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      Thousands of novel translated open reading frames in humans inferred by ribosome footprint profiling

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          Abstract

          Accurate annotation of protein coding regions is essential for understanding how genetic information is translated into biological functions. Here we describe riboHMM, a new method that uses ribosome footprint data along with gene expression and sequence information to accurately infer translated sequences. We applied our method to human lymphoblastoid cell lines and identified 7,273 previously unannotated coding sequences, including 2,442 translated upstream open reading frames. We observed an enrichment of harringtonine-treated ribosome footprints at the inferred initiation sites, validating many of the novel coding sequences. The novel sequences exhibit significant signatures of selective constraint in the reading frames of the inferred proteins, suggesting that many of these are functional. Nearly 40% of bicistronic transcripts showed significant negative correlation in the levels of translation of their two coding sequences, suggesting a key regulatory role for these novel translated sequences. Our work significantly expands the set of known coding regions in humans.

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          Author and article information

          Journal
          bioRxiv
          November 13 2015
          Article
          10.1101/031617
          3da7e75b-c88c-47c9-97b0-caebf8f7d82c
          © 2015
          History

          Human biology,Genetics
          Human biology, Genetics

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