Strong Asymmetric Mutation Bias in Endosymbiont Genomes Coincide with Loss of Genes for Replication Restart Pathways

doi:10.1093/molbev/msj107

MBE Advance Access originally published online on February 13, 2006
Molecular Biology and Evolution 2006 23(5):1031-1039; doi:10.1093/molbev/msj107

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© The Author 2006. Published by Oxford University Press on behalf of the Society for Molecular Biology and Evolution. All rights reserved. For permissions, please e-mail: journals.permissions@oxfordjournals.org

Research Article

Strong Asymmetric Mutation Bias in Endosymbiont Genomes Coincide with Loss of Genes for Replication Restart Pathways

Lisa Klasson and Siv G. E. Andersson

Department of Molecular Evolution, Evolutionary Biology Center, Uppsala University, Uppsala, Sweden

E-mail: siv.andersson{at}ebc.uu.se.

A large majority of bacterial genomes show strand asymmetry,such that G and T preferentially accumulate on the leading strand.The mechanisms are unknown, but cytosine deaminations are thoughtto play an important role. Here, we have examined DNA strandasymmetry in three strains of the aphid endosymbiont Buchneraaphidicola. These are phylogenetically related, have similargenomic GC contents, and conserved gene order structures, yetB. aphidicola (Bp) shows a fourfold higher replication-inducedstrand bias than B. aphidicola (Sg) and (Ap). We rule out anincrease in the overall substitution frequency as the majorcause of the stronger strand bias in B. aphidicola (Bp). Instead,the results suggest that the higher GC skew in this speciesis caused by a different spectrum of mutations, including arelatively higher frequency of C to T mutations on the leadingstrand and/or of G to A mutations on the lagging strand. A comparativeanalysis of 20 ${gamma}$ -proteobacterial genomes revealed that endosymbiontgenomes lacking recA and other genes involved in replicationrestart processes, such as priA, which codes for primosomalhelicase PriA, displayed the strongest strand bias. We hypothesizethat cytosine deaminations accumulate during single-strand exposureat arrested replication forks and that inefficient restart mechanismsmay lead to high DNA strand asymmetry in bacterial genomes.

Key Words: Buchnera • molecular evolution • nucleotide composition • strand asymmetry

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