Literature DB >> 18158134

Computational methods for analysis of cellular functions and pathways collectively targeted by differentially expressed microRNA.

Yuriy Gusev1.   

Abstract

This report presents computational methods of analysis of cellular processes, functions, and pathways affected by differentially expressed microRNA, a statistical basis of the gene enrichment analysis method, a modification of enrichment analysis method accounting for combinatorial targeting of Gene Ontology categories by multiple miRNAs and examples of the global functional profiling of predicted targets of differentially expressed miRNAs in cancer. We have also summarized an application of Ingenuity Pathway Analysis tools for in depth analysis of microRNA target sets that may be useful for the biological interpretation of microRNA profiling data. To illustrate the utility of these methods, we report the main results of our recent computational analysis of five published datasets of aberrantly expressed microRNAs in five human cancers (pancreatic cancer, breast cancer, colon cancer, lung cancer, and lymphoma). Using a combinatorial target prediction algorithm and statistical enrichment analysis, we have determined Gene Ontology categories as well as biological functions, disease categories, toxicological categories, and signaling pathways that are: targeted by multiple microRNAs; statistically significantly enriched with target genes; and known to be affected in specific cancers. Our recent computational analysis of predicted targets of co-expressed miRNAs in five human cancers suggests that co-expressed miRNAs provide systemic compensatory response to the abnormal phenotypic changes in cancer cells by targeting a broad range of functional categories and signaling pathways reportedly affected in a particular cancer.

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Year:  2008        PMID: 18158134     DOI: 10.1016/j.ymeth.2007.10.005

Source DB:  PubMed          Journal:  Methods        ISSN: 1046-2023            Impact factor:   3.608


  40 in total

1.  Computational methods for the identification of microRNA targets.

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Journal:  Open Access Bioinformatics       Date:  2010-05-01

2.  MiR-15b and miR-152 reduce glioma cell invasion and angiogenesis via NRP-2 and MMP-3.

Authors:  Xuguang Zheng; Michael Chopp; Yong Lu; Benjamin Buller; Feng Jiang
Journal:  Cancer Lett       Date:  2012-11-07       Impact factor: 8.679

3.  Development of a robust, low cost stem-loop real-time quantification PCR technique for miRNA expression analysis.

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Journal:  Mol Biol Rep       Date:  2013-01-10       Impact factor: 2.316

Review 4.  Concise review: new frontiers in microRNA-based tissue regeneration.

Authors:  Jessica E Frith; Enzo R Porrello; Justin J Cooper-White
Journal:  Stem Cells Transl Med       Date:  2014-05-29       Impact factor: 6.940

5.  MicroRNA-19 (miR-19) regulates tissue factor expression in breast cancer cells.

Authors:  Xiaoxi Zhang; Haijun Yu; Jessica R Lou; Jie Zheng; Hua Zhu; Narcis-Ioan Popescu; Florea Lupu; Stuart E Lind; Wei-Qun Ding
Journal:  J Biol Chem       Date:  2010-11-08       Impact factor: 5.157

Review 6.  MicroRNA in pancreatic cancer: pathological, diagnostic and therapeutic implications.

Authors:  Satyanarayana Rachagani; Sushil Kumar; Surinder K Batra
Journal:  Cancer Lett       Date:  2009-12-09       Impact factor: 8.679

7.  Characterization of global microRNA expression reveals oncogenic potential of miR-145 in metastatic colorectal cancer.

Authors:  Greg M Arndt; Lesley Dossey; Lara M Cullen; Angela Lai; Riki Druker; Michael Eisbacher; Chunyan Zhang; Nham Tran; Hongtao Fan; Kathy Retzlaff; Anton Bittner; Mitch Raponi
Journal:  BMC Cancer       Date:  2009-10-20       Impact factor: 4.430

8.  MicroRNA and mRNA integrated analysis (MMIA): a web tool for examining biological functions of microRNA expression.

Authors:  Seungyoon Nam; Meng Li; Kwangmin Choi; Curtis Balch; Sun Kim; Kenneth P Nephew
Journal:  Nucleic Acids Res       Date:  2009-05-06       Impact factor: 16.971

9.  Exosomes from docetaxel-resistant breast cancer cells alter chemosensitivity by delivering microRNAs.

Authors:  Wei-Xian Chen; Yan-Qin Cai; Meng-Meng Lv; Lin Chen; Shan-Liang Zhong; Teng-Fei Ma; Jian-Hua Zhao; Jin-Hai Tang
Journal:  Tumour Biol       Date:  2014-06-27

10.  Moderate strength (0.23-0.28 T) static magnetic fields (SMF) modulate signaling and differentiation in human embryonic cells.

Authors:  Zhiyun Wang; Anshu Sarje; Pao-Lin Che; Kevin J Yarema
Journal:  BMC Genomics       Date:  2009-08-04       Impact factor: 3.969

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