Murine interleukin-12 prevents the development of cancer cachexia in a murine model
Corresponding Author
Kazushige Mori
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Department of Oncology, Nippon Roche Research Center, 200 Kajiwara, Kamakura City 247, Japan. Fax: 81 467 45 6782Search for more papers by this authorKaori Fujimoto-Ouchi
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorTohru Ishikawa
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorFumiko Sekiguchi
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorHideo Ishitsuka
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorYutaka Tanaka
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorCorresponding Author
Kazushige Mori
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Department of Oncology, Nippon Roche Research Center, 200 Kajiwara, Kamakura City 247, Japan. Fax: 81 467 45 6782Search for more papers by this authorKaori Fujimoto-Ouchi
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorTohru Ishikawa
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorFumiko Sekiguchi
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorHideo Ishitsuka
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorYutaka Tanaka
Department of Oncology, Nippon Roche Research Center, Kamakura City, Japan
Search for more papers by this authorAbstract
Murine colon 26 carcinoma causes cachexia even when the tumor burden is small. In this tumor model, murine IL-12 suppressed the induction of cancer cachexia and also inhibited tumor growth. IL-12 reduced the serum levels of IL-6, a cachexia mediator in this model, and alleviated the body weight loss and other abnormalities associated with cachexia, such as adipose tissue wasting and hypoglycemia. The anticachectic activity was observed even at low doses of IL-12, insufficient to inhibit tumor growth. IL-12 greatly increased levels of IFN-γ in the tumor tissue and, to a lesser extent, in the circulation. IFN-γ given intraperitoneally also prevented cancer cachexia, although it did not reduce IL-6 levels either in the tumor or in the circulation. In athymic mice bearing the same colon 26 tumor, IL-12 was no longer anticachectic and did not induce IFN-γ. These results indicate that the anticachectic activity of IL-12 is T-cell-dependent and results from at least 2 mechanisms, the down-regulation of IL-6 and the up-regulation of IFN-γ. © 1996 Wiley-Liss, Inc.
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