Gene gun-mediated skin transfection with interleukin 12 gene results in regression of established primary and metastatic murine tumors.

Abstract: Particle-mediated (gene gun) in vivo delivery of the murine interleukin 12 (IL-12) gene in an expression plasmid was evaluated for antitumor activity. Transfer of IL-12 cDNA into epidermal cells overlying an implanted intradermal tumor resulted in detectable levels (266.0 ± 27.8 pg) of the transgenic protein at the skin tissue treatment site. Despite these low levels of transgenic IL-12, complete regression of established tumors (0.4-0.8 cm in diameter) was achieved in mice bearing Renca, MethA, SA-1, or L5178… Show more

“…These cytokines were repeatedly shown to exhibit functional biological activity, as many researchers have previously reported. 22,29,30 A comparison of the results from our current study versus those reported by Rajagopalan and Malter 22 suggests that 3 0 cDNA structural features may influence transgenic protein expression via additional mechanisms besides mRNA stability and polysome-run-on efficiency. It is currently unclear to us as to which mechanism(s) (eg, RNA stability) is playing the key role for enhanced cytokine gene expression, and additional experiments are needed to demonstrate the possible post-transcriptional, translational or other processing regulations of these transgenic RNA or DNA vector systems.…”

“…The quantity of transgenic murine IL-12 protein heterodimer was determined by a cell proliferation bioassay using ConA-activated splenocytes, as previously described. 30 Human IL-12 levels were determined via a p35/p40 heterodimer-specific ELISA kit (R&D Systems, Minneapolis, MN, USA). Based on results from this study, we estimate that an increase of at least seven to 30-fold in various cytokine transgene expression levels could be readily obtained by employing a combination of such molecular strategies for vector, promoter or other sequence constructions.…”

“…This was demonstrated by their capacity to elicit CTL or histological inflammatory activity and potent antitumor activities effectively. 12,13,29,[30][31][32] Together with the findings of the relative capacities of different cDNA constructs in the current study, we believe that these results can be usefully employed by researchers for the proper and specified use of 3 0 UTR deletion for cytokine expression vectors in a clinically relevant study, that is, different as well as the same cytokine species can differ drastically in transgene expression under different in vivo and ex vitro conditions, and hence specific cytokine expression vectors do need to be carefully tested in target or related cells/tissues before clinical studies.…”

“…In previous studies on cytokine gene expression, it has been documented that mutating the AU-rich sequences of mRNA in the 3 0 UTR can effectively enhance mRNA stability, resulting in an augmented transgenic cytokine protein expression [18][19][20]22,30 These results were accomplished via an overlapping PCR technique, in which the AUUUA regions of the 3 0 UTR were replaced with AUGUA pentamer repeats. 20,22 There were also suggestions that a group of cytokine gene constructs, with the 3 0 UTR totally removed by cDNA cloning, expressed very well in transgenic studies.…”

Molecular strategies for improving cytokine transgene expression in normal and malignant tissues

“…These cytokines were repeatedly shown to exhibit functional biological activity, as many researchers have previously reported. 22,29,30 A comparison of the results from our current study versus those reported by Rajagopalan and Malter 22 suggests that 3 0 cDNA structural features may influence transgenic protein expression via additional mechanisms besides mRNA stability and polysome-run-on efficiency. It is currently unclear to us as to which mechanism(s) (eg, RNA stability) is playing the key role for enhanced cytokine gene expression, and additional experiments are needed to demonstrate the possible post-transcriptional, translational or other processing regulations of these transgenic RNA or DNA vector systems.…”

“…The quantity of transgenic murine IL-12 protein heterodimer was determined by a cell proliferation bioassay using ConA-activated splenocytes, as previously described. 30 Human IL-12 levels were determined via a p35/p40 heterodimer-specific ELISA kit (R&D Systems, Minneapolis, MN, USA). Based on results from this study, we estimate that an increase of at least seven to 30-fold in various cytokine transgene expression levels could be readily obtained by employing a combination of such molecular strategies for vector, promoter or other sequence constructions.…”

“…This was demonstrated by their capacity to elicit CTL or histological inflammatory activity and potent antitumor activities effectively. 12,13,29,[30][31][32] Together with the findings of the relative capacities of different cDNA constructs in the current study, we believe that these results can be usefully employed by researchers for the proper and specified use of 3 0 UTR deletion for cytokine expression vectors in a clinically relevant study, that is, different as well as the same cytokine species can differ drastically in transgene expression under different in vivo and ex vitro conditions, and hence specific cytokine expression vectors do need to be carefully tested in target or related cells/tissues before clinical studies.…”

“…In previous studies on cytokine gene expression, it has been documented that mutating the AU-rich sequences of mRNA in the 3 0 UTR can effectively enhance mRNA stability, resulting in an augmented transgenic cytokine protein expression [18][19][20]22,30 These results were accomplished via an overlapping PCR technique, in which the AUUUA regions of the 3 0 UTR were replaced with AUGUA pentamer repeats. 20,22 There were also suggestions that a group of cytokine gene constructs, with the 3 0 UTR totally removed by cDNA cloning, expressed very well in transgenic studies.…”

Molecular strategies for improving cytokine transgene expression in normal and malignant tissues

“…These include injection of genetically engineered fibroblasts for the secretion of IL-12 in an orthotopic melanoma model; direct transfer of IL-12 cDNA via gene gun-mediated transfection of skin tissue overlaying subcutaneous melanomas; direct intratumoral injection of adenovirus expressing IL-12 in ectopic breast and colon cancer models; and intradermal injection of IL-12 cDNA and vaccination using irradiated IL-12-transfected tumor cells in a metastatic colon cancer model. [15][16][17][18][19][20][21] These models suggest that IL-12 gene therapy results in tumor regression and suppression of metastasis.…”

Adenovirus-mediated interleukin-12 gene therapy for prostate cancer: suppression of orthotopic tumor growth and pre-established lung metastases in an orthotopic model

Active specific immunotherapy with polyvalent melanoma cell vaccine for patients with in-transit melanoma metastases