Abstract:Errors in protein synthesis can lead to non-genetic phenotypic mutations, which contribute to generating a wide range of protein diversity. There are currently no methods to measure proteome-wide amino acid misincorporations in a high-throughput fashion, limiting their detection to specific sites and few codon-anticodon pairs. Therefore, it has been technically challenging to estimate the evolutionary impact of translation errors. Here, we developed a computational pipeline, integrated with a novel mechanistic… Show more
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