4.3 Article

Characterization of Synonymous Codon Usage Bias in the Duck Plague Virus UL35 Gene

INTERVIROLOGY (2009)

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Journal

INTERVIROLOGY
Volume 52, Issue 5, Pages 266-278

Publisher

KARGER
DOI: 10.1159/000231992

Keywords

Duck plague virus; UL35 gene; Codon usage bias

Categories

Virology

Funding

  1. National Natural Science Foundation of China [30771598]
  2. Changjiang Scholars and Innovative Research Team in University [PCSIRT0848]
  3. Modern Agro-Industry Technology Research System
  4. New Century Excellent Talents Program in University [NCET-06-0818]
  5. Scientific and Technological Innovation Major Project Funds in University [706050]
  6. Cultivation Fund of the Key Scientific and Technical Innovation Project
  7. Department of Education of Sichuan Province [07ZZ028]
  8. Sichuan Province Basic Research Program [07JY029-016/17]

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Objective: The aim was to identify the codon usage bias between the newly identified duck plague virus (DPV) UL35 gene (GenBank accession No. EF643558) and the UL35-like genes of 27 other reference herpesviruses. Methods: A comparative analysis of the codon usage bias of the 28 herpesviruses was performed by using the CodonW 1.4 program and CUSP (create a codon usage table) program of EMBOSS (The European Molecular Biology Open Software Suite). Results: The results showed obvious differences of the synonymous codon usage bias in the 28 herpesviruses indicated by the Codon Adaptation Index, effective number of codons (ENc), and the value of G + C content at the 3rd codon position. The codon usage pattern of the DPV UL35 gene was phylogenetically conserved and similar to that of the UL35-like genes of the avian alpha-herpesvirus, with a strong bias towards the codons with A and T at the 3rd codon position. A cluster analysis of codon usage pattern of the DPV UL35 gene with other reference herpesviruses demonstrated that the codon usage bias of the UL35 genes of the 28 herpesviruses had a very close relation with their gene function. The ENc-plot revealed that the genetic heterogeneity in the DPV UL35 gene and the 27 reference herpesviruses were constrained by G + C content, while gene length exerted relatively weaker influences. In addition, comparisons of the codon preferences in the UL35 gene of DPV with those of Escherichia coli, yeast and humans revealed that there were 33 codons showing distinct usage differences between the DPV and yeast, and 38 between the DPV and humans, but only 31 between the DPV and E. coli. Therefore, the E. coli system may be more suitable for the expression of the DPV UL35 gene. Conclusion: Together, these results may improve our understanding of the evolution, pathogenesis and functional studies of DPV, as well as contribute significantly to the area of herpesvirus research and possibly studies with other viruses. Copyright (C) 2009 S. Karger AG, Basel

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