Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:2.7.13.3 (
histidine kinase
)
2,405
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Enteroaggregative
Escherichia coli
(EAEC) from the O104:H4 specific serotype caused a large outbreak of bloody diarrhea with some complicated cases of hemolytic-uremic syndrome (HUS) in Europe in 2011. The outbreak strain consisted in an EAEC capable to produce the Shiga toxin (Stx) subtype 2a, a characteristic from enterohemorrhagic
E. coli
QseBC two-component system detects AI-3/Epi/NE and mediates the chemical signaling between pathogen and mammalian host. This system coordinates a cascade of virulence genes expression in important human enteropathogens. The blocking of QseC of EAEC C227-11 (Stx
+
) strain by
N
-phenyl-4-{[(phenylamino) thioxomethyl]amino}-benzenesulfonamide (also known as LED209)
in vivo
demonstrated a lower efficiency of colonization. The periplasmic protein VisP, which is related to survival mechanisms in a
colitis
model of infection, bacterial membrane maintenance, and stress resistance, here presented high levels of expression during the initial infection within the host. Under acid stress conditions,
visP
expression levels were differentiated in an Stx-dependent way. Together, these results emphasize the important role of VisP and the
histidine kinase
sensor QseC in the C227-11 (Stx
+
) outbreak strain for the establishment of the infectious niche process in the C57BL/6 mouse model and of LED209 as a promising antivirulence drug strategy against these enteric pathogens.
IMPORTANCE
EAEC is a remarkable etiologic agent of acute and persistent diarrhea worldwide. The isolates harbor specific subsets of virulence genes and their pathogenesis needs to be better understood. Chemical signaling via
histidine kinase
sensor QseC has been shown as a potential target to elucidate the orchestration of the regulatory cascade of virulence factors.
...
PMID:QseC Signaling in the Outbreak O104:H4
Escherichia coli
Strain Combines Multiple Factors during Infection. 3123 11
The
Salmonella enterica
PhoP/PhoQ two-component signaling system coordinates the spatiotemporal expression of key virulence factors that confer pathogenic traits. Through biochemical and structural analyses, we found that the sensor
histidine kinase
PhoQ acted as a receptor for long-chain unsaturated fatty acids (LCUFAs), which induced a conformational change in the periplasmic domain of the PhoQ protein. This resulted in the repression of PhoQ autokinase activity, leading to inhibition of the expression of PhoP/PhoQ-dependent genes. Recognition of the LCUFA linoleic acid (LA) by PhoQ was not stereospecific because positional and geometrical isomers of LA equally inhibited PhoQ autophosphorylation, which was conserved in multiple
S. enterica
serovars. Because orally acquired
Salmonella
encounters conjugated LA (CLA), a product of the metabolic conversion of LA by microbiota, in the human intestine, we tested how short-term oral administration of CLA affected gut colonization and systemic dissemination in a mouse model of
Salmonella
-induced
colitis
. Compared to untreated mice, CLA-treated mice showed increased gut colonization by wild-type
Salmonella
, as well as increased dissemination to the spleen. In contrast, the inability of the
phoP
strain to disseminate systemically remained unchanged by CLA treatment. Together, our results reveal that, by inhibiting PhoQ, environmental LCUFAs fine-tune the fate of
Salmonella
during infection. These findings may aid in the design of new anti-
Salmonella
therapies.
...
PMID:PhoQ is an unsaturated fatty acid receptor that fine-tunes
Salmonella
pathogenic traits. 3231 68
