Profiling of terminating ribosomes reveals translational control at stop codons

Accurate termination of protein synthesis is paramount for the integrity of cellular proteome. Here we establish profiling of terminating ribosomes in mammalian cells and report a wide range of ribosome pausing at individual stop codons. We identify a sequence motif upstream of stop codons that contributes to termination pausing, which was confirmed by massively paralleled reporter assays. Lack of termination pausing increases the chance of stop codon slippage, generating proteins with mixed C-terminal extensions. We demonstrate that the sequence- dependent termination pausing is a result of post-decoding mRNA scanning by the 3' end of 18S rRNA. We further uncover tissue-specific termination pausing that correlates with the stoichiometry of Rps26, which constrains mRNA:rRNA interaction. Termination pausing represents a translational signature associated with translational control at stop codons. Overall design: Ribo-seq under 18S rRNA mutation, RPS26 knockdown, and RPS26 overexpression; Ribo-seq from mouse liver, testis, kidney, brain, and heart.