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Interleukin-12 genetic administration suppressed metastatic liver tumor unsusceptible to CTL
Authors:Itokawa Yoshiki  Mazda Osam  Ueda Yuji  Kishida Tsunao  Asada Hidetsugu  Cui Feng De  Fuji Nobuaki  Fujiwara Hitoshi  Shin-Ya Masaharu  Yasutomi Kakei  Imanishi Jiro  Yamagishi Hisakazu
Affiliation:Department of Digestive Surgery, Kyoto Prefectural University of Medicine, 602-8566, Kyoto, Japan.
Abstract:A cytokine gene therapy approach was conducted against metastatic lesions of cytotoxic T lymphocyte (CTL)-unsusceptible tumor in mice. The EBV-based and conventional plasmid vectors that encode murine interleukin-12 (IL-12) gene (pGEG.mIL-12 and pG.mIL-12, respectively) were intravenously transfected into the mice that had received a subcutaneous inoculation of M5076 sarcoma cells. The pGEG.mIL-12 transfection drastically suppressed the subcutaneous as well as hepatic metastatic tumors, resulting in significant prolongation of survival period of the animals. Although single administration with pG.mIL-12 was not effective, repetitive transfection with the plasmid significantly prolonged the longevity of the mice-bearing the metastatic liver tumors. Multiple transfection with either pGEG.mIL-12 or pG.mIL-12 also suppressed peritoneal carcinomatosis in mice that had been injected with M5076 cells into the peritoneal cavity. It was suggested that a high level IL-12 production elicited by the intravenous delivery of the cytokine gene may be quite effective in inhibiting metastatic and CTL-unsusceptible neoplasms.
Keywords:Interleukin-12   Tumor   Liver metastasis   Peritoneal carcinomatosis   Cytotoxic T lymphocytes   Epstein-Barr virus-based plasmid vector   Hydrodynamics-based transfection   Gene therapy
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