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首页> 外文期刊>Frontiers in Cell and Developmental Biology >Hypoxia-Induced LIN28A mRNA Promotes the Metastasis of Colon Cancer in a Protein-Coding-Independent Manner
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Hypoxia-Induced LIN28A mRNA Promotes the Metastasis of Colon Cancer in a Protein-Coding-Independent Manner

机译:缺氧诱导的LIN28a mRNA以蛋白质编码 - 独立的方式促进结肠癌转移

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The hypoxic microenvironment is beneficial to the metastasis but not to the proliferation of cancer cells. However, the mechanisms regarding to hypoxia differentially regulating cancer metastasis and proliferation are largely unknown. In this study, we revealed that hypoxia induced the expression of LIN28A at mRNA level but segregated LIN28A mRNAs in the P-bodies and thus inhibits the production of LIN28A protein. This unexpected finding suggests that there may be non-coding role for LIN28A mRNA in the progression of colon cancer. We further showed that the non-coding LIN28A mRNA promotes the metastasis but not proliferation of colon cancer cells in vitro and in vivo. Mechanistically, we revealed that Methionyl aminopeptidase 2 (METAP2) is one of the up-regulated metastasis regulators upon over-expression of non-coding LIN28A identified by mass spectrum, and confirmed that it is non-coding LIN28A mRNA instead of LIN28A protein promotes the expression of METAP2. Moreover, we demonstrated that knockdown of DICER abolished the promotional effects of non-coding LIN28A on the metastasis and METAP2 expression. Conclusively, we showed that hypoxia induces the production of LIN28A mRNAs but segregated them into the P-bodies together with miRNAs targeting both LIN28A and METAP2, and then promotes the metastasis by positively regulating the expression of METAP2. This study uncovered a distinctive role of hypoxia in manipulating the metastasis and proliferation by differently regulating the expression of LIN28A at mRNA and protein level.
机译:缺氧微环境有益于转移,但不适用于癌细胞的增殖。然而,关于缺氧差异调节癌症转移和增殖的机制在很大程度上是未知的。在这项研究中,我们揭示了缺氧在mRNA水平下诱导LIN28a的表达,但在p-体中分离LIN28a mRNA,因此抑制LIN28a蛋白的产生。这种意外的发现表明Lin28a mRNA在结肠癌进展中可能存在非编码作用。我们进一步表明,非编码LIN28A mRNA在体外和体内促进转移但不扩散结肠癌细胞。机械地,我们揭示了甲硫醇氨基肽酶2(Metap2)是通过质谱鉴定的非编码Lin28a的上调转移调节剂之一,并证实它是非编码LiN28a mRNA而不是Lin28a蛋白促进metap2的表达。此外,我们证明了Dicer的敲低取消了非编码LIN28a对转移和MetaP2表达的促进作用。最后,我们表明缺氧诱导林28A mRNA的生产,但与靶向LIN28A和METAP2的miRNA一起分离它们进入p-体,然后通过阳性调节Metap2的表达来促进转移。本研究通过不同地调节mRNA和蛋白质水平的不同调节LIN28a的表达来揭示缺氧在操纵转移和增殖中的独特作用。

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