BMC Immunology (May 2011)

Efficient induction of CD25<sup>- </sup>iTreg by co-immunization requires strongly antigenic epitopes for T cells

  • Li Jinyao,
  • Jin Huali,
  • Pavlakis George,
  • Kang Youmin,
  • Yu Yang,
  • Geng Shuang,
  • Hu Yanxin,
  • Hu Weibin,
  • Wang Shuang,
  • Wang Bin

DOI
https://doi.org/10.1186/1471-2172-12-27
Journal volume & issue
Vol. 12, no. 1
p. 27

Abstract

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Abstract Background We previously showed that co-immunization with a protein antigen and a DNA vaccine coding for the same antigen induces CD40low IL-10high tolerogenic DCs, which in turn stimulates the expansion of antigen-specific CD4+CD25-Foxp3+ regulatory T cells (CD25- iTreg). However, it was unclear how to choose the antigen sequence to maximize tolerogenic antigen presentation and, consequently, CD25- iTreg induction. Results In the present study, we demonstrated the requirement of highly antigenic epitopes for CD25- iTreg induction. Firstly, we showed that the induction of CD25- iTreg by tolerogenic DC can be blocked by anti-MHC-II antibody. Next, both the number and the suppressive activity of CD25- iTreg correlated positively with the overt antigenicity of an epitope to activate T cells. Finally, in a mouse model of dermatitis, highly antigenic epitopes derived from a flea allergen not only induced more CD25- iTreg, but also more effectively prevented allergenic reaction to the allergen than did weakly antigenic epitopes. Conclusions Our data thus indicate that efficient induction of CD25- iTreg requires highly antigenic peptide epitopes. This finding suggests that highly antigenic epitopes should be used for efficient induction of CD25- iTreg for clinical applications such as flea allergic dermatitis.