Immune-checkpoint protein VISTA critically regulates the IL-23/IL-17 inflammatory axis

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作者
Na Li
Wenwen Xu
Ying Yuan
Natarajan Ayithan
Yasutomo Imai
Xuesong Wu
Halli Miller
Michael Olson
Yunfeng Feng
Yina H. Huang
Mary Jo Turk
Samuel T. Hwang
Subramaniam Malarkannan
Li Wang
机构
[1] Department of Microbiology and Immunology,Institute of Human Virology
[2] Department of Dermatology,Department of Dermatology
[3] Medical College of Wisconsin,Department of Histology and Embryology
[4] Department of Medicine,undefined
[5] Medical College of Wisconsin,undefined
[6] Department of Pediatrics,undefined
[7] Medical College of Wisconsin,undefined
[8] Department of Blood Research Institute,undefined
[9] Department of Microbiology and Immunology,undefined
[10] Geisel School of Medicine at Dartmouth,undefined
[11] Shanghai University of Traditional Chinese Medicine,undefined
[12] College of Pharmacy,undefined
[13] University of Maryland School of Medicine,undefined
[14] Department of Dermatology,undefined
[15] University of California Davis,undefined
[16] Harbin Medical University,undefined
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摘要
V-domain Immunoglobulin Suppressor of T cell Activation (VISTA) is an inhibitory immune-checkpoint molecule that suppresses CD4+ and CD8+ T cell activation when expressed on antigen-presenting cells. Vsir−/− mice developed loss of peripheral tolerance and multi-organ chronic inflammatory phenotypes. Vsir−/− CD4+ and CD8+ T cells were hyper-responsive towards self- and foreign antigens. Whether or not VISTA regulates innate immunity is unknown. Using a murine model of psoriasis induced by TLR7 agonist imiquimod (IMQ), we show that VISTA deficiency exacerbated psoriasiform inflammation. Enhanced TLR7 signaling in Vsir−/− dendritic cells (DCs) led to the hyper-activation of Erk1/2 and Jnk1/2, and augmented the production of IL-23. IL-23, in turn, promoted the expression of IL-17A in both TCRγδ+ T cells and CD4+ Th17 cells. Furthermore, VISTA regulates the peripheral homeostasis of CD27− γδ T cells and their activation upon TCR-mediated or cytokine-mediated stimulation. IL-17A-producing CD27− γδ T cells were expanded in the Vsir−/− mice and amplified the inflammatory cascade. In conclusion, this study has demonstrated that VISTA critically regulates the inflammatory responses mediated by DCs and IL-17-producing TCRγδ+ and CD4+ Th17 T cells following TLR7 stimulation. Our finding provides a rationale for therapeutically enhancing VISTA-mediated pathways to benefit the treatment of autoimmune and inflammatory disorders.
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