OncoImmunology (Jul 2018)

Transforming the prostatic tumor microenvironment with oncolytic virotherapy

  • Matthew J. Atherton,
  • Kyle B. Stephenson,
  • Fanny Tzelepis,
  • David Bakhshinyan,
  • Jake K. Nikota,
  • Hwan Hee Son,
  • Anna Jirovec,
  • Charles Lefebvre,
  • Anna Dvorkin-Gheva,
  • Ali A. Ashkar,
  • Yonghong Wan,
  • David F. Stojdl,
  • Eric C. Belanger,
  • Rodney H. Breau,
  • John C. Bell,
  • Fred Saad,
  • Sheila K. Singh,
  • Jean-Simone Diallo,
  • Brian D. Lichty

DOI
https://doi.org/10.1080/2162402X.2018.1445459
Journal volume & issue
Vol. 7, no. 7

Abstract

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Prostate cancer (PCa) was estimated to have the second highest global incidence rate for male non-skin tumors and is the fifth most deadly in men thus mandating the need for novel treatment options. MG1-Maraba is a potent and versatile oncolytic virus capable of lethally infecting a variety of prostatic tumor cell lines alongside primary PCa biopsies and exerts direct oncolytic effects against large TRAMP-C2 tumors in vivo. An oncolytic immunotherapeutic strategy utilizing a priming vaccine and intravenously administered MG1-Maraba both expressing the human six-transmembrane antigen of the prostate (STEAP) protein generated specific CD8+ T-cell responses against multiple STEAP epitopes and resulted in functional breach of tolerance. Treatment of mice with bulky TRAMP-C2 tumors using oncolytic STEAP immunotherapy induced an overt delay in tumor progression, marked intratumoral lymphocytic infiltration with an active transcriptional profile and up-regulation of MHC class I. The preclinical data generated here offers clear rationale for clinically evaluating this approach for men with advanced PCa.

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