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Amino Acid Usage Is Asymmetrically Biased in AT- and GC-Rich Microbial Genomes

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  • Jon Bohlin
  • Ola Brynildsrud
  • Tammi Vesth
  • Eystein Skjerve
  • David W Ussery

Abstract

Introduction: Genomic base composition ranges from less than 25% AT to more than 85% AT in prokaryotes. Since only a small fraction of prokaryotic genomes is not protein coding even a minor change in genomic base composition will induce profound protein changes. We examined how amino acid and codon frequencies were distributed in over 2000 microbial genomes and how these distributions were affected by base compositional changes. In addition, we wanted to know how genome-wide amino acid usage was biased in the different genomes and how changes to base composition and mutations affected this bias. To carry this out, we used a Generalized Additive Mixed-effects Model (GAMM) to explore non-linear associations and strong data dependences in closely related microbes; principal component analysis (PCA) was used to examine genomic amino acid- and codon frequencies, while the concept of relative entropy was used to analyze genomic mutation rates. Results: We found that genomic amino acid frequencies carried a stronger phylogenetic signal than codon frequencies, but that this signal was weak compared to that of genomic %AT. Further, in contrast to codon usage bias (CUB), amino acid usage bias (AAUB) was differently distributed in AT- and GC-rich genomes in the sense that AT-rich genomes did not prefer specific amino acids over others to the same extent as GC-rich genomes. AAUB was also associated with relative entropy; genomes with low AAUB contained more random mutations as a consequence of relaxed purifying selection than genomes with higher AAUB. Conclusion: Genomic base composition has a substantial effect on both amino acid- and codon frequencies in bacterial genomes. While phylogeny influenced amino acid usage more in GC-rich genomes, AT-content was driving amino acid usage in AT-rich genomes. We found the GAMM model to be an excellent tool to analyze the genomic data used in this study.

Suggested Citation

  • Jon Bohlin & Ola Brynildsrud & Tammi Vesth & Eystein Skjerve & David W Ussery, 2013. "Amino Acid Usage Is Asymmetrically Biased in AT- and GC-Rich Microbial Genomes," PLOS ONE, Public Library of Science, vol. 8(7), pages 1-10, July.
  • Handle: RePEc:plo:pone00:0069878
    DOI: 10.1371/journal.pone.0069878
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    References listed on IDEAS

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    1. Jon Bohlin & Eystein Skjerve, 2009. "Examination of Genome Homogeneity in Prokaryotes Using Genomic Signatures," PLOS ONE, Public Library of Science, vol. 4(12), pages 1-12, December.
    2. Jon Bohlin & Eystein Skjerve & David W Ussery, 2008. "Investigations of Oligonucleotide Usage Variance Within and Between Prokaryotes," PLOS Computational Biology, Public Library of Science, vol. 4(4), pages 1-9, April.
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    Cited by:

    1. Sophia S Liu & Adam J Hockenberry & Andrea Lancichinetti & Michael C Jewett & Luís A N Amaral, 2016. "NullSeq: A Tool for Generating Random Coding Sequences with Desired Amino Acid and GC Contents," PLOS Computational Biology, Public Library of Science, vol. 12(11), pages 1-12, November.

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