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The staphylococcal toxins γ-haemolysin AB and CB differentially target phagocytes by employing specific chemokine receptors

Author

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  • András N. Spaan

    (University Medical Center Utrecht
    CIRI, International Center for Infectiology Research, Université Lyon 1 and Ecole Normale Supérieure de Lyon
    Inserm, U1111)

  • Manouk Vrieling

    (University Medical Center Utrecht)

  • Pierre Wallet

    (CIRI, International Center for Infectiology Research, Université Lyon 1 and Ecole Normale Supérieure de Lyon
    Inserm, U1111
    CNRS, UMR5308)

  • Cédric Badiou

    (CIRI, International Center for Infectiology Research, Université Lyon 1 and Ecole Normale Supérieure de Lyon
    Inserm, U1111
    CNRS, UMR5308)

  • Tamara Reyes-Robles

    (New York University School of Medicine)

  • Elizabeth A. Ohneck

    (New York University School of Medicine)

  • Yvonne Benito

    (CIRI, International Center for Infectiology Research, Université Lyon 1 and Ecole Normale Supérieure de Lyon
    Inserm, U1111
    CNRS, UMR5308
    Centre National de Référence des Staphylocoques, Hospices Civils de Lyon)

  • Carla J. C. de Haas

    (University Medical Center Utrecht)

  • Christopher J. Day

    (Institute for Glycomics, Griffith University)

  • Michael P. Jennings

    (Institute for Glycomics, Griffith University)

  • Gérard Lina

    (CIRI, International Center for Infectiology Research, Université Lyon 1 and Ecole Normale Supérieure de Lyon
    Inserm, U1111
    CNRS, UMR5308
    Centre National de Référence des Staphylocoques, Hospices Civils de Lyon)

  • François Vandenesch

    (CIRI, International Center for Infectiology Research, Université Lyon 1 and Ecole Normale Supérieure de Lyon
    Inserm, U1111
    CNRS, UMR5308
    Centre National de Référence des Staphylocoques, Hospices Civils de Lyon)

  • Kok P. M. van Kessel

    (University Medical Center Utrecht)

  • Victor J. Torres

    (New York University School of Medicine)

  • Jos A. G. van Strijp

    (University Medical Center Utrecht)

  • Thomas Henry

    (CIRI, International Center for Infectiology Research, Université Lyon 1 and Ecole Normale Supérieure de Lyon
    Inserm, U1111)

Abstract

Evasion of the host phagocyte response by Staphylococcus aureus is crucial to successful infection with the pathogen. γ-haemolysin AB and CB (HlgAB, HlgCB) are bicomponent pore-forming toxins present in almost all human S. aureus isolates. Cellular tropism and contribution of the toxins to S. aureus pathophysiology are poorly understood. Here we identify the chemokine receptors CXCR1, CXCR2 and CCR2 as targets for HlgAB, and the complement receptors C5aR and C5L2 as targets for HlgCB. The receptor expression patterns allow the toxins to efficiently and differentially target phagocytic cells. Murine neutrophils are resistant to HlgAB and HlgCB. CCR2 is the sole murine receptor orthologue compatible with γ-haemolysin. In a murine peritonitis model, HlgAB contributes to S. aureus bacteremia in a CCR2-dependent manner. HlgAB-mediated targeting of CCR2+ cells highlights the involvement of inflammatory macrophages during S. aureus infection. Functional quantification identifies HlgAB and HlgCB as major secreted staphylococcal leukocidins.

Suggested Citation

  • András N. Spaan & Manouk Vrieling & Pierre Wallet & Cédric Badiou & Tamara Reyes-Robles & Elizabeth A. Ohneck & Yvonne Benito & Carla J. C. de Haas & Christopher J. Day & Michael P. Jennings & Gérard , 2014. "The staphylococcal toxins γ-haemolysin AB and CB differentially target phagocytes by employing specific chemokine receptors," Nature Communications, Nature, vol. 5(1), pages 1-11, December.
    • Handle: RePEc:nat:natcom:v:5:y:2014:i:1:d:10.1038_ncomms6438
    DOI: 10.1038/ncomms6438
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