PLoS ONE (Jan 2014)

Limited density of an antigen presented by RMA-S cells requires B7-1/CD28 signaling to enhance T-cell immunity at the effector phase.

  • Xiao-Lin Li,
  • Marjolein Sluijter,
  • Elien M Doorduijn,
  • Shubha P Kale,
  • Harris McFerrin,
  • Yong-Yu Liu,
  • Yan Li,
  • Madhusoodanan Mottamal,
  • Xin Yao,
  • Fengkun Du,
  • Baihan Gu,
  • Kim Hoang,
  • Yen H Nguyen,
  • Nichelle Taylor,
  • Chelsea R Stephens,
  • Thorbald van Hall,
  • Qian-Jin Zhang

DOI
https://doi.org/10.1371/journal.pone.0108192
Journal volume & issue
Vol. 9, no. 11
p. e108192

Abstract

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The association of B7-1/CD28 between antigen presenting cells (APCs) and T-cells provides a second signal to proliferate and activate T-cell immunity at the induction phase. Many reports indicate that tumor cells transfected with B7-1 induced augmented antitumor immunity at the induction phase by mimicking APC function; however, the function of B7-1 on antitumor immunity at the effector phase is unknown. Here, we report direct evidence of enhanced T-cell antitumor immunity at the effector phase by the B7-1 molecule. Our experiments in vivo and in vitro indicated that reactivity of antigen-specific monoclonal and polyclonal T-cell effectors against a Lass5 epitope presented by RMA-S cells is increased when the cells expressed B7-1. Use of either anti-B7-1 or anti-CD28 antibodies to block the B7-1/CD28 association reduced reactivity of the T effectors against B7-1 positive RMA-S cells. Transfection of Lass5 cDNA into or pulse of Lass5 peptide onto B7-1 positive RMA-S cells overcomes the requirement of the B7-1/CD28 signal for T effector response. To our knowledge, the data offers, for the first time, strong evidence that supports the requirement of B7-1/CD28 secondary signal at the effector phase of antitumor T-cell immunity being dependent on the density of an antigenic peptide.