BMC Immunology (Jul 2012)

Role of gamma-delta T cells in host response against <it>Staphylococcus aureus</it>-induced pneumonia

  • Cheng Ping,
  • Liu Tao,
  • Zhou Wei-Ying,
  • Zhuang Yuan,
  • Peng Liu-sheng,
  • Zhang Jin-yu,
  • Yin Zhi-Nan,
  • Mao Xu-hu,
  • Guo Gang,
  • Shi Yun,
  • Zou Quan-ming

DOI
https://doi.org/10.1186/1471-2172-13-38
Journal volume & issue
Vol. 13, no. 1
p. 38

Abstract

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Abstract Background Staphylococcus aureus is the major cause of hospital-acquired and community-acquired pneumonia. Host defense to S.aureus infection is largely mediated by the innate immune system. γδ T cells play an important role in innate immunity to many infectious diseases. However, less is known about the role of these cells during S.aureus-induced pneumonia. In this study, we examined the response and the role of γδ T cells to pulmonary S.aureus infection. Results Mice infected with S. aureus intranasally showed rapid γδ T cells accumulation in the lung. Deficiency of γδ T cells led to attenuated bacterial clearance and less tissue damage in lung compared with WT mice. Moreover, TCR-δ−/− mice exhibited impaired neutrophil recruitment and reduced cytokine production at the site of infection. The γδ T cells in response to pulmonary S. aureus infection mainly secreted IL-17 and γδ T cells deficiency reduced IL-17 production, which might regulate the production of neutrophil-inducing cytokine/chemokine in the S. aureus-infected lungs. Conclusions Accumulation of γδ T cells in the lungs to S. aureus infection is beneficial for bacteria clearance and also contributes to the tissue damage. These cells were the primary source of IL-17, which might influence the recruitment of neutrophils at the early stage of infection.