Summary
Translation is the process by which ribosomes synthesize proteins. Ribosome profiling recently revealed that many short sequences previously thought to be noncoding are pervasively translated. To identify protein-coding genes in this noncanonical translatome, we combine an integrative framework for extremely sensitive ribosome profiling analysis, iRibo, with high-powered selection inferences tailored for short sequences. We construct a reference translatome for Saccharomyces cerevisiae comprising 5,400 canonical and almost 19,000 noncanonical translated elements. Only 14 noncanonical elements were evolving under detectable purifying selection. Surprisingly, a representative subset of translated elements lacking signatures of selection demonstrated involvement in processes including DNA repair, stress response and post-transcriptional regulation. Our results suggest that most translated elements are not conserved protein-coding genes and contribute to genotype-phenotype relationships through fast-evolving molecular mechanisms.
Competing Interest Statement
A.-R.C. is a member of the scientific advisory board for Flagship Labs 69, Inc.
Footnotes
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Many analyses have been updated and new experiments conducted and described.
