PLoS Pathogens (Jan 2013)

Preclinical therapy of disseminated HER-2⁺ ovarian and breast carcinomas with a HER-2-retargeted oncolytic herpesvirus.

  • Patrizia Nanni,
  • Valentina Gatta,
  • Valentina Gatta,
  • Laura Menotti,
  • Carla De Giovanni,
  • Marianna Ianzano,
  • Arianna Palladini,
  • Valentina Grosso,
  • Massimiliano Dall'ora,
  • Stefania Croci,
  • Giordano Nicoletti,
  • Lorena Landuzzi,
  • Manuela Iezzi,
  • Gabriella Campadelli-Fiume,
  • Pier-Luigi Lollini

DOI
https://doi.org/10.1371/journal.ppat.1003155
Journal volume & issue
Vol. 9, no. 1
p. e1003155

Abstract

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Oncolytic viruses aim to specifically kill tumor cells. A major challenge is the effective targeting of disseminated tumors in vivo. We retargeted herpes simplex virus (HSV) tropism to HER-2 oncoprotein p185, overexpressed in ovary and breast cancers. The HER-2-retargeted R-LM249 exclusively infects and kills tumor cells expressing high levels of human HER-2. Here, we assessed the efficacy of systemically i.p. delivered R-LM249 against disseminated tumors in mouse models that recapitulate tumor spread to the peritoneum in women. The human ovarian carcinoma SK-OV-3 cells implanted intraperitoneally (i.p.) in immunodeficient Rag2⁻/⁻;Il2rg⁻/⁻ mice gave rise to a progressive peritoneal carcinomatosis which mimics the fatal condition in advanced human patients. I.p. administration of R-LM249 strongly inhibited carcinomatosis, resulting in 60% of mice free from peritoneal diffusion, and 95% reduction in the total weight of neoplastic nodules. Intraperitoneal metastases are a common outcome in breast cancer: i.p. administration of R-LM249 strongly inhibited the growth of ovarian metastases of HER-2+ MDA-MB-453 breast cells. Brain metastases were also reduced. Cumulatively, upon i.p. administration the HER-2-redirected oncolytic HSV effectively reduced the growth of ovarian and breast carcinoma disseminated to the peritoneal cavity.