Cell & Bioscience (Jan 2011)

<it>In vivo </it>microRNA-155 expression influences antigen-specific T cell-mediated immune responses generated by DNA vaccination

  • Mao Chih-Ping,
  • He Liangmei,
  • Tsai Ya-Chea,
  • Peng Shiwen,
  • Kang Tae,
  • Pang Xiaowu,
  • Monie Archana,
  • Hung Chien-Fu,
  • Wu T-C

DOI
https://doi.org/10.1186/2045-3701-1-3
Journal volume & issue
Vol. 1, no. 1
p. 3

Abstract

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Abstract Background MicroRNA (miRNA) molecules are potent mediators of post-transcriptional gene silencing that are emerging to be critical in the regulation of innate and adaptive immunity. Results Here we report that miR-155--an oncogenic miRNA with important function in the mammalian immune system--is induced in dendritic cells (DCs) upon maturation and potentially attenuates their ability to activate T cells. Biolistic epidermal transfection with DNA encoding miR-155 suppressed the induction of antigen-specific T cell-mediated immunity, whereas reduction of endogenous miR-155 by a partially complementary antisense sequence reversed this effect. Because DCs represent a significant component of epidermal tissue and are among the most potent of antigen-presenting cells, the inhibitory actions of miR-155 could be mediated through this subset of cells. Conclusions These results suggest that miR-155 may repress the expression of key molecules involved in lymph node migration, antigen presentation, or T cell activation in DCs, and thus forms part of a negative regulatory pathway that dampens the generation of T cell-mediated immune responses. Modulation of miR-155 expression in epidermis therefore represents a potentially promising form of gene therapy for the control of diseases ranging from autoimmunity to cancer and viral infection.