PLoS Pathogens (Dec 2009)

Analysis of FOXP3+ regulatory T cells that display apparent viral antigen specificity during chronic hepatitis C virus infection.

  • Shuo Li,
  • Stefan Floess,
  • Alf Hamann,
  • Silvana Gaudieri,
  • Andrew Lucas,
  • Margaret Hellard,
  • Stuart Roberts,
  • Geza Paukovic,
  • Magdalena Plebanski,
  • Bruce E Loveland,
  • Campbell Aitken,
  • Simon Barry,
  • Louis Schofield,
  • Eric J Gowans

DOI
https://doi.org/10.1371/journal.ppat.1000707
Journal volume & issue
Vol. 5, no. 12
p. e1000707

Abstract

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We reported previously that a proportion of natural CD25(+) cells isolated from the PBMC of HCV patients can further upregulate CD25 expression in response to HCV peptide stimulation in vitro, and proposed that virus-specific regulatory T cells (Treg) were primed and expanded during the disease. Here we describe epigenetic analysis of the FOXP3 locus in HCV-responsive natural CD25(+) cells and show that these cells are not activated conventional T cells expressing FOXP3, but hard-wired Treg with a stable FOXP3 phenotype and function. Of approximately 46,000 genes analyzed in genome wide transcription profiling, about 1% were differentially expressed between HCV-responsive Treg, HCV-non-responsive natural CD25(+) cells and conventional T cells. Expression profiles, including cell death, activation, proliferation and transcriptional regulation, suggest a survival advantage of HCV-responsive Treg over the other cell populations. Since no Treg-specific activation marker is known, we tested 97 NS3-derived peptides for their ability to elicit CD25 response (assuming it is a surrogate marker), accompanied by high resolution HLA typing of the patients. Some reactive peptides overlapped with previously described effector T cell epitopes. Our data offers new insights into HCV immune evasion and tolerance, and highlights the non-self specific nature of Treg during infection.