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The dynamics of mucosal-associated invariant T cells in multiple sclerosis

机译:多发性硬化症中与黏膜相关的恒定T细胞的动力学

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摘要

Background: Multiple sclerosis (MS) is an autoimmune disease characterized by inflammatory demyelination, gliosis and axonal loss in the Central Nervous System. Although the etiology of the disease has remained enigmatic, recent studies have suggested a role of the innate-like T cells, called Mucosal Associated Invariant T cells (MAITs) in the pathophysiology. In the present study, we have analyzed the relative frequency of MAITs and the expression of the cell surface antigens in MAITs to seek a possible link to the disease. Results: There was little difference in the frequency of total MAITs between healthy donors (HDs) and untreated MS patients, whereas the latter harbored more CD8lo/neg (DN) MAITs concomitant with a decrease in CD8high MAITs and in CD4 MAITs compared with those in HDs. While the expression of CCR5, CCR6, CD95, CD127, and CD150 has increased in untreated subjects compared with that in HDs, CD45RO has declined in untreated subjects in both DN MAITs and CD8hi MAITs. FTY720 therapy has increased the relative frequency of total MAITs in a time-dependent fashion up to 2 years. Intriguingly, FTY720 therapy for 3 years reversed the above phenotype, engendering more CD8high MAITs accompanied with decreased DN MAITs. FTY720 therapy affected the cytokine production from CD4 T cells and also enhanced the relative frequency of cells producing both TNF-α and IFN-γ from MAITs, CD8 T cells, and CD4 T cells compared with that in untreated subjects. Conclusions: FTY 720 therapy enhanced the relative frequency of MAITs in MS patients in a time-dependent manner. Although the expression of CD8 in MAITs has been affected early by FTY720, longer treatment has reversed the phenotypic change. These data demonstrated that FTY720 induced dynamic change in the relative frequency and in the phenotype of MAITs in MS.
机译:背景:多发性硬化症(MS)是一种自身免疫性疾病,其特征在于中枢神经系统出现炎症性脱髓鞘,神经胶质增生和轴突丢失。尽管该病的病因学仍然是谜,但最近的研究表明,先天性T细胞在病理生理学中的作用称为粘膜相关不变T细胞(MAITs)。在本研究中,我们分析了MAITs的相对频率以及MAITs中细胞表面抗原的表达,以寻求与该疾病的可能联系。结果:健康供体(HD)和未经治疗的MS患者之间的总MAIT发生频率差异不大,而后者的CD8lo / neg(DN)MAIT则更多,与之相比,CD8high MAIT和CD4 MAIT降低。 HDs。与HDs相比,未经治疗的受试者中CCR5,CCR6,CD95,CD127和CD150的表达增加,而DN MAIT和CD8hi MAIT中未经治疗的受试者中CD45RO的表达均下降。 FTY720治疗以时间依赖性方式增加了总MAIT的相对频率,长达2年。有趣的是,FTY720治疗3年逆转了上述表型,产生了更多的CD8高MAIT,同时伴有DN MAIT降低。与未治疗的受试者相比,FTY720治疗影响了CD4 T细胞的细胞因子产生,并且还提高了从MAIT,CD8 T细胞和CD4 T细胞产生TNF-α和IFN-γ的细胞的相对频率。结论:FTY 720治疗以时间依赖性方式提高了MS患者中MAIT的相对频率。尽管FTY720早期已影响MAITs中CD8的表达,但更长的治疗已逆转了表型变化。这些数据表明FTY720诱导了MS中MAITs的相对频率和表型的动态变化。

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