1. Preclinical study of an ex vivo gene therapy protocol for hepatocarcinoma.
- Author
-
Lortal, B, Gross, F., Peron, J. M., Pénary, M., Berg, D., Hennebelle, I., Favre, G., and Couderc, B.
- Subjects
LIVER cancer ,GENE therapy ,IMMUNOTHERAPY ,CIRRHOSIS of the liver ,FIBROBLASTS ,ANIMAL models in research ,CLINICAL trials - Abstract
Preclinical studies in several animal models as well as clinical trials have shown a reduction in tumor growth following immunotherapy with interleukin-12 (IL-12). This cytokine is appropriate to test in therapeutic clinical trials to treat hepatocarcinoma (HC), a pathology often associated with hepatitis B or C-induced cirrhosis. The local delivery into the liver would be achieved through ex vivo gene transfer using retroviral (rv) vectors in autologous fibroblast carriers. In support of this clinical trial, a rv vector has been constructed to express coordinately both chains p35 and p40 of human IL-12. Here, we have tested good manufacturing practices (GMP) clinical lots of viral vectors derived from the transfected packaging cell line, PG13rvIL-12. We have also devised methods to facilitate the isolation of fibroblasts from freshly harvested skin specimens, enhance their outgrowth in large-scale cultures and assay IL-12 production following transduction, without any selection and irradiation. Twenty-four human skin specimens were processed to obtain fibroblast suspensions that were typically maintained for up to 8 or 12 passages. The mean ±s.d. overall time for obtaining the required number of transduced cells for the highest IL-12 need was 40 days. The procedure, in accordance with the French medical agency for gene therapy clinical trials, is now ready to begin a clinical trial.Cancer Gene Therapy (2009) 16, 329–337; doi:10.1038/cgt.2008.88; published online 7 November 2008 [ABSTRACT FROM AUTHOR]
- Published
- 2009
- Full Text
- View/download PDF