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首页> 外文期刊>Journal of cellular and molecular medicine. >miR24‐2 accelerates progression of liver cancer cells by activating Pim1 through tri‐methylation of Histone H3 on the ninth lysine
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miR24‐2 accelerates progression of liver cancer cells by activating Pim1 through tri‐methylation of Histone H3 on the ninth lysine

机译:通过在第九赖氨酸上通过组织H3的三甲基化激活PIM1来加速肝癌细胞的进展

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Several microRNAs are associated with carcinogenesis and tumour progression. Herein, our observations suggest both miR24‐2 and Pim1 are up‐regulated in human liver cancers, and miR24‐2 accelerates growth of liver cancer cells in vitro and in vivo. Mechanistically, miR24‐2 increases the expression of N6‐adenosine‐methyltransferase METTL3 and thereafter promotes the expression of miR6079 via RNA methylation modification. Furthermore, miR6079 targets JMJD2A and then increased the tri‐methylation of histone H3 on the ninth lysine (H3K9me3). Therefore, miR24‐2 inhibits JMJD2A by increasing miR6079 and then increases H3K9me3. Strikingly, miR24‐2 increases the expression of Pim1 dependent on H3K9me3 and METTL3. Notably, our findings suggest that miR24‐2 alters several related genes (pHistone H3, SUZ12, SUV39H1, Nanog, MEKK4, pTyr) and accelerates progression of liver cancer cells through Pim1 activation. In particular, Pim1 is required for the oncogenic action of miR24‐2 in liver cancer. This study elucidates a novel mechanism for miR24‐2 in liver cancer and suggests that miR24‐2 may be used as novel therapeutic targets of liver cancer.
机译:几个microRNAS与致癌和肿瘤进展相关。在此,我们的观察结果表明MiR24-2和PIM1在人肝癌中占据上调,MiR24-2在体外和体内加速肝癌细胞的生长。机械地,MiR24-2增加了N6-腺苷 - 甲基转移酶MetT13的表达,然后通过RNA甲基化改性促进miR6079的表达。此外,MIR6079靶向JMJD2A,然后在第九赖氨酸(H3K9ME3)上增加组蛋白H3的三甲基化。因此,MiR24-2通过增加MiR6079抑制JMJD2A,然后增加H3K9ME3。尖锐的是,MiR24-2增加了PIM1的表达依赖于H3K9ME3和MetT13。值得注意的是,我们的研究结果表明MiR24-2改变了几种相关基因(磷氨锡H3,SUZ12,SUV39H1,Nanog,Mekk4,Ptyr),并通过PIM1活化加速肝癌细胞的进展。特别是,PIM1需要MIR24-2在肝癌中的致癌作用。本研究阐明了肝癌中MiR24-2的新机制,并表明MIR24-2可用作肝癌的新疗法靶标。

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