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dc.contributor.author고광석*
dc.date.accessioned2016-08-28T10:08:18Z-
dc.date.available2016-08-28T10:08:18Z-
dc.date.issued2013*
dc.identifier.issn0021-9738*
dc.identifier.otherOAK-9648*
dc.identifier.urihttps://dspace.ewha.ac.kr/handle/2015.oak/223340-
dc.description.abstractMicroRNAs (miRNAs) and methionine adenosyltransferase 1A (MAT1A) are dysregulated in hepatocellular carcinoma (HCC), and reduced MAT1A expression correlates with worse HCC prognosis. Expression of miR- 664, miR-485-3p, and miR-495, potential regulatory miRNAs of MAT1A, is increased in HCC. Knockdown of these miRNAs individually in Hep3B and HepG2 cells induced MAT1A expression, reduced growth, and increased apoptosis, while combined knockdown exerted additional effects on all parameters. Subcutaneous and intraparenchymal injection of Hep3B cells stably overexpressing each of this trio of miRNAs promoted tumorigenesis and metastasis in mice. Treatment with miRNA-664 (miR-664), miR-485-3p, and miR-495 siRNAs reduced tumor growth, invasion, and metastasis in an orthotopic liver cancer model. Blocking MAT1A induction significantly reduced the antitumorigenic effect of miR-495 siRNA, whereas maintaining MAT1A expression prevented miRNA-mediated enhancement of growth and metastasis. Knockdown of these miRNAs increased total and nuclear level of MAT1A protein, global CpG methylation, lin-28 homolog B (Caenorhabditis elegans) (LIN28B) promoter methylation, and reduced LIN28B expression. The opposite occurred with forced expression of these miRNAs. In conclusion, upregulation of miR-664, miR-485-3p, and miR-495 contributes to lower MAT1A expression in HCC, and enhanced tumorigenesis may provide potential targets for HCC therapy.*
dc.languageEnglish*
dc.titleMicroRNAs regulate methionine adenosyltransferase 1A expression in hepatocellular carcinoma*
dc.typeArticle*
dc.relation.issue1*
dc.relation.volume123*
dc.relation.indexSCI*
dc.relation.indexSCIE*
dc.relation.indexSCOPUS*
dc.relation.startpage285*
dc.relation.lastpage298*
dc.relation.journaltitleJournal of Clinical Investigation*
dc.identifier.doi10.1172/JCI63861*
dc.identifier.wosidWOS:000313598500033*
dc.identifier.scopusid2-s2.0-84873812316*
dc.author.googleYang H.*
dc.author.googleCho M.E.*
dc.author.googleLi T.W.H.*
dc.author.googlePeng H.*
dc.author.googleKo K.S.*
dc.author.googleMato J.M.*
dc.author.googleLu S.C.*
dc.contributor.scopusid고광석(25027852000)*
dc.date.modifydate20240301081003*


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