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T-cell activation occurs simultaneously in local and peripheral lymphoid tissue following oral administration of a range of doses of immunogenic or tolerogenic antigen although tolerized T cells display a defect in cell division

机译:口服一定剂量的免疫原性或耐受性抗原后,T细胞活化同时在局部和周围淋巴组织中发生,尽管耐受性T细胞在细胞分裂中表现出缺陷

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摘要

How the mucosal immune system promotes active immunity against harmful organisms but tolerance to commensal bacteria or dietary antigens is poorly understood. Thus, the antigen-presenting cell (APC), site of antigen presentation, and effector mechanisms responsible for oral priming and tolerance remain unclear. Characterizing differences between oral priming and tolerance may improve the exploitation of oral tolerance for therapeutic applications and aid the design of oral vaccines. To address these questions we compared the mucosal and systemic activation and localization of antigen-specific T cells during the induction of oral priming and tolerance. Activation marker expression and cell division by tg T cells was determined in conjunction with their anatomical location. These studies show that after feeding, T cells are activated in both peripheral and local lymphoid tissues within 6 hr, irrespective of the presence of adjuvant. Subsequently, T-cell accumulation can be detected simultaneously in peripheral and mesenteric lymph nodes and Peyer's patches within 24 hr of feeding, but only after 3 days post feeding in the lamina propria. Primed and tolerized T cells adopted similar phenotypes as assessed by activation marker expression. However, within the mesenteric lymph nodes (MLN) tolerized T cells underwent significantly fewer divisions than primed T cells. Thus, T-cell activation and expansion occurs throughout the animal after feeding a range of doses of antigen, irrespective of whether priming or tolerance is the eventual outcome. However, the presence of an adjuvant enhances clonal expansion in the MLN while tolerized T cells display defective cell division.
机译:粘膜免疫系统如何促进对有害生物的主动免疫,但对共生细菌或饮食抗原的耐受性却知之甚少。因此,尚不清楚抗原呈递细胞(APC),抗原呈递位点以及负责口服引发和耐受的效应子机制。表征口服引发和耐受性之间的差异可能会改善对治疗应用的口服耐受性,并有助于口服疫苗的设计。为了解决这些问题,我们比较了口服引发和耐受期间抗原特异性T细胞的黏膜和全身激活及定位。结合它们的解剖位置确定激活标记的表达和tg T细胞的细胞分裂。这些研究表明,进食后,无论是否存在佐剂,T细胞均会在6小时内在外周和局部淋巴组织中被激活。随后,可以在进食后24小时内同时在外周和肠系膜淋巴结和Peyer斑中同时检测到T细胞蓄积,但仅在进食后固有层中的3天后才能检测到。经激活标记表达评估,初免和耐受的T细胞采用相似的表型。然而,在肠系膜淋巴结(MLN)内,耐受的T细胞的分裂明显少于引发的T细胞。因此,在喂食一定剂量的抗原后,无论最终的结果是引发还是耐受,T细胞的活化和扩增都会在整个动物中发生。但是,佐剂的存在会增强MLN中的克隆扩增,而耐受的T细胞则显示出细胞分裂缺陷。

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