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Improved Ribo-seq enables identification of cryptic translation events.

Florian ErhardAnne HaleniusCosima ZimmermannAnne L'HernaultDaniel J KowalewskiMichael P WeekesStefan StevanovicRalf ZimmerLars Dölken
Published in: Nature methods (2018)
Ribosome profiling has been used to predict thousands of short open reading frames (sORFs) in eukaryotic cells, but it suffers from substantial levels of noise. PRICE (https://github.com/erhard-lab/price) is a computational method that models experimental noise to enable researchers to accurately resolve overlapping sORFs and noncanonical translation initiation. We experimentally validated translation using major histocompatibility complex class I (MHC I) peptidomics and observed that sORF-derived peptides efficiently enter the MHC I presentation pathway and thus constitute a substantial fraction of the antigen repertoire.
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