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| Paper |
| Intratumoral coinjection of adenoviral vectors expressing IL-2 and IL-12 results in enhanced frequency of regression of injected and untreated distal tumors |
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| C L Addison1,b, J L Bramson1,3,c, M M Hitt1, W J Muller3, J Gauldie3 and F L Graham1,3,a |
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1Department of Biology, McMaster University, Hamilton, Ontario, Canada
3Department of Pathology, McMaster University, Hamilton, Ontario, Canada
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aCorrespondence: FL Graham, Department of Biology, McMaster University, 1280 Main Street West, Hamilton, Ontario, Canada, L8S 4K1 bPresent addresses: University of Michigan, Division of Pulmonary and Critical Care Medicine, 1150 West Medical Center Drive, Ann Arbor, Michigan, USA, 48109-0642; cInex Pharmaceuticals, 1779 75th Avenue West, Vancouver, British Columbia, Canada, V6P 6P2 |
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| Abstract |
| We have studied the ability of adenoviral (Ad) vectors expressing the cytokines IL-2 or IL-12 to mediate regression of established tumors in a mouse model of mammary adenocarcinoma. Previous results indicated that intratumoral injection of vectors expressing IL-2 (AdCAIL-2) or IL-12 (AdmIL-12.1) induced complete tumor regression in approximately 30-40% of treated animals. In the current studies, we investigated the mechanism of tumor killing in responding animals and the efficacy of AdIL-2 and AdIL-12 vector administration in combination compared with the use of either vector alone. Animals bearing subcutaneous mammary tumors were injected intratumorally with Ad vectors expressing IL-2 or IL-12 or were coinjected with both vectors. Animals receiving the combination treatment responded substantially better than animals which had received either vector alone, with 65% of animals treated with both vectors undergoing complete tumor regression. In all three treatment regimens, tumor regression was associated with the presence of specific antitumor antigen cytotoxic T-lymphocytes (CTLs), which secreted elevated levels of IFN- . Consistent with circulating CTLs being involved in regression, when animals bearing bilateral tumors were inoculated in a single tumor with IL-2 or IL-12 expressing vectors, both tumors regressed in many cases. Again, treatment with both AdCAIL-2 and AdmIL-12.1 was most effective, with 63% of animals undergoing complete regression of both treated and untreated tumors, compared to 18 or 22% of animals injected with either AdCAIL-2 or AdmIL-12.1 alone. These data indicate that the combination of IL-2 and IL-12 is a more effective inducer of antitumor immune responses than either one alone, and that the resulting antitumor responses are effective in mediating the regression of distal untreated tumors, a property which may aid in the treatment of metastatic disease. |
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| Keywords |
| immunotherapy; cancer; gene therapy; adenovirus; cytokines |
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| Received 6 November 1997; accepted 24 April 1998 |
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| October 1998, Volume 5, Number 10, Pages 1400-1409 |
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