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首页> 外文期刊>Nucleic Acid Therapeutics >The Regulatory Network Menin-MicroRNA 26a As a Possible Target forTI The Regulatory Network Menin-MicroRNA 26a As a Possible Target for RNA-Based Therapy of Bone Diseases
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The Regulatory Network Menin-MicroRNA 26a As a Possible Target forTI The Regulatory Network Menin-MicroRNA 26a As a Possible Target for RNA-Based Therapy of Bone Diseases

机译:监管网络Menin-MicroRNA 26A作为可能的目标Forti调节网络Menin-MicroRNA 26a作为骨病RNA治疗的可能靶标

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摘要

MicroRNAs (miRNAs) are post-transcriptional regulators of gene expression, interplaying with transcription factors in complex regulatory networks. Menin is the product of the MEN1 oncosuppressor gene, responsible for multiple endocrine neoplasia type 1 syndrome. Recent data suggest that menin functions as a general regulator of transcription. Menin expression modulates mesenchymal cell commitment to the myogenic or osteogenic lineages. The microRNA 26a (miR-26a) modulates the expression of SMAD1 protein during the osteoblastic differentiation of human adipose tissue-derived stem cells (hADSCs). We used siRNA silencing against MEN1 mRNA and pre-miR-26 mimics to study the interplay between them and to investigate the interplay between menin and miR-26a as regulators of osteogenic differentiation in the hADSCs. We found that in hADSCs the siRNA-induced silencing of MEN1 mRNA resulted in a down regulation of miR-26a, with a consequent upregulation of SMAD1 protein. Chromatin immunoprecipitation (ChIP) showed that menin occupies the miR-26-a gene promoter, thus inducing its expression and confirming that menin is a positive regulator of miR-26a. In conclusion, results from this study evidenced, for the first time, a direct interaction between menin transcription factor and miRNA, interaction that seems to play a pivotal role during the hADSCs osteogenesis, thus suggesting a novel target for bone disease RNA-based therapy.
机译:MicroRNAs(miRNA)是基因表达后转录调节因子,与复杂的监管网络中的转录因子相互作用。 Menin是MEN1 oncosup压抑器基因的产物,负责多种内分泌瘤形成1型综合征。最近的数据表明Menin用作转录的一般调节器。 menin表达调节对肌原素或骨质发生谱系的间充质细胞承诺。 MicroRNA 26a(miR-26a)在人脂肪组织衍生的干细胞(HADSCs)的骨细胞分化期间调节SMAD1蛋白的表达。我们使用SiRNA对Men1 mRNA和预先模仿的MIRNA沉默,以研究它们之间的相互作用,并调查Menin和MiR-26a之间的相互作用作为HADSCs中的骨质发生分化的调节因子。我们发现,在HADSCS中,SiRNA诱导的MEN1 mRNA的沉默导致miR-26a的调节,随后对Smad1蛋白的上调。染色质免疫沉淀(芯片)显示Menin占据MiR-26-A基因启动子,从而诱导其表达并证实Menin是miR-26a的阳性调节剂。总之,这项研究的结果首次证明了Menin转录因子和miRNA之间的直接相互作用,似乎在HADSCS骨质发生过程中发挥关键作用的相互作用,因此表明了一种基于骨病RNA治疗的新靶点。

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