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Published July 3, 2013 | Accepted Version
Journal Article Open

Ribosome Profiling Provides Evidence that Large Noncoding RNAs Do Not Encode Proteins

Abstract

Large noncoding RNAs are emerging as an important component in cellular regulation. Considerable evidence indicates that these transcripts act directly as functional RNAs rather than through an encoded protein product. However, a recent study of ribosome occupancy reported that many large intergenic ncRNAs (lincRNAs) are bound by ribosomes, raising the possibility that they are translated into proteins. Here, we show that classical noncoding RNAs and 5′ UTRs show the same ribosome occupancy as lincRNAs, demonstrating that ribosome occupancy alone is not sufficient to classify transcripts as coding or noncoding. Instead, we define a metric based on the known property of translation whereby translating ribosomes are released upon encountering a bona fide stop codon. We show that this metric accurately discriminates between protein-coding transcripts and all classes of known noncoding transcripts, including lincRNAs. Taken together, these results argue that the large majority of lincRNAs do not function through encoded proteins.

Additional Information

© 2013 Elsevier Inc. Received: January 9, 2013; Revised: June 7, 2013; Accepted: June 10, 2013; Published: June 27, 2013. We thank Manuel Garber and John Rinn for helpful discussions and thoughtful comments on the manuscript, Moran Cabili and Jesse Engreitz for critical reading and suggestions on the manuscript, Alex Shishkin for generating the non-polyA-selected RNA-seq libraries, Shari Grossman for help with population-level dN/dS calculations, and Leslie Gaffney for assistance with figures. This work was funded by an NIH Director's Early Independence Award (DP5OD012190 to M.G.), NHGRI (U54HG003067 to E.S.L.), and funds from the Broad Institute of MIT and Harvard.

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Created:
August 19, 2023
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October 24, 2023