Characterization of a new cytotoxin that contributes to Staphylococcus aureus pathogenesis

DuMont, Ashley L.; Nygaard, Tyler K.; Watkins, Robert L.; Smith, Amanda; Kozhaya, Lina; Kreiswirth, Barry N.; Shopsin, Bo; Unutmaz, Derya; Voyich, Jovanka M.; Torres, Victor J.

doi:10.1111/j.1365-2958.2010.07490.x

Cited by 168 publications

(278 citation statements)

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“…SaeRS regulates transcription of multiple toxins, including γ-toxin (hlgA, hlgB, hlgC), LukSF-PVL, and LukAB/LukGH, which have been shown to contribute to PMN lysis (26)(27)(28)(29)(30)(31). Additionally, transcription of the saePQRS operon and SaeR target genes are activated in response to PMN phagocytosis and PMN components (32)(33)(34).…”

Section: Mutagenesis Of the Predicted Extracellular Loop Of Saes Idenmentioning

confidence: 99%

Differential regulation of staphylococcal virulence by the sensor kinase SaeS in response to neutrophil-derived stimuli

Flack

Zurek

Meishery

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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Two-component systems (TCSs) are highly conserved across bacteria and are used to rapidly sense and respond to changing environmental conditions. The human pathogen Staphylococcus aureus uses the S. aureus exoprotein expression (sae) TCS to sense host signals and activate transcription of virulence factors essential to pathogenesis. Despite its importance, the mechanism by which the histidine kinase SaeS recognizes specific host stimuli is unknown. After mutagenizing the predicted extracellular loop of SaeS, we discovered one methionine residue (M31) was essential for the ability of S. aureus to transcribe sae target genes, including hla, lukAB/lukGH, and hlgA. This single M31A mutation also significantly reduced cytotoxicity in human neutrophils to levels observed in cells following interaction with ΔsaeS. Another important discovery was that mutation of two aromatic anchor residues (W32A and F33A) disrupted the normal basal signaling of SaeS in the absence of inducing signals, yet both mutant kinases had appropriate activation of effector genes following exposure to neutrophils. Although the transcriptional profile of aromatic mutation W32A was consistent with that of WT in response to human α-defensin 1, mutant kinase F33A did not properly transcribe the γ-toxin genes in response to this stimulus. Taken together, our results provide molecular evidence for how SaeS recognizes host signals and triggers activation of select virulence factors to facilitate evasion of innate immunity. These findings have important implications for signal transduction in prokaryotes and eukaryotes due to conservation of aromatic anchor residues across both of these domains and the important role they play in sensor protein structure and function.host-pathogen interactions | membrane proteins

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Section: Mutagenesis Of the Predicted Extracellular Loop Of Saes Idenmentioning

confidence: 99%

Differential regulation of staphylococcal virulence by the sensor kinase SaeS in response to neutrophil-derived stimuli

Flack

Zurek

Meishery

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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“…A single S. aureus strain can produce up to five different leukotoxins including two versions of γ-hemolysin (HlgAB and HlgCB), leukocidin E/D (LukED), Panton-Valentine leukocidin (PVL), and leukocidin A/B (LukAB, also known as LukGH) (4)(5)(6). The sequence similarity among these leukocidins ranges from 60% to 80% with the exception of LukAB, which is only 30-40% similar to the others (9,10). LukAB is the most recently identified member of the bicomponent leukocidin family (9,10).…”

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confidence: 99%

“…The sequence similarity among these leukocidins ranges from 60% to 80% with the exception of LukAB, which is only 30-40% similar to the others (9,10). LukAB is the most recently identified member of the bicomponent leukocidin family (9,10). This toxin contributes to the cytotoxicity of clinical isolates toward innate immune cells and has been shown to play an important role in the success of S. aureus in both ex vivo and in vivo models of infection (9,11).…”

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confidence: 99%

“…LukAB is the most recently identified member of the bicomponent leukocidin family (9,10). This toxin contributes to the cytotoxicity of clinical isolates toward innate immune cells and has been shown to play an important role in the success of S. aureus in both ex vivo and in vivo models of infection (9,11). LukAB specifically targets phagocytes such as polymorphonuclear cells (PMNs or neutrophils) (9)(10)(11)(12), which are an integral part of the host innate immune response to S. aureus (13).…”

mentioning

confidence: 99%

“…This toxin contributes to the cytotoxicity of clinical isolates toward innate immune cells and has been shown to play an important role in the success of S. aureus in both ex vivo and in vivo models of infection (9,11). LukAB specifically targets phagocytes such as polymorphonuclear cells (PMNs or neutrophils) (9)(10)(11)(12), which are an integral part of the host innate immune response to S. aureus (13). The capacity to kill PMNs is conserved among all leukocidins (4,5), although the actions of LukED (14) and Hlg (15) are not limited to phagocytes (5).…”

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Staphylococcus aureusLukAB cytotoxin kills human neutrophils by targeting the CD11b subunit of the integrin Mac-1

DuMont

Yoong

Day

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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Staphylococcus aureus causes diseases ranging from superficial wound infections to more invasive manifestations like osteomyelitis and endocarditis. The evasion of host phagocytes recruited to the site of infection is essential to the success of S. aureus as a pathogen. A single S. aureus strain can produce up to five different bicomponent pore-forming leukotoxins that lyse immune cells by forming pores in the cellular plasma membrane. Although these leukotoxins have been considered redundant due to their cytotoxic activity toward human neutrophils, each toxin displays varied species and celltype specificities. This suggests that cellular factors may influence which cells each toxin targets. Here we describe the identification of CD11b, the α subunit of the αM/β2 integrin (CD11b/CD18), macrophage-1 antigen, or complement receptor 3, as a cellular receptor for leukocidin A/B (LukAB), an important toxin that contributes to S. aureus killing of human neutrophils. We demonstrate that CD11b renders human neutrophils susceptible to LukAB-mediated killing by purified LukAB as well as during S. aureus infection ex vivo. LukAB directly interacts with human CD11b by binding to the I domain, a property that determines the species specificity exhibited by this toxin. Identification of a LukAB cellular target has broad implications for the use of animal models to study the role of LukAB in S. aureus pathogenesis, explains the toxin's tropism toward human neutrophils and other phagocytes, and provides a cellular therapeutic target to block the effect of LukAB toward human neutrophils.toxin receptor | pore-forming cytotoxin

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Pathogenesis of Staphylococcus aureus in Humans

DeLeo

2015

Human Emerging and Re‐emerging Infections

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Characterization of a new cytotoxin that contributes to Staphylococcus aureus pathogenesis

Cited by 168 publications

References 43 publications

Differential regulation of staphylococcal virulence by the sensor kinase SaeS in response to neutrophil-derived stimuli

Differential regulation of staphylococcal virulence by the sensor kinase SaeS in response to neutrophil-derived stimuli

Staphylococcus aureusLukAB cytotoxin kills human neutrophils by targeting the CD11b subunit of the integrin Mac-1

Pathogenesis of Staphylococcus aureus in Humans

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