Recruitment Of Neutrophils Mediated By V Gamma 2 Gamma Delta T Cells Deteriorates Liver Fibrosis Induced By Schistosoma Japonicum Infection In C57bl/6 Mice

INFECTION AND IMMUNITY(2017)

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摘要
Conventional adaptive T cell responses contribute to the pathogenesis of Schistosoma japonicum infection, leading to liver fibrosis. However, the role of gamma-delta (gamma delta) T cells in this disease is less clear. gamma delta T cells are known to secrete interleukin-17 (IL-17) in response to infection, exerting either protective or pathogenic functions. In the present study, mice infected with S. japonicum are used to characterize the role of gamma delta T cells. Combined with the infection of S. japonicum, an extremely significant increase in the percentage of neutrophils in the CD45(+) cells was detected (from approximately 2.45% to 46.10% in blood and from 0.18% to 7.34% in spleen). Further analysis identified two different gamma delta T cell subsets that have different functions in the formation of granulomas in S. japonicum-infected mice. The V gamma 1 T cells secrete gamma interferon (IFN-gamma) only, while the V gamma 2 T cells secrete both IL-17A and IFN-gamma. Both subtypes lose the ability to secrete cytokine during the late stage of infection (12 weeks postinfection). When we depleted the V gamma 2 T cells in infected mice, the percentage of neutrophils in blood and spleen decreased significantly, the liver fibrosis in the granulomas was reduced, and the level of IL-17A in the serum decreased (P < 0.05). These results suggest that during S. japonicum infection, V gamma 2 T cells can recruit neutrophils and aggravate liver fibrosis by secreting IL-17A. This is the first report that a subset of gamma delta T cells plays a partial role in the pathological process of schistosome infection.
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关键词
gamma delta T cell, neutrophil, mice, Schistosoma japonicum, liver fibrosis, IL-17A
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