Gene therapy of cancer using an interleukin-2 transmembrane construct (original) (raw)

Cancer Research, 2004

Abstract

658 Selective expression of cytokines on the surface of tumors is likely to stimulate tumor-infiltrating lymphocytes that are primed and already recognize tumor antigens. This may result in enhanced tumor recognition and killing. This gene therapy approach may avoid toxicity associated with systemic therapy with high doses of the cytokines needed to achieve the same effects. In order to test this concept, we have evaluated an IL-2 gene construct that is designed to induce tumor cells to express a membrane bound form of IL-2 (IL-2tm). A mammalian plasmid expression vector was designed to express a fusion gene consisting of human interleukin 2 with a Fc receptor epsilon transmembrane anchor derived from the gamma subunit of the Fc receptor epsilon. We demonstrated that mRNA and protein for the IL-2tm fusion protein was expressed in transfected RD995 tumor cells. Expression of the IL-2tm protein on the tumor cell surface membrane was confirmed by laser confocal microscopy. In order to assess biological function, RD995 transfected with IL-2tm or the empty expression vector (pCMV2b) were implanted subcutaneously into C3H/HEN mice. Non-transfected RD995 was also implanted subcutaneously for tumor growth comparison (control group). Groups of mice implanted with 10 6 or 10 5 RD995 transfected with IL-2tm grew considerably more slowly than RD995 transfected with pCMV2b or non-transfected control RD995 implanted tumors. Further preclinical evaluation of the IL-2tm gene therapy as a possible cancer treatment is underway.

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