Staphylococcal Panton-Valentine Leukocidin Induces Pro-Inflammatory Cytokine Production and Nuclear Factor-Kappa B Activation in Neutrophils

A Zivkovic; AL Genestier; B Barr; B Konig; B Löffler; B Wu; BA Diep; BA Diep; C Liu; C Lopez-Aguilar; CP Montgomery; Cuiping Zhang; CW Tseng; D Boehning; D Boehning; EL Brown; Fangyou Yu; FD Lowy; G Miles; K Purcell; L Jayasinghe; LB Ware; M Gilbert; M Labandeira-Rey; M Otto; P Dubrous; R Wang; RB Goodman; S Boyle-Vavra; SK Fridkin; Stefan Bereswill; SV Kazakova; Wenjiao Chang; Xiaoling Ma; Xin Zhou; Y Gillet

Staphylococcal Panton-Valentine Leukocidin Induces Pro-Inflammatory Cytokine Production and Nuclear Factor-Kappa B Activation in Neutrophils

Authors: A Zivkovic
AL Genestier
B Barr
B Konig
B Löffler
B Wu
BA Diep
BA Diep
C Liu
C Lopez-Aguilar
CP Montgomery
Cuiping Zhang
CW Tseng
D Boehning
D Boehning
EL Brown
Fangyou Yu
FD Lowy
G Miles
K Purcell
L Jayasinghe
LB Ware
M Gilbert
M Labandeira-Rey
M Otto
P Dubrous
R Wang
RB Goodman
S Boyle-Vavra
SK Fridkin
Stefan Bereswill
SV Kazakova
Wenjiao Chang
Xiaoling Ma
Xin Zhou
Y Gillet
Publication date: 18 April 2012
Publisher: Public Library of Science
Doi

Abstract

Panton-Valentine leukocidin (PVL) is a cytotoxin secreted by Staphylococcus aureus and associated with severe necrotizing infections. PVL targets polymorphonuclear leukocytes, especially neutrophils, which are the first line of defense against infections. Although PVL can induce neutrophil death by necrosis or apoptosis, the specific inflammatory responses of neutrophils to this toxin are unclear. In this study, both in vivo and in vitro studies demonstrated that recombinant PVL has an important cytotoxic role in human neutrophils, leading to apoptosis at low concentrations and necrosis at high concentrations. Recombinant PVL also increased the levels of pro-inflammatory cytokine secretion from neutrophils. The up-regulation of pro-inflammatory cytokines was due to nuclear factor-kappa B (NF-κB) activation induced by PVL. Moreover, blocking NF-κB inhibited the production of inflammatory cytokines. To test the role of neutrophil immune responses during the pathogenesis of PVL-induced acute lung injury, we used immunocompetent or neutropenic rabbits to develop a model of necrotizing pneumonia. Immunocompetent rabbits challenged with PVL demonstrated increased inflammation containing neutrophilic infiltrates. In addition, there were elevated levels of inflammatory cytokines (IL-6, IL-8, TNF-α and IL-10) and NF-κB in the lung homogenate. In contrast, the lung tissues from neutropenic rabbits contained mild or moderate inflammation, and the levels of inflammatory cytokines and NF-κB increased only slightly. Data from the current study support growing evidence that neutrophils play an important role in the pathogenesis of PVL-induced tissue injury and inflammation. PVL can stimulate neutrophils to release pro-inflammatory mediators, thereby causing an acute inflammatory response. The ability of PVL to induce inflammatory cytokine release may be associated with the activation of NF-κB or its pore-forming properties