Highly Efficient Electro-Gene Therapy of Solid Tumor by Using an Expression Plasmid for the Herpes Simplex Virus Thymidine Kinase Gene

We report successful electro-gene therapy (EGT) by using plasmid DNA for tumor-bearing mice. Subcutaneously inoculated CT26 tumor was subjected to EGT, which consists of intratumoral injection of a naked plasmid encoding a marker gene or a therapeutic gene, followed by in vivo electroporation (EP)....

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Veröffentlicht in:Proceedings of the National Academy of Sciences - PNAS 2000-01, Vol.97 (1), p.354-359
Hauptverfasser: Goto, Tomoaki, Nishi, Toru, Tamura, Takahiko, Dev, Sukhendu B., Takeshima, Hideo, Kochi, Masato, Yoshizato, Kimio, Kuratsu, Jun-ichi, Sakata, Tsuneaki, Hofmann, Gunter A., Ushio, Yukitaka
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Sprache:eng
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Zusammenfassung:We report successful electro-gene therapy (EGT) by using plasmid DNA for tumor-bearing mice. Subcutaneously inoculated CT26 tumor was subjected to EGT, which consists of intratumoral injection of a naked plasmid encoding a marker gene or a therapeutic gene, followed by in vivo electroporation (EP). When this treatment modality is carried out with the plasmid DNA for the green fluorescent protein gene, followed by in vivo EP with the optimized pulse parameters, numerous intensely bright green fluorescent signals appeared within the tumor. EGT, by using the "A" fragment of the diphtheria toxin gene significantly inhibited the growth of tumors, by about 30%, on the flank of mice. With the herpes simplex virus thymidine kinase gene, followed by systemic injection of ganciclovir, EGT was far more effective in retarding tumor growth, varying between 50% and 90%, compared with the other controls. Based on these results, it appears that EGT can be used successfully for treating murine solid tumors.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.97.1.354