Abstract

The immunosurveillance of transformed cells by the immune system remains one of the most controversial and poorly understood areas of immunity. Gene-targeted mice have greatly aided our understanding of the key effector molecules in tumor immunity. Herein, we describe spontaneous tumor development in gene-targeted mice lacking interferon (IFN)-γ and/or perforin (pfp), or the immunoregulatory cytokines, interleukin (IL)-12, IL-18, and tumor necrosis factor (TNF). Both IFN-γ and pfp were critical for suppression of lymphomagenesis, however the level of protection afforded by IFN-γ was strain specific. Lymphomas arising in IFN-γ-deficient mice were very nonimmunogenic compared with those derived from pfp-deficient mice, suggesting a comparatively weaker immunoselection pressure by IFN-γ. Single loss of IL-12, IL-18, or TNF was not sufficient for spontaneous tumor development. A significant incidence of late onset adenocarcinoma observed in both IFN-γ– and pfp-deficient mice indicated that some epithelial tissues were also subject to immunosurveillance.

Keywords

ImmunosurveillancePerforinInterferon gammaTumor necrosis factor alphaBiologyImmune systemImmunologyCytokineInterferonLymphomaCancer researchImmunityCD8

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2004 Clinical and Vaccine Immunology 52 citations

Publication Info

Year
2002
Type
article
Volume
196
Issue
1
Pages
129-134
Citations
367
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Shayna E.A. Street, Joseph A. Trapani, Duncan MacGregor et al. (2002). Suppression of Lymphoma and Epithelial Malignancies Effected by Interferon γ. The Journal of Experimental Medicine , 196 (1) , 129-134. https://doi.org/10.1084/jem.20020063

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DOI
10.1084/jem.20020063