Department of Rheumatology and Clinical Immunology, University of Groningen, University Medical Center Groningen, Hanzeplein 1, 9713 GZ Groningen, The Netherlands.
Department of Pulmonary Medicine, Erasmus Medical Center, 's-Gravendijkwal 230, 3015 CE Rotterdam, The Netherlands.
J Autoimmun. 2018 Feb;87:16-25. doi: 10.1016/j.jaut.2017.11.003. Epub 2017 Nov 27.
Th17 cells play an important physiological role at mucosal barriers, and are involved in inflammatory responses to pathogens. Th17 cells and their signature cytokine IL-17 are also present in salivary gland lesions of primary Sjögren's syndrome (pSS) patients and can be elevated in their peripheral blood. In pSS patients, clear correlations between increased Th17 cell activity and symptoms of the disease have not been found, but Th17 cells may contribute to disease progression, for example by supporting autoreactive B cell responses. In mouse models of pSS, Th17 cells play an important role in pathogenesis, particularly at disease onset, when there is a disturbed balance between T effector and T regulatory cells. Studying the pathogenicity of Th17 cells in humans is complicated due to the plasticity of this cell subset, allowing them to obtain different effector functions depending on the local environment. Th17 cells can develop towards Th17.1 cells, producing both IL-17 and IFN-γ, or even towards Th1-like cells producing IFN-γ in the absence of IL-17. These effector subsets may be more pathogenic than bona fide Th17 cells. Co-expression of IFN-γ by Th17 cells has been shown to promote chronic inflammation in several autoimmune diseases and may also contribute to pSS pathogenesis. In line with the noticeable role of IL-17 in pSS mouse models, interference with Th17 cell generation, recruitment or effector functions (e.g. IL-17 inhibition) can prevent or ameliorate disease in these models. Therapies targeting Th17 cells or IL-17 have not been tested so far in pSS patients, although treatment with rituximab seems to lower local and systemic IL-17 protein levels, and to a lesser extent also chemokine receptor-defined Th17 cells. In this review we discuss current knowledge of pathogenicity and plasticity of Th17 cells in human pSS and murine models of pSS. We postulate that plasticity towards Th17.1 cells in pSS may enhance pathogenicity of Th17 cells at the main target sites of the disease, i.e. salivary and lacrimal glands.
Th17 细胞在黏膜屏障中发挥重要的生理作用,并参与对病原体的炎症反应。Th17 细胞及其特征性细胞因子 IL-17 也存在于原发性干燥综合征 (pSS) 患者的唾液腺病变中,并可在外周血中升高。在 pSS 患者中,尚未发现 Th17 细胞活性增加与疾病症状之间有明确的相关性,但 Th17 细胞可能会促进疾病进展,例如通过支持自身反应性 B 细胞反应。在 pSS 的小鼠模型中,Th17 细胞在发病机制中发挥重要作用,尤其是在疾病发病时,此时 T 效应细胞和 T 调节细胞之间的平衡被打乱。由于该细胞亚群的可塑性,研究 Th17 细胞在人类中的致病性较为复杂,使其能够根据局部环境获得不同的效应功能。Th17 细胞可向 Th17.1 细胞分化,产生 IL-17 和 IFN-γ,甚至在没有 IL-17 的情况下向产生 IFN-γ的 Th1 样细胞分化。这些效应亚群可能比真正的 Th17 细胞更具致病性。在几种自身免疫性疾病中,Th17 细胞共表达 IFN-γ可促进慢性炎症,并且可能也有助于 pSS 的发病机制。与 IL-17 在 pSS 小鼠模型中的显著作用一致,干扰 Th17 细胞的产生、募集或效应功能(例如,IL-17 抑制)可预防或改善这些模型中的疾病。迄今为止,尚未在 pSS 患者中测试针对 Th17 细胞或 IL-17 的治疗方法,尽管利妥昔单抗治疗似乎降低了局部和全身的 IL-17 蛋白水平,并且在较小程度上也降低了趋化因子受体定义的 Th17 细胞水平。在这篇综述中,我们讨论了 Th17 细胞在人类 pSS 和 pSS 小鼠模型中的致病性和可塑性的现有知识。我们假设,在 pSS 中向 Th17.1 细胞的可塑性可能会增强疾病主要靶位(即唾液腺和泪腺)中 Th17 细胞的致病性。
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