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miR-106b-responsive gene landscape identifies regulation of Kruppel-like factor family

机译:miR-106b响应基因景观识别Kruppel样因子家族的调节

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摘要

MicroRNA dysregulation is a common feature of cancer and due to the promiscuity of microRNA binding this can result in a wide array of genes whose expression is altered. miR-106b is an oncomiR overexpressed in cholangiocarcinoma and its upregulation in this and other cancers often leads to repression of anti-tumorigenic targets. The goal of this study was to identify the miR-106b-regulated gene landscape in cholangiocarcinoma cells using a genome-wide, unbiased mRNA analysis. Through RNA-Seq we found 112 mRNAs significantly repressed by miR-106b. The majority of these genes contain the specific miR-106b seed-binding site. We have validated 11 genes from this set at the mRNA level and demonstrated regulation by miR-106b of 7 proteins. Combined analysis of our miR-106b-regulated mRNA data set plus published reports indicate that miR-106b binding is anchored by G: C pairing in and near the seed. Novel targets Kruppel-like factor 2 (KLF2) and KLF6 were verified both at the mRNA and at the protein level. Further investigation showed regulation of four other KLF family members by miR-106b. We have discovered coordinated repression of multiple members of the KLF family by miR-106b that may play a role in cholangiocarcinoma tumor biology.
机译:MicroRNA失除量是癌症的常见特征,并且由于MicroRNA结合的滥交,这可能导致各种基因阵列的表达被改变。 miR-106b是胆管癌中过表达的腹腔,其上调和其他癌症通常会导致抑制抗致致致致致致致致致致致致毒性的靶标。本研究的目的是使用基因组 - 宽的未偏见的mRNA分析来鉴定胆管癌细胞中的miR-106b调节基因景观。通过RNA-SEQ,我们发现112 MRNA被MIR-106B显着压抑。这些基因的大多数含有特定的miR-106b种子结合位点。我们已经从该组合的MRNA水平验证了11个基因,并通过7个蛋白质的miR-106b进行了调节。我们的miR-106b调节mRNA数据集的综合分析加上已公布的报告表明MIR-106B结合由G:C在种子内部和附近锚定。新型靶标Kruppel样因子2(KLF2)和KLF6在mRNA和蛋白质水平验证。进一步调查显示MIR-106B对另外四个KLF家族成员的调节。我们已经发现了MIR-106B的多个成员的协调镇压,可能在胆管癌肿瘤生物学中发挥作用。

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