Gene/Protein
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Gene/Protein
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Target Concepts:
Gene/Protein
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Enzyme
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Query: EC:2.7.13.3 (
histidine kinase
)
2,405
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Transmembrane receptors are integral components of sensory pathways in prokaryotes. These receptors share a common dimeric architecture, consisting in its basic form of an N-terminal extracellular sensor, transmembrane helices, and an intracellular effector. As an exception, we have identified an archaeal receptor family--exemplified by Af1503 from Archaeoglobus fulgidus--that is C-terminally shortened, lacking a recognizable effector module. Instead, a HAMP domain forms the sole extension for signal transduction in the cytosol. Here, we examine the gene environment of Af1503-like receptors and find a frequent association with transmembrane transport proteins. Furthermore, we identify and define a closely associated new protein domain family, which we characterize structurally using Af1502 from A. fulgidus. Members of this family are found both as stand-alone proteins and as domains within extant receptors. In general, the latter appear as connectors between the solute carrier 5 (SLC5)-like transmembrane domains and two-component signal transduction (TCST) domains. This is seen, for example, in the
histidine kinase
CbrA, which is a global regulator of metabolism, virulence, and antibiotic resistance in Pseudomonads. We propose that this newly identified domain family mediates signal transduction in systems regulating transport processes and name it
STAC
, for SLC and TCST-Associated Component.
...
PMID:STAC--A New Domain Associated with Transmembrane Solute Transport and Two-Component Signal Transduction Systems. 2632 Dec 52
Vibrio cholerae
controls the pathogenicity of interactions with arthropod hosts via the activity of the CrbS/R two-component system. This signaling pathway regulates the consumption of acetate, which in turn alters the relative virulence of interactions with arthropods, including
Drosophila melanogaster
CrbS is a
histidine kinase
that links a transporter-like domain to its signaling apparatus via putative
STAC
and PAS domains. CrbS and its cognate response regulator are required for the expression of acetyl coenzyme A (acetyl-CoA) synthetase (product of
acs
), which converts acetate to acetyl-CoA. We demonstrate that the
STAC
domain of CrbS is required for signaling in culture; without it,
acs
transcription is reduced in LB medium, and
V. cholerae
cannot grow on acetate minimal media. However, the strain remains virulent toward
Drosophila
and expresses
acs
similarly to the wild type during infection. This suggests that there is a unique signal or environmental variable that modulates CrbS in the gastrointestinal tract of
Drosophila
Second, we present evidence in support of CrbR, the response regulator that interacts with CrbS, binding directly to the
acs
promoter, and we identify a region of the promoter that CrbR may target. We further demonstrate that nutrient signals, together with the cAMP receptor protein (CRP)-cAMP system, control
acs
transcription, but regulation may occur indirectly, as CRP-cAMP activates the expression of the
crbS
and
crbR
genes. Finally, we define the role of the Pta-AckA system in
V. cholerae
and identify redundancy built into acetate excretion pathways in this pathogen.
IMPORTANCE
CrbS is a member of a unique family of sensor histidine kinases, as its structure suggests that it may link signaling to the transport of a molecule. However, mechanisms through which CrbS senses and communicates information about the outside world are unknown. In the
Vibrionaceae
, orthologs of CrbS regulate acetate metabolism, which can, in turn, affect interactions with host organisms. Here, we situate CrbS within a larger regulatory framework, demonstrating that
crbS
is regulated by nutrient-sensing systems. Furthermore, CrbS domains may play various roles in signaling during infection and growth in culture, suggesting a unique mechanism of host recognition. Finally, we define the roles of additional pathways in acetate flux, as a foundation for further studies of this metabolic nexus point.
...
PMID:Modulation of CrbS-Dependent Activation of the Acetate Switch in Vibrio cholerae. 3022 39
