Molecular Therapy: Oncolytics (Sep 2021)

Potent anti-tumor effects of receptor-retargeted syncytial oncolytic herpes simplex virus

  • Takuma Suzuki,
  • Hiroaki Uchida,
  • Tomoko Shibata,
  • Yasuhiko Sasaki,
  • Hitomi Ikeda,
  • Mika Hamada-Uematsu,
  • Ryota Hamasaki,
  • Kosaku Okuda,
  • Shigeru Yanagi,
  • Hideaki Tahara

Journal volume & issue
Vol. 22
pp. 265 – 276

Abstract

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Most oncolytic virotherapy has thus far employed viruses deficient in genes essential for replication in normal cells but not in cancer cells. Intra-tumoral injection of such viruses has resulted in clinically significant anti-tumor effects on the lesions in the vicinity of the injection sites but not on distant visceral metastases. To overcome this limitation, we have developed a receptor-retargeted oncolytic herpes simplex virus employing a single-chain antibody for targeting tumor-associated antigens (RR-oHSV) and its modified version with additional mutations conferring syncytium formation (RRsyn-oHSV). We previously showed that RRsyn-oHSV exhibits preserved antigen specificity and an ∼20-fold higher tumoricidal potency in vitro relative to RR-oHSV. Here, we investigated the in vivo anti-tumor effects of RRsyn-oHSV using human cancer xenografts in immunodeficient mice. With only a single intra-tumoral injection of RRsyn-oHSV at very low doses, all treated tumors regressed completely. Furthermore, intra-venous administration of RRsyn-oHSV resulted in robust anti-tumor effects even against large tumors. We found that these potent anti-tumor effects of RRsyn-oHSV may be associated with the formation of long-lasting tumor cell syncytia not containing non-cancerous cells that appear to trigger death of the syncytia. These results strongly suggest that cancer patients with distant metastases could be effectively treated with our RRsyn-oHSV.

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