Induction of antitumor effect on human esophageal carcinoma cells by the retroviral expression of granulocyte macrophage-colony stimulating factor gene.

Sugaya,M; Tagawa,M; Matsubara,H; Gunji,Y; Takenaga,K; Maeda,T; Koide,Y; Asano,T; Ochiai,T; Isono,K; Sakiyama,S

doi:10.3892/ijo.12.2.321

Induction of antitumor effect on human esophageal carcinoma cells by the retroviral expression of granulocyte macrophage-colony stimulating factor gene.

Authors:
- M Sugaya
- M Tagawa
- H Matsubara
- Y Gunji
- K Takenaga
- T Maeda
- Y Koide
- T Asano
- T Ochiai
- K Isono
- S Sakiyama
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Affiliations: Department of Surgery (II), School of Medicine, Chiba University, 1-8-1 Inohana, Chuo-ku, Chiba 260, Japan.
Published online on: February 1, 1998 https://doi.org/10.3892/ijo.12.2.321
Pages: 321-325

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Abstract

We have examined antitumor effect of human esophageal carcinoma cells (T.Tn) which were retrovirally transduced to express mouse granulocyte macrophage-colony stimulating factor (mGM-CSF) gene. Nude mice inoculated with T.Tn cells secreting mGM-CSF developed small tumors but the tumors regressed spontaneously, although the proliferation in vitro of transduced cells was not different from that of wild-type cells. In contrast, the tumor of T.Tn cells transduced with human GM-CSF grew as that of wild-type cells, since murine GM-CSF receptors do not bind to human GM-CSF. Histological examination of the regressing tumor of mGM-CSF-producing T.Tn cells revealed predominant infiltration of inflammatory cells including macrophages. In addition, local injection of mGM-CSF-producing T.Tn cells into the established wild-type tumors significantly induced the retardation of subsequent wild-type tumor growth, suggesting that T-cell independent local response plays a crucial role in destroying tumor cells.