regulation of the activity of the dual-function dnaa protein in caulobacter crescentus监管活动的双重职能dnaa蛋白质茎菌属crescentus.pdfVIP
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regulation of the activity of the dual-function dnaa protein in caulobacter crescentus监管活动的双重职能dnaa蛋白质茎菌属crescentus
Regulation of the Activity of the Dual-Function DnaA
Protein in Caulobacter crescentus
Carmen Fernandez-Fernandez, Diego Gonzalez, Justine Collier*
Department of Fundamental Microbiology, Faculty of Biology and Medicine, University of Lausanne, Lausanne, Switzerland
Abstract
DnaA is a conserved essential bacterial protein that acts as the initiator of chromosomal replication as well as a master
transcriptional regulator in Caulobacter crescentus. Thus, the intracellular levels of active DnaA need to be tightly regulated
during the cell cycle. Our previous work suggested that DnaA may be regulated at the level of its activity by the replisome-
associated protein HdaA. Here, we describe the construction of a mutant DnaA protein [DnaA(R357A)]. The R357 residue in
the AAA+ domain of the C. crescentus DnaA protein is equivalent to the R334 residue of the E. coli DnaA protein, which is
required for the Regulatory Inactivation of DnaA (RIDA). We found that the expression of the DnaA(R357A) mutant protein
in C. crescentus, but not the expression of the wild-type DnaA protein at similar levels, causes a severe phenotype of over-
initiation of chromosomal replication and that it blocks cell division. Thus, the mutant DnaA(R357A) protein is hyper-active
to promote the initiation of DNA replication, compared to the wild-type DnaA protein. DnaA(R357A) could not replace DnaA
in vivo, indicating that the switch in DnaA activity once chromosomal replication has started may be an essential process in
C. crescentus. We propose that the inactivation of DnaA is the main mechanism ensuring that chromosomal replication starts
only once per cell cycle. We further observed that the R357A substitution in DnaA does not promote the activity of DnaA as
a direct transcriptional activator of four important genes, encoding HdaA, the GcrA master cell cycle regulator, the FtsZ cell
division pr
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