青少年特发性关节炎患者滑液免疫代谢分析。

Vincent D Giacalone, Alexandre Cammarata-Mouchtouris, Diego Moncada-Giraldo, Sreekala P V Shenoy, Lori A Ponder, Talia R Gergely, Susan O Kim, Joshua D Chandler, Patricia Vega-Fernandez, Cynthia K Manos, Elaine R Flanagan, Sampath Prahalad, Rabindra Tirouvanziam
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摘要

幼年特发性关节炎(JIA)是一种炎症性风湿性疾病。多形态核中性粒细胞(PMNs)存在于JIA滑液(SF)中,但频率可变。JIA中的SF PMN先前显示出高的外泌细胞但低的吞噬和免疫调节活性。为了进一步评估SF中性粒细胞增多症的程度是否与JIA免疫反应的改变有关,我们收集了16名青少年JIA患者的SF和血液。用流式细胞术分析SF和血白细胞。SF和血浆用于免疫介质定量和代谢组学。在SF中培养健康供体血T细胞以评估其免疫调节活性。JIA SF中的PMN和T细胞频率为双峰,描绘了PMN高/T细胞低(PMNHigh)和PMN低/T细胞高(PMNLow)样本。与患者血浆相比,SF的促炎介质增加,PMNHigh SF的促炎症和抗炎介质进一步升高。与血液相比,SF PMNs表现出增加的胞吐和程序性死亡-1/程序性死亡配体-1的表达,SF PMNs和单核细胞/巨噬细胞具有增加的表面结合精氨酸酶-1。SPADE分析显示,SF单核细胞/巨噬细胞亚群共表达程序性死亡-1和程序性死亡配体-1,在PMNHigh SF中表达更高。与PMNLow SF相比,健康供体T细胞在PMNHigh刺激时显示出共受体表达减少。然而,与精氨酸酶-1和IDO-1途径相关的氨基酸代谢产物在两组之间没有差异。因此,在一部分JIA患者的SF中,PMN占优势与免疫介质浓度升高有关,并可能改变SF单核细胞/巨噬细胞表型和T细胞活化,而不改变免疫调节氨基酸。
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Immunometabolic Analysis of Synovial Fluid from Juvenile Idiopathic Arthritis Patients.

Juvenile idiopathic arthritis (JIA) is an inflammatory rheumatic disorder. Polymorphonuclear neutrophils (PMNs) are present in JIA synovial fluid (SF), but with variable frequency. SF PMNs in JIA were previously shown to display high exocytic but low phagocytic and immunoregulatory activities. To further assess whether the degree of SF neutrophilia associated with altered immune responses in JIA, we collected SF and blood from 16 adolescent JIA patients. SF and blood leukocytes were analyzed by flow cytometry. SF and plasma were used for immune mediator quantification and metabolomics. Healthy donor blood T cells were cultured in SF to evaluate its immunoregulatory activities. PMN and T cell frequencies were bimodal in JIA SF, delineating PMN high/T cell low (PMNHigh) and PMN low/T cell high (PMNLow) samples. Proinflammatory mediators were increased in SF compared with plasma across patients, and pro- and anti-inflammatory mediators were further elevated in PMNHigh SF. Compared to blood, SF PMNs showed increased exocytosis and programmed death-1/programmed death ligand-1 expression, and SF PMNs and monocytes/macrophages had increased surface-bound arginase-1. SPADE analysis revealed SF monocyte/macrophage subpopulations coexpressing programmed death-1 and programmed death ligand-1, with higher expression in PMNHigh SF. Healthy donor T cells showed reduced coreceptor expression when stimulated in PMNHigh versus PMNLow SF. However, amino acid metabolites related to the arginase-1 and IDO-1 pathways did not differ between the two groups. Hence, PMN predominance in the SF of a subset of JIA patients is associated with elevated immune mediator concentration and may alter SF monocyte/macrophage phenotype and T cell activation, without altering immunoregulatory amino acids.

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