Abstract

Choice of synonymous codons depends on nucleotide/dinucleotide composition of the genome (termed mutational pressure) and relative abundance of tRNAs in a cell (translational pressure). Mutational pressure is commonly simplified to genomic GC content; however mononucleotide and dinucleotide frequencies in different genomes or mRNAs may vary significantly, especially in RNA viruses. A series of in silico shuffling algorithms were developed to account for these features and analyze the relative impact of mutational pressure components on codon usage bias in RNA viruses. Total GC content was a poor descriptor of viral genome composition and causes of codon usage bias. Genomic nucleotide content was the single most important factor of synonymous codon usage. Moreover, the choice between compatible amino acids (e.g., leucine and isoleucine) was strongly affected by genomic nucleotide composition. Dinucleotide composition at codon positions 2-3 had additional effect on codon usage. Together with mononucleotide composition bias, it could explain almost the entire codon usage bias in RNA viruses. On the other hand, strong dinucleotide content bias at codon position 3-1 found in some viruses had very little effect on codon usage. A hypothetical innate immunity sensor for CpG in RNA could partially explain the codon usage bias, but due to dependence of virus translation upon biased host translation machinery, experimental studies are required to further explore the source of dinucleotide bias in RNA viruses.

Highlights

  • Amino acid sequence of proteins is encoded by nucleotide triplets

  • A well-known feature of genomes in general, and RNA viruses in particular, is dinucleotide bias [36], which complements to codon usage bias (CUB) [34]

  • Dinucleotide content varies between codon positions 2-3 and 3-1

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Summary

Introduction

Amino acid sequence of proteins is encoded by nucleotide triplets. The majority of organisms use the standard genetic code, with 61 sense codons translated into 20 amino acids. Most amino acids are encoded by several synonymous codons, which are not used evenly. This codon usage bias (CUB) can have distinct causes and consequences in different organisms. While the implications of translational pressure are ubiquitous (reviewed in [10,11]), a growing body of evidence suggests that it is not the main driver of synonymous codon preference

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