Affiliation:
1. Laboratoire de Microbiologie et Génétique Moléculaire, Centre National de Recherche Scientifique, 118 route de Narbonne, 31062 Toulouse, France
Abstract
ABSTRACT
Most bacterial chromosomes carry an analogue of the
parABS
systems that govern plasmid partition, but their role in chromosome partition is ambiguous.
parABS
systems might be particularly important for orderly segregation of multipartite genomes, where their role may thus be easier to evaluate. We have characterized
parABS
systems in
Burkholderia cenocepacia
, whose genome comprises three chromosomes and one low-copy-number plasmid. A single
parAB
locus and a set of ParB-binding (
parS
) centromere sites are located near the origin of each replicon. ParA and ParB of the longest chromosome are phylogenetically similar to analogues in other multichromosome and monochromosome bacteria but are distinct from those of smaller chromosomes. The latter form subgroups that correspond to the taxa of their hosts, indicating evolution from plasmids. The
parS
sites on the smaller chromosomes and the plasmid are similar to the “universal”
parS
of the main chromosome but with a sequence specific to their replicon. In an
Escherichia coli
plasmid stabilization test, each
parAB
exhibits partition activity only with the
parS
of its own replicon. Hence,
parABS
function is based on the independent partition of individual chromosomes rather than on a single communal system or network of interacting systems. Stabilization by the smaller chromosome and plasmid systems was enhanced by mutation of
parS
sites and a promoter internal to their
parAB
operons, suggesting autoregulatory mechanisms. The small chromosome ParBs were found to silence transcription, a property relevant to autoregulation.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
Cited by
88 articles.
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