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Human Gene Therapy
Phase I Study of Liposome–DNA Complexes Encoding the Interleukin-2 Gene in Dogs with Osteosarcoma Lung Metastases

To cite this article:
Steven Dow, Robyn Elmslie, Ilene Kurzman, Gregory Macewen, Federica Pericle, Denny Liggitt. Human Gene Therapy. August 2005, 16(8): 937-946. doi:10.1089/hum.2005.16.937.

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Dr. Steven Dow
Department of Clinical Sciences, Colorado State University, Fort Collins, CO 80523.
Robyn Elmslie
Veterinary Cancer Specialists, Englewood, CO 80110.
Ilene Kurzman
Department of Veterinary Medical Sciences, University of Wisconsin, Madison, WI 53706.
Gregory Macewen
Department of Veterinary Medical Sciences, University of Wisconsin, Madison, WI 53706.
Federica Pericle
Valentis, Burlingame, CA 94010.
Denny Liggitt
Department of Comparative Pathology, University of Washington, Seattle, WA 98105.

Systemic gene delivery using cationic liposome–DNA complexes (LDCs) has been shown to elicit potent antitumor activity in mice with tumor metastases to the lungs. However, intravenous gene delivery for treatment of established cancer has not been evaluated previously in a spontaneous, large animal model. We therefore evaluated the safety, toxicity, and efficacy of intravenous gene delivery, using LDCs in dogs with established tumor metastases. Twenty dogs with chemotherapy-resistant osteosarcoma metastases to the lungs received a series of intravenous infusions of cationic liposomes and plasmid DNA encoding the canine interleukin-2 (IL-2) cDNA. Effects of intravenous gene delivery on immune activation, clinical and hematologic parameters, tumor responses, and survival times were assessed. We found that slow intravenous administration of IL-2 LDCs resulted in detectable IL-2 transgene expression in lung tissues of dogs. Repeated intravenous infusions of LDCs were well tolerated by dogs with lung tumor metastases and elicited systemic immune activation, as reflected by fever, leukogram changes, monocyte activation, and increased natural killer cell activity. Three of 20 dogs experienced partial or complete regression of lung metastases after infusion of IL-2 LDCs. Overall survival times were significantly increased in treated dogs compared with historical control animals with the same stage of disease. We conclude that repeated intravenous infusion of LDCs in cancerbearing dogs is safe and well tolerated at low doses and may be capable of eliciting antitumor activity in some animals with advanced tumor metastases.

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