Antigen Availability Shapes T Cell Differentiation and Function during Tuberculosis.

نویسندگان

  • Albanus O Moguche
  • Munyaradzi Musvosvi
  • Adam Penn-Nicholson
  • Courtney R Plumlee
  • Helen Mearns
  • Hennie Geldenhuys
  • Erica Smit
  • Deborah Abrahams
  • Virginie Rozot
  • One Dintwe
  • Søren T Hoff
  • Ingrid Kromann
  • Morten Ruhwald
  • Peter Bang
  • Ryan P Larson
  • Shahin Shafiani
  • Shuyi Ma
  • David R Sherman
  • Alessandro Sette
  • Cecilia S Lindestam Arlehamn
  • Denise M McKinney
  • Holden Maecker
  • Willem A Hanekom
  • Mark Hatherill
  • Peter Andersen
  • Thomas J Scriba
  • Kevin B Urdahl
چکیده

CD4 T cells are critical for protective immunity against Mycobacterium tuberculosis (Mtb), the cause of tuberculosis (TB). Yet to date, TB vaccine candidates that boost antigen-specific CD4 T cells have conferred little or no protection. Here we examined CD4 T cell responses to two leading TB vaccine antigens, ESAT-6 and Ag85B, in Mtb-infected mice and in vaccinated humans with and without underlying Mtb infection. In both species, Mtb infection drove ESAT-6-specific T cells to be more differentiated than Ag85B-specific T cells. The ability of each T cell population to control Mtb in the lungs of mice was restricted for opposite reasons: Ag85B-specific T cells were limited by reduced antigen expression during persistent infection, whereas ESAT-6-specific T cells became functionally exhausted due to chronic antigenic stimulation. Our findings suggest that different vaccination strategies will be required to optimize protection mediated by T cells recognizing antigens expressed at distinct stages of Mtb infection.

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عنوان ژورنال:
  • Cell host & microbe

دوره 21 6  شماره 

صفحات  -

تاریخ انتشار 2017