Curcumin reverses T cell-mediated adaptive immune dysfunctions in tumor-bearing hosts

被引:0
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作者
Sankar Bhattacharyya
Dewan Md Sakib Hossain
Suchismita Mohanty
Gouri Sankar Sen
Sreya Chattopadhyay
Shuvomoy Banerjee
Juni Chakraborty
Kaushik Das
Diptendra Sarkar
Tanya Das
Gaurisankar Sa
机构
[1] Bose Institute,Division of Molecular Medicine
来源
Cellular & Molecular Immunology | 2010年 / 7卷
关键词
CD4; /CD8; T cell; Effector T cell; T-regulatory cell; FoxP3; Th1/Th2;
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摘要
Immune dysfunction is well documented during tumor progression and likely contributes to tumor immune evasion. CD8+ cytotoxic T lymphocytes (CTLs) are involved in antigen-specific tumor destruction and CD4+ T cells are essential for helping this CD8+ T cell-dependent tumor eradication. Tumors often target and inhibit T-cell function to escape from immune surveillance. This dysfunction includes loss of effector and memory T cells, bias towards type 2 cytokines and expansion of T regulatory (Treg) cells. Curcumin has previously been shown to have antitumor activity and some research has addressed the immunoprotective potential of this plant-derived polyphenol in tumor-bearing hosts. Here we examined the role of curcumin in the prevention of tumor-induced dysfunction of T cell-based immune responses. We observed severe loss of both effector and memory T-cell populations, downregulation of type 1 and upregulation of type 2 immune responses and decreased proliferation of effector T cells in the presence of tumors. Curcumin, in turn, prevented this loss of T cells, expanded central memory T cell (TCM)/effector memory T cell (TEM) populations, reversed the type 2 immune bias and attenuated the tumor-induced inhibition of T-cell proliferation in tumor-bearing hosts. Further investigation revealed that tumor burden upregulated Treg cell populations and stimulated the production of the immunosuppressive cytokines transforming growth factor (TGF)-β and IL-10 in these cells. Curcumin, however, inhibited the suppressive activity of Treg cells by downregulating the production of TGF-β and IL-10 in these cells. More importantly, curcumin treatment enhanced the ability of effector T cells to kill cancer cells. Overall, our observations suggest that the unique properties of curcumin may be exploited for successful attenuation of tumor-induced suppression of cell-mediated immune responses.
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页码:306 / 315
页数:9
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