γδ T cells recognize a microbial encoded B cell antigen to initiate a rapid antigen-specific interleukin-17 response.

نویسندگان

  • Xun Zeng
  • Yu-Ling Wei
  • Jun Huang
  • Evan W Newell
  • Hongxiang Yu
  • Brian A Kidd
  • Michael S Kuhns
  • Ray W Waters
  • Mark M Davis
  • Casey T Weaver
  • Yueh-hsiu Chien
چکیده

γδ T cells contribute uniquely to immune competence. Nevertheless, how they function remains an enigma. It is unclear what most γδ T cells recognize, what is required for them to mount an immune response, and how the γδ T cell response is integrated into host immune defense. Here, we report that a noted B cell antigen, the algae protein phycoerythrin (PE), is a murine and human γδ T cell antigen. Employing this specificity, we demonstrated that antigen recognition activated naive γδ T cells to make interleukin-17 and respond to cytokine signals that perpetuate the response. High frequencies of antigen-specific γδ T cells in naive animals and their ability to mount effector response without extensive clonal expansion allow γδ T cells to initiate a swift, substantial response. These results underscore the adaptability of lymphocyte antigen receptors and suggest an antigen-driven rapid response in protective immunity prior to the maturation of classical adaptive immunity.

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عنوان ژورنال:
  • Immunity

دوره 37 3  شماره 

صفحات  -

تاریخ انتشار 2012