validation of bacterial replication termination models using simulation of genomic mutations验证细菌复制终止使用模拟模型的基因突变.pdfVIP
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validation of bacterial replication termination models using simulation of genomic mutations验证细菌复制终止使用模拟模型的基因突变
Validation of Bacterial Replication Termination Models
Using Simulation of Genomic Mutations
Nobuaki Kono, Kazuharu Arakawa*, Masaru Tomita
Institute for Advanced Biosciences, Keio University, Fujisawa, Kanagawa, Japan
Abstract
In bacterial circular chromosomes and most plasmids, the replication is known to be terminated when either of the
following occurs: the forks progressing in opposite directions meet at the distal end of the chromosome or the replication
forks become trapped by Tus proteins bound to Ter sites. Most bacterial genomes have various polarities in their genomic
structures. The most notable feature is polar genomic compositional asymmetry of the bases G and C in the leading and
lagging strands, called GC skew. This asymmetry is caused by replication-associated mutation bias, and this ‘‘footprint’’ of
the replication machinery suggests that, in contrast to the two known mechanisms, replication termination occurs near the
chromosome dimer resolution site dif. To understand this difference between the known replication machinery and
genomic compositional bias, we undertook a simulation study of genomic mutations, and we report here how different
replication termination models contribute to the generation of replication-related genomic compositional asymmetry.
Contrary to naive expectations, our results show that a single finite termination site at dif or at the GC skew shift point is not
sufficient to reconstruct the genomic compositional bias as observed in published sequences. The results also show that the
known replication mechanisms are sufficient to explain the position of the GC skew shift point.
Citation: Kono N, Arakawa K, Tomita M (2012) Validation of Bacterial Replication Termination Models Using Simulation of Genomic Mutations. PLoS ONE 7(4):
e34526. doi:10.1371/journal.pone.0034526
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