此外,这些miRNA的过表达导致其他类型的半胱天冬酶3依赖性细胞死亡减少,并在形态发生测定中提高了MCF10A腺泡细胞的存活率,表明其可能作为癌基因。总而言之,这种新颖的方法为鉴定涉及特定生物学过程的新颖小RNA提供了一种强大而有效的方法。

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