Mirna expression profiles identify drivers in colorectal and pancreatic cancers |
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| Authors: | Piepoli Ada Tavano Francesca Copetti Massimiliano Mazza Tommaso Palumbo Orazio Panza Anna di Mola Francesco Fabio Pazienza Valerio Mazzoccoli Gianluigi Biscaglia Giuseppe Gentile Annamaria Mastrodonato Nicola Carella Massimo Pellegrini Fabio di Sebastiano Pierluigi Andriulli Angelo |
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| Affiliation: | Department and Laboratory of Gastroenterology, IRCCS Casa Sollievo della Sofferenza, Research Hospital, San Giovanni Rotondo, Italy. a.piepoli@operapadrepio.it |
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| Abstract: | Background and AimAltered expression of microRNAs (miRNAs) hallmarks many cancer types. The study of the associations of miRNA expression profile and cancer phenotype could help identify the links between deregulation of miRNA expression and oncogenic pathways.MethodsExpression profiling of 866 human miRNAs in 19 colorectal and 17 pancreatic cancers and in matched adjacent normal tissues was investigated. Classical paired t-test and random forest analyses were applied to identify miRNAs associated with tissue-specific tumors. Network analysis based on a computational approach to mine associations between cancer types and miRNAs was performed.ResultsThe merge between the two statistical methods used to intersect the miRNAs differentially expressed in colon and pancreatic cancers allowed the identification of cancer-specific miRNA alterations. By miRNA-network analysis, tissue-specific patterns of miRNA deregulation were traced: the driving miRNAs were miR-195, miR-1280, miR-140-3p and miR-1246 in colorectal tumors, and miR-103, miR-23a and miR-15b in pancreatic cancers.ConclusionMiRNA expression profiles may identify cancer-specific signatures and potentially useful biomarkers for the diagnosis of tissue specific cancers. miRNA-network analysis help identify altered miRNA regulatory networks that could play a role in tumor pathogenesis. |
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