Immuno-gene therapy with adenoviruses expressing fms-like tyrosine kinase 3 ligand and CD40 ligand for mouse hepatoma cells in vivo

  • Authors:
    • Kenji Yanagi
    • Yuji Nagayama
    • Kazuhiko Nakao
    • Akira Saeki
    • Koujirou Matsumoto
    • Tatsuki Ichikawa
    • Hiroki Ishikawa
    • Keisuke Hamasaki
    • Nobuko Ishii
    • Katsumi Eguchi
  • View Affiliations

  • Published online on: February 1, 2003     https://doi.org/10.3892/ijo.22.2.345
  • Pages: 345-351
Metrics: Total Views: 0 (Spandidos Publications: | PMC Statistics: )
Total PDF Downloads: 0 (Spandidos Publications: | PMC Statistics: )


Abstract

Introduction of genes encoding immuno-stimulatory cytokines into cancer cells is known to enhance antitumor immunity. CD40 ligand (CD40L, CD154) and fms-like tyrosine kinase 3 ligand (Flt3L) are recently identified cytokines, which have been demonstrated to stimulate antitumor immunity in several cancer models. However little is known about antitumor activity of Ftl3L and CD40L against hepatocellular carcinoma (HCC). In the present study, we constructed replication-defective adenoviruses expressing Flt3L and CD40L and examined their therapeutic efficacy on mouse HCC, MH134 cells. Subcutaneous injection of MH134 cells genetically engineered to express Flt3L and/or CD40L developed tumors in all the syngeneic immunocompetent mice, but tumor growth was significantly delayed as compared to control mice. Partial inhibition of this antitumor effect in athymic nude mice suggests that both innate and adaptive immunity appear to play a role. It was shown by immunodepletion of NK cells with anti-asialo-GM1 antibody that the effector cells involved in innate immunity are NK cells. In a therapeutic setting, however, injection of adenovirus expressing Flt3L or CD40L into pre-established MH134 tumors exhibited no efficacy. These data demonstrate that Flt3L and CD40L induce significant, but only weak, antitumor immunity against MH134 cells presumably through both innate and adaptive immunity. Our results suggest that immuno-gene therapy with Flt3L and CD40L may need adjuvant modalities to achieve strong immune response.

Related Articles

Journal Cover

February 2003
Volume 22 Issue 2

Print ISSN: 1019-6439
Online ISSN:1791-2423

Sign up for eToc alerts

Recommend to Library

Copy and paste a formatted citation
x
Spandidos Publications style
Yanagi K, Nagayama Y, Nakao K, Saeki A, Matsumoto K, Ichikawa T, Ishikawa H, Hamasaki K, Ishii N, Eguchi K, Eguchi K, et al: Immuno-gene therapy with adenoviruses expressing fms-like tyrosine kinase 3 ligand and CD40 ligand for mouse hepatoma cells in vivo. Int J Oncol 22: 345-351, 2003.
APA
Yanagi, K., Nagayama, Y., Nakao, K., Saeki, A., Matsumoto, K., Ichikawa, T. ... Eguchi, K. (2003). Immuno-gene therapy with adenoviruses expressing fms-like tyrosine kinase 3 ligand and CD40 ligand for mouse hepatoma cells in vivo. International Journal of Oncology, 22, 345-351. https://doi.org/10.3892/ijo.22.2.345
MLA
Yanagi, K., Nagayama, Y., Nakao, K., Saeki, A., Matsumoto, K., Ichikawa, T., Ishikawa, H., Hamasaki, K., Ishii, N., Eguchi, K."Immuno-gene therapy with adenoviruses expressing fms-like tyrosine kinase 3 ligand and CD40 ligand for mouse hepatoma cells in vivo". International Journal of Oncology 22.2 (2003): 345-351.
Chicago
Yanagi, K., Nagayama, Y., Nakao, K., Saeki, A., Matsumoto, K., Ichikawa, T., Ishikawa, H., Hamasaki, K., Ishii, N., Eguchi, K."Immuno-gene therapy with adenoviruses expressing fms-like tyrosine kinase 3 ligand and CD40 ligand for mouse hepatoma cells in vivo". International Journal of Oncology 22, no. 2 (2003): 345-351. https://doi.org/10.3892/ijo.22.2.345