PLoS ONE (Jan 2011)

Theiler's murine encephalomyelitis virus as a vaccine candidate for immunotherapy.

  • Kevin D Pavelko,
  • Megan A Girtman,
  • Yoshihiro Mitsunaga,
  • Yanice V Mendez-Fernandez,
  • Michael P Bell,
  • Michael J Hansen,
  • Kathleen S Allen,
  • Moses Rodriguez,
  • Larry R Pease

DOI
https://doi.org/10.1371/journal.pone.0020217
Journal volume & issue
Vol. 6, no. 5
p. e20217

Abstract

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The induction of sterilizing T-cell responses to tumors is a major goal in the development of T-cell vaccines for treating cancer. Although specific components of anti-viral CD8+ immunity are well characterized, we still lack the ability to mimic viral CD8+ T-cell responses in therapeutic settings for treating cancers. Infection with the picornavirus Theiler's murine encephalomyelitis virus (TMEV) induces a strong sterilizing CD8+ T-cell response. In the absence of sterilizing immunity, the virus causes a persistent infection. We capitalized on the ability of TMEV to induce strong cellular immunity even under conditions of immune deficiency by modifying the virus to evaluate its potential as a T-cell vaccine. The introduction of defined CD8+ T-cell epitopes into the leader sequence of the TMEV genome generates an attenuated vaccine strain that can efficiently drive CD8+ T-cell responses to the targeted antigen. This virus activates T-cells in a manner that is capable of inducing targeted tissue damage and glucose dysregulation in an adoptive T-cell transfer model of diabetes mellitus. As a therapeutic vaccine for the treatment of established melanoma, epitope-modified TMEV can induce strong cytotoxic T-cell responses and promote infiltration of the T-cells into established tumors, ultimately leading to a delay in tumor growth and improved survival of vaccinated animals. We propose that epitope-modified TMEV is an excellent candidate for further development as a human T-cell vaccine for use in immunotherapy.