Two Unique Phosphorylation-Driven Signaling Pathways Crosstalk in <i>Staphylococcus aureus</i> to Modulate the Cell-Wall Charge: Stk1/Stp1 Meets GraSR

Fridman, Michael D.; Williams, Gwillym Declan; Muzamal, Uzma; Hunter, Howard N.; Siu, Kin Wai Michael; Golemi-Kotra, Dasantila

doi:10.1021/bi401177n

Cited by 65 publications

(75 citation statements)

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“…Cross-talk between Stk1/Stp1 and GraS/GraR signalling pathways was shown in S. aureus (Fridman et al, 2013). Stk1/Stp1 is a Hanks-type STK/phosphatase pair and GraS/GraR is a TCS which controls the resistance to cationic antimicrobial peptides.…”

Section: A Kalantari and Othersmentioning

confidence: 99%

Serine/threonine/tyrosine phosphorylation regulates DNA binding of bacterial transcriptional regulators

et al. 2015

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Reversible phosphorylation of bacterial transcriptional regulators (TRs) belonging to the family of two-component systems (TCSs) is a well-established mechanism for regulating gene expression. Recent evidence points to the fact that reversible phosphorylation of bacterial TRs on other types of residue, i.e. serine, threonine, tyrosine and cysteine, is also quite common. The phosphorylation of the ester type (phospho-serine/threonine/tyrosine) is more stable than the aspartate phosphorylation of TCSs. The kinases which catalyse these phosphorylation events (Hanks-type serine/threonine protein kinases and bacterial protein tyrosine kinases) are also much more promiscuous than the TCS kinases, i.e. each of them can phosphorylate several substrate proteins. As a consequence, the dynamics and topology of the signal transduction networks depending on these kinases differ significantly from the TCSs. Here, we present an overview of different classes of bacterial TR phosphorylated and regulated by serine/threonine and tyrosine kinases. Particular attention is given to examples when serine/threonine and tyrosine kinases interact with TCSs, phosphorylating either the histidine kinases or the response regulators. We argue that these promiscuous kinases connect several signal transduction pathways and serve the role of signal integration. Bacterial two-component systems (TCSs)TCSs are signal transduction devices that were initially discovered in bacteria (Ninfa & Magasani, 1986;Nixon et al., 1986). They play an important role in signal sensing and response to various stimuli, enabling the organisms to adapt to environmental changes. A typical TCS consists of a histidine kinase (HK) and a corresponding response regulator (RR) (Stock et al., 2000;Gao & Stock, 2009). HK usually possesses a highly variable sensor domain and a conserved kinase core. Following environmental stimulus, a signal ligand binds to the sensor domain and results in the autophosphorylation of the kinase core at a conserved histidine residue, at the expense of ATP. Next, the phosphoryl group is transferred from HK to a conserved aspartate in the regulatory domain of the RR. RRs usually contain two domains: a regulatory domain with the conserved phosphorylatable aspartate and a variable effector domain. Phosphorylation activates the effector domain of RRs, triggering the physiological response. As phosphohistidine has a very short half-life in aqueous solutions at neutral pH, in the absence of the environmental signal the system switches itself off very rapidly.Many effector domains of bacterial RRs have DNA-binding capacity. This allows RRs to function as transcriptional regulators (TRs) and consequently change gene transcription when they become phosphorylated. In Escherichia coli, osmoregulation of porin proteins OmpF and OmpC is under transcriptional control of the TCS EnvZ/OmpR. The phosphorylation of OmpR by EnvZ changes its affinity for the promoter region of ompF and ompC, resulting in different transcriptional levels of these genes (Forst et al., 1...

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Section: A Kalantari and Othersmentioning

confidence: 99%

Serine/threonine/tyrosine phosphorylation regulates DNA binding of bacterial transcriptional regulators

et al. 2015

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“…101 What is known is that GraR is another substrate of the S. aureus PASTA-containing eSTK Stk1. 102 By employing in vitro kinase reactions combined with tandem mass spectrometry analyses, Fridman et al show that GraR phosphorylation by Stk1 occurs on 3 threonine residues, namely Thr128, Thr130 and Thr149 102 (Fig. 5).…”

