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    Date Issued2016 (1)2011 (1)2007 (1)Author
    Liu, X. Shirley (3)
    Rinn, John L. (2)Adams, David J. (1)Berger, Bonnie (1)Brown, Myles (1)View MoreUMass Chan AffiliationDepartment of Molecular Genetics and Microbiology (1)Department of Pathology (1)Department of Pediatric Oncology (1)Program in Gene Function and Expression (1)Program in Molecular Medicine (1)Document TypeJournal Article (3)KeywordAlu Elements; Base Sequence; *Gene Duplication; Humans; In Situ Hybridization, Fluorescence; Leukemia-Lymphoma, Adult T-Cell; Models, Biological; Models, Genetic; Molecular Sequence Data; Nucleic Acid Hybridization; Polymerase Chain Reaction; Proto-Oncogene Proteins c-myb; Recombination, Genetic (1)Cancer Biology (1)Genetics and Genomics (1)Genomics (1)Life Sciences (1)View MoreJournalGenome biology (1)Nature communications (1)The Journal of experimental medicine (1)

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    Integrative analyses reveal a long noncoding RNA-mediated sponge regulatory network in prostate cancer

    Du, Zhou; Sun, Tong; Hacisuleyman, Ezgi; Fei, Teng; Wang, Xiaodong; Brown, Myles; Rinn, John L.; Lee, Mary Gwo-Shu; Chen, Yiwen; Kantoff, Philip W.; et al. (2016-03-15)
    Mounting evidence suggests that long noncoding RNAs (lncRNAs) can function as microRNA sponges and compete for microRNA binding to protein-coding transcripts. However, the prevalence, functional significance and targets of lncRNA-mediated sponge regulation of cancer are mostly unknown. Here we identify a lncRNA-mediated sponge regulatory network that affects the expression of many protein-coding prostate cancer driver genes, by integrating analysis of sequence features and gene expression profiles of both lncRNAs and protein-coding genes in tumours. We confirm the tumour-suppressive function of two lncRNAs (TUG1 and CTB-89H12.4) and their regulation of PTEN expression in prostate cancer. Surprisingly, one of the two lncRNAs, TUG1, was previously known for its function in polycomb repressive complex 2 (PRC2)-mediated transcriptional regulation, suggesting its sub-cellular localization-dependent function. Our findings not only suggest an important role of lncRNA-mediated sponge regulation in cancer, but also underscore the critical influence of cytoplasmic localization on the efficacy of a sponge lncRNA.
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    Genomics in 2011: challenges and opportunities

    Adams, David J.; Berger, Bonnie; Harismendy, Olivier; Huttenhower, Curtis; Liu, X. Shirley; Myers, Chad L.; Oshlack, Alicia; Rinn, John L.; Walhout, Albertha J. M. (2011-12-28)
    As we come to the end of 2011, Genome Biology has asked some members of our Editorial Board for their views on the state of play in genomics. What was their favorite paper of 2011? What are the challenges in their particular research area? Who has had the biggest influence on their careers? What advice would they give to young researchers embarking on a career in research?
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    Alu elements mediate MYB gene tandem duplication in human T-ALL

    O'Neil, Jennifer Elinor; Tchinda, Joelle; Gutierrez, Alejandro; Moreau, Lisa A.; Maser, Richard S.; Wong, Kwok-Kin; Li, Wei; McKenna, Keith; Liu, X. Shirley; Feng, Bin; et al. (2007-12-12)
    Recent studies have demonstrated that the MYB oncogene is frequently duplicated in human T cell acute lymphoblastic leukemia (T-ALL). We find that the human MYB locus is flanked by 257-bp Alu repeats and that the duplication is mediated somatically by homologous recombination between the flanking Alu elements on sister chromatids. Nested long-range PCR analysis indicated a low frequency of homologous recombination leading to MYB tandem duplication in the peripheral blood mononuclear cells of approximately 50% of healthy individuals, none of whom had a MYB duplication in the germline. We conclude that Alu-mediated MYB tandem duplication occurs at low frequency during normal thymocyte development and is clonally selected during the molecular pathogenesis of human T-ALL.
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