PURPOSE: Interleukin (IL)-2 therapy is currently used for therapy of renal cell carcinoma (RCC). However, it is only effective in approximately 10% to 15% of patients, showing a need for additional therapies. We have previously described a replication-defective fowlpox vector encoding three costimulatory molecules (B7-1, ICAM-1, and LFA-3), designated rF-TRICOM. Here, we show that intratumoral administration of rF-TRICOM in an orthotopic RCC model effectively enhances tumor immunogenicity and reduces tumor burden in mice and the combination of rF-TRICOM and IL-2 is more effective than either therapy alone. EXPERIMENTAL DESIGN: RCC cells were implanted under the capsule of the kidney, and mice were given rF-TRICOM intratumorally 14 days later. We compared the effect of rF-TRICOM, rF-granulocyte macrophage colony-stimulating factor (GM-CSF), and two doses of IL-2 and combinations of the above on antitumor efficacy and survival. Host CD4(+) and CD8(+) T-cell responses were also evaluated. RESULTS: The results show that (a) systemic IL-2 therapy was moderately effective in the reduction of tumor burden in an orthotopic RCC model; (b) a single intratumoral injection of rF-TRICOM and rF-GM-CSF significantly reduced tumor burden; (c) the addition of systemic IL-2 to intratumoral rF-TRICOM/rF-GM-CSF administration resulted in further reduction of tumor burden, decrease in the incidence of metastasis, and extended survival in tumor-bearing mice above that seen with either treatment alone; and (d) CD8(+) T cells played a critical role in the antitumor effect seen with rF-TRICOM/rF-GM-CSF + IL-2 therapy. Finally, the addition of systemic recombinant IL-15 or intratumoral vector-delivered IL-15 to intratumoral rF-TRICOM/rF-GM-CSF administration resulted in substantially more tumor-free mice than either therapy alone. CONCLUSIONS: These studies show that intratumoral administration of rF-TRICOM admixed with rF-GM-CSF is effective at reducing tumor burden in mice and the addition of IL-2 further contributes to this effect. These studies thus form the rationale for combination immunotherapy clinical trials in patients with RCC.
PURPOSE:Interleukin (IL)-2 therapy is currently used for therapy of renal cell carcinoma (RCC). However, it is only effective in approximately 10% to 15% of patients, showing a need for additional therapies. We have previously described a replication-defective fowlpox vector encoding three costimulatory molecules (B7-1, ICAM-1, and LFA-3), designated rF-TRICOM. Here, we show that intratumoral administration of rF-TRICOM in an orthotopic RCC model effectively enhances tumor immunogenicity and reduces tumor burden in mice and the combination of rF-TRICOM and IL-2 is more effective than either therapy alone. EXPERIMENTAL DESIGN:RCC cells were implanted under the capsule of the kidney, and mice were given rF-TRICOM intratumorally 14 days later. We compared the effect of rF-TRICOM, rF-granulocyte macrophage colony-stimulating factor (GM-CSF), and two doses of IL-2 and combinations of the above on antitumor efficacy and survival. Host CD4(+) and CD8(+) T-cell responses were also evaluated. RESULTS: The results show that (a) systemic IL-2 therapy was moderately effective in the reduction of tumor burden in an orthotopic RCC model; (b) a single intratumoral injection of rF-TRICOM and rF-GM-CSF significantly reduced tumor burden; (c) the addition of systemic IL-2 to intratumoral rF-TRICOM/rF-GM-CSF administration resulted in further reduction of tumor burden, decrease in the incidence of metastasis, and extended survival in tumor-bearing mice above that seen with either treatment alone; and (d) CD8(+) T cells played a critical role in the antitumor effect seen with rF-TRICOM/rF-GM-CSF + IL-2 therapy. Finally, the addition of systemic recombinant IL-15 or intratumoral vector-delivered IL-15 to intratumoral rF-TRICOM/rF-GM-CSF administration resulted in substantially more tumor-free mice than either therapy alone. CONCLUSIONS: These studies show that intratumoral administration of rF-TRICOM admixed with rF-GM-CSF is effective at reducing tumor burden in mice and the addition of IL-2 further contributes to this effect. These studies thus form the rationale for combination immunotherapy clinical trials in patients with RCC.
Authors: Jeffrey S Miller; Chihiro Morishima; Douglas G McNeel; Manish R Patel; Holbrook E K Kohrt; John A Thompson; Paul M Sondel; Heather A Wakelee; Mary L Disis; Judith C Kaiser; Martin A Cheever; Howard Streicher; Steven P Creekmore; Thomas A Waldmann; Kevin C Conlon Journal: Clin Cancer Res Date: 2017-12-04 Impact factor: 12.531
Authors: Kevin C Conlon; Enrico Lugli; Hugh C Welles; Steven A Rosenberg; Antonio Tito Fojo; John C Morris; Thomas A Fleisher; Sigrid P Dubois; Liyanage P Perera; Donn M Stewart; Carolyn K Goldman; Bonita R Bryant; Jean M Decker; Jing Chen; Tat'Yana A Worthy; William D Figg; Cody J Peer; Michael C Sneller; H Clifford Lane; Jason L Yovandich; Stephen P Creekmore; Mario Roederer; Thomas A Waldmann Journal: J Clin Oncol Date: 2014-11-17 Impact factor: 44.544
Authors: Kevin C Conlon; E Lake Potter; Stefania Pittaluga; Chyi-Chia Richard Lee; Milos D Miljkovic; Thomas A Fleisher; Sigrid Dubois; Bonita R Bryant; Michael Petrus; Liyanage P Perera; Jennifer Hsu; William D Figg; Cody J Peer; Joanna H Shih; Jason L Yovandich; Stephen P Creekmore; Mario Roederer; Thomas A Waldmann Journal: Clin Cancer Res Date: 2019-05-29 Impact factor: 12.531
Authors: Thomas A Waldmann; Enrico Lugli; Mario Roederer; Liyanage P Perera; Jeremy V Smedley; Rhonda P Macallister; Carolyn K Goldman; Bonita R Bryant; Jean M Decker; Thomas A Fleisher; H Clifford Lane; Michael C Sneller; Roger J Kurlander; David E Kleiner; John M Pletcher; William D Figg; Jason L Yovandich; Stephen P Creekmore Journal: Blood Date: 2011-03-08 Impact factor: 22.113
Authors: Jennifer A Westwood; Titaina C U Potdevin Hunnam; Hollie J Pegram; Rodney J Hicks; Phillip K Darcy; Michael H Kershaw Journal: PLoS One Date: 2014-05-02 Impact factor: 3.240
Authors: Jean Gabriel de Souza; Katia L.P. Morais; Eduardo Anglés-Cano; Pamela Boufleur; Evandro Sobroza de Mello; Durvanei Augusto Maria; Clarice Silvia Taemi Origassa; Hamilton de Campos Zampolli; Niels Olsen Saraiva Câmara; Carolina Maria Berra; Rosemary Viola Bosch; Ana Marisa Chudzinski-Tavassi Journal: Oncotarget Date: 2016-09-20