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Keywords {🔍}

mirnas, lin, expression, cells, article, google, scholar, human, mouse, mirna, neuronal, organs, expressed, differentiation, cell, rna, ntd, northern, mammalian, gene, development, brain, figure, levels, biol, data, organ, detected, micrornas, conserved, predicted, utr, profiles, analysis, neurons, similar, target, cloned, brainexpressed, ambros, genes, treated, role, small, regulation, muscle, embryonal, regulatory, downregulation, sequence,

Topics {✒️}

mir-23b~mir-27b~mir-24/mir-189 exhibited [α-32p]-datp 6000 ci/mmol mir-23b~mir-27b~mir-24/mir-189 chronic lymphocytic leukemia aggressive b-cell leukemia pro-apoptotic gene hid health grant t32-ca09658 shared cis-regulatory elements mir-1d~mir-133 hairpin precursors article number r13 additional data file dartmouth-hitchcock medical center retinoic acid induces micro-rna genes mir15 size-selected rna libraries broad-complex gene activity trans-retinoic acid mir-142s/mir-142as nt2/d1 cell lines controls cell proliferation ian pitha-rowe ra-induced differentiation parallels references lagos-quintana controls temporal patterning nt2/d1 cells treated gene regulatory networks tumor suppressor gene privacy choices/manage cookies brain-enriched mirnas compared identify additional classes represent closely linked embryonal carcinoma cells trigger transcript degradation pluripotent cell state native lin-28 gene neuron-expressed mir-125b human embryonal carcinoma related subjects testing 20-nts segments biotechnology information[http dartmouth medical school skeletal muscle-enriched mirnas microrna-298-5p released supplementary regulatory role closely linked mirnas developmentally regulated microrna full size image representative ra-induced mirnas rna-rna interaction northern blot analysis

Schema {🗺️}

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         headline:Expression profiling of mammalian microRNAs uncovers a subset of brain-expressed microRNAs with possible roles in murine and human neuronal differentiation
         description:The microRNAs (miRNAs) are an extensive class of small noncoding RNAs (18 to 25 nucleotides) with probable roles in the regulation of gene expression. In Caenorhabditis elegans, lin-4 and let-7 miRNAs control the timing of fate specification of neuronal and hypodermal cells during larval development. lin-4, let-7 and other miRNA genes are conserved in mammals, and their potential functions in mammalian development are under active study. In order to identify mammalian miRNAs that might function in development, we characterized the expression of 119 previously reported miRNAs in adult organs from mouse and human using northern blot analysis. Of these, 30 miRNAs were specifically expressed or greatly enriched in a particular organ (brain, lung, liver or skeletal muscle). This suggests organ- or tissue-specific functions for miRNAs. To test if any of the 66 brain-expressed miRNAs were present in neurons, embryonal carcinoma cells were treated with all-trans-retinoic acid to promote neuronal differentiation. A total of 19 brain-expressed miRNAs (including lin-4 and let-7 orthologs) were coordinately upregulated in both human and mouse embryonal carcinoma cells during neuronal differentiation. The mammalian ortholog of C. elegans lin-28, which is downregulated by lin-4 in worms via 3' untranslated region binding, was also repressed during neuronal differentiation of mammalian embryonal carcinoma cells. Mammalian lin-28 messenger RNAs contain conserved predicted binding sites in their 3' untranslated regions for neuron-expressed miR-125b (a lin-4 ortholog), let-7a, and miR-218. The identification of a subset of brain-expressed miRNAs whose expression behavior is conserved in both mouse and human differentiating neurons implicates these miRNAs in mammalian neuronal development or function.
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      headline:Expression profiling of mammalian microRNAs uncovers a subset of brain-expressed microRNAs with possible roles in murine and human neuronal differentiation
      description:The microRNAs (miRNAs) are an extensive class of small noncoding RNAs (18 to 25 nucleotides) with probable roles in the regulation of gene expression. In Caenorhabditis elegans, lin-4 and let-7 miRNAs control the timing of fate specification of neuronal and hypodermal cells during larval development. lin-4, let-7 and other miRNA genes are conserved in mammals, and their potential functions in mammalian development are under active study. In order to identify mammalian miRNAs that might function in development, we characterized the expression of 119 previously reported miRNAs in adult organs from mouse and human using northern blot analysis. Of these, 30 miRNAs were specifically expressed or greatly enriched in a particular organ (brain, lung, liver or skeletal muscle). This suggests organ- or tissue-specific functions for miRNAs. To test if any of the 66 brain-expressed miRNAs were present in neurons, embryonal carcinoma cells were treated with all-trans-retinoic acid to promote neuronal differentiation. A total of 19 brain-expressed miRNAs (including lin-4 and let-7 orthologs) were coordinately upregulated in both human and mouse embryonal carcinoma cells during neuronal differentiation. The mammalian ortholog of C. elegans lin-28, which is downregulated by lin-4 in worms via 3' untranslated region binding, was also repressed during neuronal differentiation of mammalian embryonal carcinoma cells. Mammalian lin-28 messenger RNAs contain conserved predicted binding sites in their 3' untranslated regions for neuron-expressed miR-125b (a lin-4 ortholog), let-7a, and miR-218. The identification of a subset of brain-expressed miRNAs whose expression behavior is conserved in both mouse and human differentiating neurons implicates these miRNAs in mammalian neuronal development or function.
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         Plant Genetics and Genomics
         Microbial Genetics and Genomics
         Bioinformatics
         Evolutionary Biology
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