E2F6 通过靶向 miR-5000-3p/FBXW7 轴下调 MIR22HG 促进喉癌的进展。

E2F6-Mediated Downregulation of MIR22HG Facilitates the Progression of Laryngocarcinoma by Targeting the miR-5000-3p/FBXW7 Axis.

机构信息

I. M. Sechenov First Moscow State Medical University, Moscow, Russian Federation.

N. N. Blokhin National Medical Research Center of the Oncology of the Ministry of Health of the Russian Federation, Moscow, Russian Federation

出版信息

Mol Cell Biol. 2020 Apr 28;40(10). doi: 10.1128/MCB.00496-19.

DOI:10.1128/MCB.00496-19

PMID:32094308

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7189097/

Abstract

Recently, abundant evidence has clarified that long noncoding RNAs (lncRNAs) play an oncogenic or anticancer role in the tumorigenesis and development of diverse human cancers. Described as a crucial regulator in some cancers, MIR22HG has not yet been studied in laryngocarcinoma and therefore the underlying regulatory role of MIR22HG in laryngocarcinoma is worth detecting. In this study, MIR22HG expression in laryngocarcinoma cells was confirmed to be downregulated, and upregulated MIR22HG expression led to suppressive effects on laryngocarcinoma cell proliferation and migration. Molecular mechanism assays revealed that MIR22HG sponges miR-5000-3p in laryngocarcinoma cells. Besides, decreased expression of miR-5000-3p suppressed laryngocarcinoma cell proliferation and migration. Moreover, the FBXW7 gene was reported to be a downstream target gene of miR-5000-3p in laryngocarcinoma cells. More importantly, rescue assays verified that FBXW7 depletion or miR-5000-3p upregulation countervailed the repressive effects of MIR22HG overexpression on laryngocarcinoma progression. In addition, E2F6 was proved to be capable of inhibiting MIR22HG transcription in laryngocarcinoma cells. To sum up, E2F6-induced downregulation of MIR22HG promotes laryngocarcinoma progression through the miR-5000-3p/FBXW7 axis.

摘要

最近，大量证据表明长非编码 RNA（lncRNA）在多种人类癌症的发生和发展中发挥致癌或抗癌作用。MIR22HG 被描述为某些癌症中的关键调节剂，但在喉癌中尚未进行研究，因此检测 MIR22HG 在喉癌中的潜在调节作用是值得的。在这项研究中，证实 MIR22HG 在喉癌细胞中的表达下调，上调 MIR22HG 的表达导致喉癌细胞增殖和迁移受到抑制。分子机制分析表明，MIR22HG 在喉癌细胞中作为 miR-5000-3p 的海绵分子。此外，miR-5000-3p 的表达下调抑制了喉癌细胞的增殖和迁移。此外，据报道，FBXW7 基因是 miR-5000-3p 在喉癌细胞中的下游靶基因。更重要的是，挽救实验验证了 FBXW7 缺失或 miR-5000-3p 上调抵消了 MIR22HG 过表达对喉癌进展的抑制作用。此外，已经证明 E2F6 能够抑制喉癌细胞中 MIR22HG 的转录。总之，E2F6 诱导的 MIR22HG 下调通过 miR-5000-3p/FBXW7 轴促进喉癌的进展。

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