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TNF-alpha Inhibitors Decrease Classical CD14(hi)CD16-Monocyte Subsets in Highly Active, Conventional Treatment Refractory Rheumatoid Arthritis and Ankylosing Spondylitis

机译:TNF-α抑制剂在高活性,常规治疗难治性类风湿性关节炎和强直性脊柱炎中降低经典CD14(HI)CD16-单核细胞亚群

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摘要

Monocytes are pivotal cells in inflammatory joint diseases. We aimed to determine the effect of TNF-alpha inhibitors (TNFi) on peripheral blood monocyte subpopulations and their activation in ankylosing spondylitis (AS) and rheumatoid arthritis (RA) patients with high disease activity. To address this, we studied 50 (32 AS, 18 RA) patients with highly active disease with no prior history of TNFi use who were recruited and assigned to TNFi or placebo treatment for 12 weeks. Cytometric and clinical assessment was determined at baseline, four, and 12 weeks after initiation of TNFi treatment. We observed that treatment with TNFi led to a significant decrease in CD14(hi)CD16- monocytes in comparison to placebo, while circulating CD14(dim)CD16+ monocytes significantly increased. The TNFi-induced monocyte subset shifts were similar in RA and AS patients. While the percentage of CD14(dim)CD16+ monocytes increased, expression of CD11b and CD11c integrins on their surface was significantly reduced by TNFi. Additionally, CD45RA+ cells were more frequent. The shift towards nonclassical CD14(dim)CD16+ monocytes in peripheral blood due to TNFi treatment was seen in both AS and RA. This may reflect reduced recruitment of these cells to sites of inflammation due to lower inflammatory burden, which is associated with decreased disease activity.
机译:单核细胞是炎症关节疾病中的枢转细胞。我们的旨在确定TNF-α抑制剂(TNFI)对高疾病活动的脊柱炎(AS)和类风湿性关节炎(RA)患者的外周血单核细胞亚流量及其活化。为了解决这一点,我们研究了50(32 AS,18 ra)患者的高活跃疾病,没有招聘患者的TNFI使用历史,并分配给TNFI或安慰剂治疗12周。在发酵TNFI治疗后,在基线,四个和12周确定细胞仪和临床评估。我们观察到,与安慰剂相比,使用TNFI的处理导致CD14(HI)CD16-单核细胞的显着降低,同时循环CD14(DIM)CD16 +单核细胞显着增加。 TNFI诱导的单核细胞子集移位在RA和患者中相似。虽然CD14(DIM)CD16 +单核细胞的百分比增加,TNFI显着降低了CD11b和CD11c整合蛋白的表达。另外,CD45ra +细胞更频繁。在AS和RA中观察到由于TNFI治疗引起的外周血中的非生效CD14(DIM)CD16 +单核细胞的转变。这可能反映由于炎症负担较低的炎症负担,减少对炎症部位的招募,这与疾病活动降低有关。

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