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Activation of Complement Alternative Pathway in Rheumatoid Arthritis: Implications in Peripheral Neutrophils Functions

机译:类风湿关节炎补体旁路的激活:外围中性粒细胞功能的影响。

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Evaluation of the respiratory burst induced by receptors FcγR and CR was carried out in peripheral blood neutrophils (PBN) in rheumatoid arthritis (RA) patients with active and inactive disease. Simultaneously, cooperation between these receptors and their expression, PBN chemotaxis, and complement system systemic activity were also investigated. Neutrophils were stimulated with IC-IgG opsonized with normal human serum (NHS) or not, or with IC-IgG opsonized with RA human serum (RAHS). ROS production was increased in neutrophils of patients with active or inactive RA stimulated of IC-IgG opsonized with NHS compared to the response of the cells mediated by ICIgG. However, there was poor FcγR/CR cooperation in these RA neutrophils, as indicated by decreased ROS production upon stimulation with IC-IgG opsonized with RAHS. In the case of active RA patients, neutrophils presented significantly higher CR1 and CR3 expression, as well as slight elevation in CD32 and CD16 expression. Positive correlations between FcγR and CR, complement alternative pathway activation, and increased RA serum chemotaxic activity were only detected in active RA patients. Taken together, these results indicate that several abnormalities of the complement system exist at the systemic level, namely impaired membrane receptor cooperation, alternative pathway activation, and presence of pre-existing chemoattractant factors in the serum, as reflected by the neutrophil function in the particular case of active RA patients. All, these abnormalities may synergistically contribute to RA pathogenesis.
机译:在患有活动性和非活动性疾病的类风湿关节炎(RA)患者中,评估了受体FcγR和CR诱发的呼吸爆发。同时,还研究了这些受体及其表达,PBN趋化性和补体系统全身活性之间的协同作用。是否用正常人血清(NHS)调理过的IC-IgG或RA人血清(RAHS)调理过的IC-IgG刺激中性粒细胞。与ICIgG介导的细胞反应相比,患有活动性或非活动性RA刺激的用NHS调理的IC-IgG的患者的中性粒细胞中ROS的产生增加。但是,这些RA中性粒细胞的FcγR/ CR协同作用较差,这可以通过用RAHS调理的IC-IgG刺激后产生的ROS减少来表明。对于活跃的RA患者,中性粒细胞的CR1和CR3表达明显升高,CD32和CD16表达略有升高。仅在活跃的RA患者中检测到FcγR和CR,补体旁路途径激活和RA血清趋化活性增加之间存在正相关。综上所述,这些结果表明补体系统的一些异常在全身性水平上存在,即膜受体协作受损,替代途径激活以及血清中存在预先存在的趋化因子,具体由嗜中性白细胞功能反映出来。活跃的RA患者。所有这些异常可能协同促成RA发病机理。

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