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      Evolutionary Dynamics of Gene and Isoform Regulation in Mammalian Tissues

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      Science
      American Association for the Advancement of Science (AAAS)

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          Abstract

          Most mammalian genes produce multiple distinct messenger RNAs through alternative splicing, but the extent of splicing conservation is not clear. To assess tissue-specific transcriptome variation across mammals, we sequenced complementary DNA from nine tissues from four mammals and one bird in biological triplicate, at unprecedented depth. We find that while tissue-specific gene expression programs are largely conserved, alternative splicing is well conserved in only a subset of tissues and is frequently lineage-specific. Thousands of previously unknown, lineage-specific, and conserved alternative exons were identified; widely conserved alternative exons had signatures of binding by MBNL, PTB, RBFOX, STAR, and TIA family splicing factors, implicating them as ancestral mammalian splicing regulators. Our data also indicate that alternative splicing often alters protein phosphorylatability, delimiting the scope of kinase signaling.

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          Author and article information

          Journal
          Science
          Science
          American Association for the Advancement of Science (AAAS)
          0036-8075
          1095-9203
          December 20 2012
          December 21 2012
          December 20 2012
          December 21 2012
          : 338
          : 6114
          : 1593-1599
          Article
          10.1126/science.1228186
          3568499
          23258891
          0df4a285-f5fe-4c43-a1a9-b3c357f4c11a
          © 2012
          History

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