TNF-alpha induction of GM2 expression on renal cell carcinomas promotes T cell dysfunction
Date
2007-05-15Author
Raval, Gira
Biswas, Soumika
Rayman, Patricia
Biswas, Kaushik
Sa, Gaurisankar
Ghosh, Sankar
Thornton, Mark
Hilston, Cynthia
Das, Tanya
Bukowski, Ronald
Finke, James H.
Tannenbaum, Charles S.
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Previous studies from our laboratory demonstrated the role of tumor-derived gangliosides as important mediators of T cell apoptosis, and hence, as one mechanism by which tumors evade immune destruction. In this study, we report that TNF-alpha secreted by infiltrating inflammatory cells and/or genetically modified tumors augments tumor-associated GM2 levels, which leads to T cell death and immune dysfunction. The conversion of weakly apoptogenic renal cell carcinoma (RCC) clones to lines that can induce T cell death requires 3-5 days of TNF-alpha pretreatment, a time frame paralleling that needed for TNF-alpha to stimulate GM2 accumulation by SK-RC-45, SK-RC-54, and. SK-RC-13. RCC tumor cell lines permanently transfected with the TNF-alpha transgene are similarly toxic for T lymphocytes, which correlates with their constitutively elevated levels of GM2. TNF-alpha increases GM2 ganglioside expression by enhancing the mRNA levels encoding its synthetic enzyme, GM2 synthase, as demonstrated by both RT-PCR and Southern analysis. The contribution of GM2 gangliosides to tumor-induced T cell death was supported by the finding that anti-GM2 Abs significantly blocked T cell apoptosis mediated by TNF-alpha-treated tumor cells, and by the observation that small interfering RNA directed against TNF-alpha abrogated GM2 synthase expression by TNF-transfected SK-RC-45, diminished its GM2 accumulation, and inhibited its apoptogenicity for T lymphocytes. Our results indicate that TNF-alpha signaling promotes RCCinduced killing of T cells by stimulating the acquisition of a distinct ganglioside assembly in RCC tumor cells. The Journal of Immunology, 2007, 178: 6642-6652.
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1. Full Text Link ->http://www.jimmunol.org/content/178/10/6642.full.pdf+html
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- Gaurisankar Sa [19]
