Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
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Drug
Enzyme
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Query: EC:3.4.24.11 (
CD10
)
9,792
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Streptococcus mutans
, a cariogenic species, is often associated with cardiovascular infections. Systemic virulence of specific
S. mutans
serotypes has been associated with the expression of the collagen- and laminin-binding protein Cnm, which is transcriptionally regulated by VicRK and CovR. In this study, we characterized a VicRK- and CovR-regulated gene,
pepO
, coding for a conserved
endopeptidase
. Transcriptional and protein analyses revealed that
pepO
is highly expressed in
S. mutans
strains resistant to complement immunity (blood isolates) compared to oral isolates. Gel mobility assay, transcriptional, and Western blot analyses revealed that
pepO
is repressed by VicR and induced by CovR. Deletion of
pepO
in the Cnm
+
strain OMZ175 (OMZpepO) or in the Cnm
-
UA159 (UApepO) led to an increased susceptibility to C3b deposition, and to low binding to complement proteins C1q and C4BP. Additionally,
pepO
mutants showed diminished
ex vivo
survival in human blood and impaired capacity to kill
G. mellonella
larvae. Inactivation of
cnm
in OMZ175 (OMZcnm) resulted in increased resistance to C3b deposition and unaltered blood survival, although both
pepO
and
cnm
mutants displayed attenuated virulence in
G. mellonella
. Unlike OMZcnm, OMZpepO could invade HCAEC endothelial cells. Supporting these phenotypes, recombinant proteins rPepO and rCnmA showed specific profiles of binding to C1q, C4BP, and to other plasma (plasminogen,
fibronectin
) and extracellular matrix proteins (type I collagen, laminin). Therefore this study identifies a novel VicRK/CovR-target required for immune evasion and host persistence,
pepO
, expanding the roles of VicRK and CovR in regulating
S. mutans
virulence.
...
PMID:
PepO
is a target of the two-component systems VicRK and CovR required for systemic virulence of
Streptococcus mutans
. 3242 40
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