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CD4+CD25+/highCD127low/- regulatory T cells are enriched in rheumatoid arthritis and osteoarthritis joints-analysis of frequency and phenotype in synovial membrane, synovial fluid and peripheral blood

机译:CD4 + CD25 + / highCD127low /-调节性T细胞富含类风湿关节炎和骨关节炎关节-滑膜,滑液和外周血的频率和表型分析

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Introduction: CD4+CD25+/highCD127low/- regulatory T cells (Tregs) play a crucial role in maintaining peripheral tolerance. Data about the frequency of Tregs in rheumatoid arthritis (RA) are contradictory and based on the analysis of peripheral blood (PB) and synovial fluid (SF). Because Tregs exert their anti-inflammatory activity in a contact-dependent manner, the analysis of synovial membrane (SM) is crucial. Published reports regarding this matter are lacking, so we investigated the distribution and phenotype of Tregs in concurrent samples of SM, SF and PB of RA patients in comparison to those of osteoarthritis (OA) patients.Methods: Treg frequency in a total of 40 patients (18 RA and 22 OA) matched for age and sex was assessed by flow cytometry. Functional status was assessed by analysis of cell surface markers representative of activation, memory and regulation.Results: CD4+ T cells infiltrate the SM to higher frequencies in RA joints than in OA joints (P = 0.0336). In both groups, Tregs accumulate more within the SF and SM than concurrently in PB (P 0.0001). Relative Treg frequencies were comparable in all compartments of RA and OA, but Treg concentration was significantly higher in the SM of RA patients (P = 0.025). Both PB and SM Tregs displayed a memory phenotype (CD45RO+RA-), but significantly differed in activation status (CD69 and CD62L) and markers associated with Treg function (CD152, CD154, CD274, CD279 and GITR) with only minor differences between RA and OA.Conclusions: Treg enrichment into the joint compartment is not specific to inflammatory arthritis, as we found that it was similarly enriched in OA. RA pathophysiology might not be due to a Treg deficiency, because Treg concentration in SM was significantly higher in RA. Synovial Tregs represent a distinct phenotype and are activated effector memory cells (CD62L-CD69+), whereas peripheral Tregs are resting central memory cells (CD62L+CD69-).
机译:简介:CD4 + CD25 + /高CD127低/-调节性T细胞(Tregs)在维持外周耐受中起着至关重要的作用。关于类风湿关节炎(RA)中Treg频率的数据是矛盾的,并且基于对外周血(PB)和滑液(SF)的分析。由于Tregs以接触依赖的方式发挥其抗炎活性,因此滑膜(SM)的分析至关重要。缺乏有关此问题的公开报道,因此我们比较了RA患者与骨关节炎(OA)患者的SM,SF和PB同时样本中Treg的分布和表型。方法:共40例患者的Treg频率通过流式细胞术评估年龄和性别匹配的患者(18 RA和22 OA)。通过分析代表激活,记忆和调节的细胞表面标志物来评估功能状态。结果:CD4 + T细胞在RA关节中的渗透率高于OA关节(P = 0.0336)。在两个组中,Tregs在SF和SM中的积累均高于同时在PB中的积累(P <0.0001)。在RA和OA的所有区室中,相对Treg频率均相当,但RA患者的SM中Treg浓度显着较高(P = 0.025)。 PB和SM Tregs均表现出记忆表型(CD45RO + RA-),但激活状态(CD69和CD62L)和与Treg功能相关的标志物(CD152,CD154,CD274,CD279和GITR)显着不同,RA之间仅有微小差异结论:Treg在关节腔内的富集不是炎性关节炎特有的,因为我们发现它在OA中也富集。 RA病理生理可能不是由于Treg缺乏引起的,因为SM中Treg的浓度明显高于RA。滑膜Treg代表不同的表型,并且是激活的效应记忆细胞(CD62L-CD69 +),而外周Treg是静止的中央记忆细胞(CD62L + CD69-)。

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