Section: Staphylococcus Aureusmentioning

confidence: 99%

“…Importantly, experiments reveal that these residues are required for efficient incorporation of D-ala into the bacterial cell wall, which could directly affect the efficiency of vancomycin binding and explain the GraR connection with vancomycin resistance. Additionally, the phosphorylation of these residues enhances the binding of GraR to the vraFG CAMP ABC transporter promoter to control its synthesis 102 (Fig. 4).…”

Section: Staphylococcus Aureusmentioning

confidence: 99%

“…Consistent with the interspecies kinase assays described for eSTK phosphorylation of CcpA (above), despite the similarity of these regulators and the conservation of serine-threonine residues at the same positions found in BceR, both were unable to accept a phosphate from the S. aureus eSTK in vitro. 102 Thus identification of conserved binding sites only indicates a potential for eSTK regulation, and therefore must be treated with caution. Future directions might include BceR and/or VraR variants from different strains to be tested, as sequences between clinical isolates can vary considerably and could therefore 'unmask' substrate specificity though subtle changes in amino acid composition.…”

Section: Staphylococcus Aureusmentioning

confidence: 99%

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Regulation of transcription by eukaryotic-like serine-threonine kinases and phosphatases in Gram-positive bacterial pathogens

Wright

Ulijasz

2014

Virulence

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“…Other studies have suggested that GraX as well as distinct two-component regulatory systems, such as VraSR and NsaSR, are also involved in S. aureus responses to antibiotics (21,22). Likewise, Stk1/Stp1 signaling appears to cross talk with GraSR in modulating S. aureus cell wall charge (23). GraSR may have special relevance to sensing peptide-based agents, including vancomycin (glycopeptide), daptomycin (lipopeptide), and structurally or functionally similar host defense peptides.…”

Section: Fig 3 Quantitative Mechanisms Of Hdps Againstmentioning

confidence: 99%

The GraS Sensor in Staphylococcus aureus Mediates Resistance to Host Defense Peptides Differing in Mechanisms of Action

et al. 2016

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f Staphylococcus aureus uses the two-component regulatory system GraRS to sense and respond to host defense peptides (HDPs). However, the mechanistic impact of GraS or its extracellular sensing loop (EL) on HDP resistance is essentially unexplored. Strains with null mutations in the GraS holoprotein (⌬graS) or its EL (⌬EL) were compared for mechanisms of resistance to HDPs of relevant immune sources: neutrophil ␣-defensin (human neutrophil peptide 1 [hNP-1]), cutaneous ␤-defensin (human ␤-defensin 2 [hBD-2]), or the platelet kinocidin congener RP-1. Actions studied by flow cytometry included energetics (ENR); membrane permeabilization (PRM); annexin V binding (ANX), and cell death protease activation (CDP). Assay conditions simulated bloodstream (pH 7.5) or phagolysosomal (pH 5.5) pH contexts. S. aureus strains were more susceptible to HDPs at pH 7.5 than at pH 5.5, and each HDP exerted a distinct effect signature. The impacts of ⌬graS and ⌬⌭L on HDP resistance were peptide and pH dependent. Both mutants exhibited defects in ANX response to hNP-1 or hBD-2 at pH 7.5, but only hNP-1 did so at pH 5.5. Both mutants exhibited hyper-PRM, -ANX, and -CDP responses to RP-1 at both pHs and hypo-ENR at pH 5.5. The actions correlated with ⌬graS or ⌬⌭L hypersusceptibility to hNP-1 or RP-1 (but not hBD-2) at pH 7.5 and to all study HDPs at pH 5.5. An exogenous EL mimic protected mutant strains from hNP-1 and hBD-2 but not RP-1, indicating that GraS and its EL play nonredundant roles in S. aureus survival responses to specific HDPs. These findings suggest that GraS mediates specific resistance countermeasures to HDPs in immune contexts that are highly relevant to S. aureus pathogenesis in humans.

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Two Unique Phosphorylation-Driven Signaling Pathways Crosstalk in Staphylococcus aureus to Modulate the Cell-Wall Charge: Stk1/Stp1 Meets GraSR

Cited by 65 publications

References 63 publications

Serine/threonine/tyrosine phosphorylation regulates DNA binding of bacterial transcriptional regulators

Serine/threonine/tyrosine phosphorylation regulates DNA binding of bacterial transcriptional regulators

Regulation of transcription by eukaryotic-like serine-threonine kinases and phosphatases in Gram-positive bacterial pathogens

The GraS Sensor in Staphylococcus aureus Mediates Resistance to Host Defense Peptides Differing in Mechanisms of Action

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