GM2 expression in renal cell carcinoma: Potential role in tumor-induced T-cell dysfunction

被引:65
作者
Biswas, Kaushik
Richmond, Amy
Rayman, Patricia
Biswas, Soumika
Thornton, Mark
Sa, Gaurisankar
Das, Tanya
Zhang, Renliang
Chahlavi, Ali
Tannenbaum, Charles S.
Novick, Andrew
Bukowski, Ronald
Finke, James H.
机构
[1] Cleveland Clin Fdn, Lerner Res Inst, Dept Immunol, Cleveland, OH 44195 USA
[2] Cleveland Clin Fdn, Lerner Res Inst, Mass Spectrometry Core, Cleveland, OH 44195 USA
[3] Cleveland Clin Fdn, Dept Neurosurg, Cleveland, OH 44195 USA
[4] Cleveland Clin Fdn, Glickman Urol Inst, Cleveland, OH 44195 USA
[5] Bose Inst, Kolkata 700009, W Bengal, India
关键词
D O I
10.1158/0008-5472.CAN-06-0250
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Multiple mechanisms have been proposed to account for immune escape by tumors. Although gangliosides have long been known to suppress T-cell immunity, few studies have examined the effect of human tumor-derived gangliosides on immune responses. Here, we show that gangliosides isolated from renal cell carcinoma (RCC) cell lines and clear cell tumor tissue can induce apoptosis in peripheral blood T cells. The RCC tissue-derived gangliosides also suppressed IFN-gamma and, in many cases, interleukin-4 production by CD4(+) T cells at concentrations (1 ng/mL-100 pg/mL) well below those that induce any detectable T-cell death (4-20 mu g/mL). Additional findings show that GM2 expressed by RCC plays a significant role in promoting T-cell dysfunction. This is supported by the demonstration that all RCC cell lines examined (n = 5) expressed GM2 as did the majority of tumors (15 of 18) derived from patients with clear cell RCC. Furthermore, an antibody specific for GM2 (DMF10.167.4) partially blocked (50-60%) T-cell apoptosis induced by coculturing lymphocytes with RCC cell lines or with RCC tissue-derived gangliosides. DMF10. 167.4 also partially blocked the suppression of IFN-gamma production induced by RCC tissue-derived gangliosides, suggesting that GM2 plays a role in down-regulating cytokine production by CD4(+) T cells.
引用
收藏
页码:6816 / 6825
页数:10
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