MIF inhibition alleviates vitiligo progression by suppressing CD8+ T cell activation and proliferation
Jianru Chen, Weinan Guo, Pengran Du, Tingting Cui, Yuqi Yang, Yinghan Wang, Pan Kang, Zhe Zhang, Qi Wang, Zhubiao Ye, Ling Liu, Zhe Jian, Tianwen Gao, Huijie Bian, Shuli Li, Chunying Li
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Abstract
In vitiligo, autoreactive CD8+ T cells have been established as the main culprit considering its pathogenic role in mediating epidermal melanocyte-specific destruction. Macrophage migration inhibitory factor (MIF) is a pleiotropic molecule that plays a central role in various immune processes including the activation and proliferation of T cells; but whether MIF is intertwined in vitiligo development and progression and its involvement in aberrantly activated CD8+ T cells remains ill-defined. In this study, we found that MIF was overabundant in vitiligo patients and a mouse model for human vitiligo. Additionally, inhibiting MIF ameliorated the disease progression in vitiligo mice, which manifested as less infiltration of CD8+ T cells and more retention of epidermal melanocytes in the tail skin. More importantly, in vitro experiments indicated that MIF-inhibition suppressed the activation and proliferation of CD8+ T cells from the lymph nodes of vitiligo mice, and the effect extended to CD8+ T cells in peripheral blood mononuclear cells of vitiligo patients. Finally, CD8+ T cells derived from MIF-inhibited vitiligo mice also exhibited an impaired capacity for activation and proliferation. Taken together, our results show that MIF might be clinically targetable in vitiligo treatment, and its inhibition might ameliorate vitiligo progression by suppressing autoreactive CD8+ T cell activation and proliferation. © 2023 The Pathological Society of Great Britain and Ireland.
MIF抑制通过抑制CD8+ T细胞的活化和增殖来缓解白癜风的进展
在白癜风中,考虑到自身反应性CD8+ T细胞介导表皮黑色素细胞特异性破坏的致病作用,已确定其为罪魁祸首。巨噬细胞迁移抑制因子(Macrophage migration inhibitory factor, MIF)是一种多用途分子,在多种免疫过程中发挥核心作用,包括T细胞的激活和增殖;但MIF是否与白癜风的发展和进展以及它是否参与异常活化的CD8+ T细胞仍不清楚。在本研究中,我们发现MIF在白癜风患者和人类白癜风小鼠模型中过量存在。此外,抑制MIF可改善白癜风小鼠的疾病进展,表现为CD8+ T细胞浸润减少,尾皮表皮黑色素细胞滞留更多。更重要的是,体外实验表明,mif抑制抑制白癜风小鼠淋巴结CD8+ T细胞的活化和增殖,并扩展到白癜风患者外周血单个核细胞中的CD8+ T细胞。最后,来自mif抑制白癜风小鼠的CD8+ T细胞也表现出活化和增殖能力受损。综上所述,我们的研究结果表明MIF可能是白癜风治疗的临床靶标,其抑制可能通过抑制自身反应性CD8+ T细胞的活化和增殖来改善白癜风的进展。©2023英国和爱尔兰病理学会。
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