Affiliation:
1. Laboratory of Bacterial Toxins, Division of Bacterial Products, Center for Biologics Evaluation and Research, Food and Drug Administration, Bethesda, Maryland 20892
Abstract
ABSTRACT
Corynebacterium diphtheriae
, the causative agent of diphtheria, utilizes various host compounds to acquire iron. The
C. diphtheriae hmuO
gene encodes a heme oxygenase that is involved in the utilization of heme and hemoglobin as iron sources. Transcription of the
hmuO
gene in
C. diphtheriae
is controlled under a dual regulatory mechanism in which the diphtheria toxin repressor protein (DtxR) and iron repress expression while either heme or hemoglobin is needed to activate transcription. In this study, two clones isolated from a
C. diphtheriae
chromosomal library were shown to activate transcription from the
hmuO
promoter in
Escherichia coli
. Sequence analysis revealed that these activator clones each carried distinct genes whose products had significant homology to response regulators of two-component signal transduction systems. Located upstream from each of these response regulator homologs are partial open reading frames that are predicted to encode the C-terminal portions of sensor kinases. The full-length sensor kinase gene for each of these systems was cloned from the
C. diphtheriae
chromosome, and constructs each carrying one complete sensor kinase gene and its cognate response regulator were constructed. One of these constructs, pTSB20, which carried the response regulator (
chrA
) and its cognate sensor kinase (
chrS
), was shown to strongly activate transcription from the
hmuO
promoter in a heme-dependent manner in
E. coli
. A mutation in
chrA
(
chrAD50N
), which changed a conserved aspartic acid residue at position 50, the presumed site of phosphorylation by ChrS, to an asparagine, abolished heme-dependent activation. These findings suggest that the sensor kinase ChrS is involved in the detection of heme and the transduction of this signal, via a phosphotransfer mechanism, to the response regulator ChrA, which then activates transcription of the
hmuO
promoter. This is the first report of a bacterial two-component signal transduction system that controls gene expression through a heme-responsive mechanism.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
Cited by
61 articles.
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