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The effect of interleukin-10 and of interleukin-12 on the in vitro production of anti-double-stranded DNA antibodies from patients with systemic lupus erythematosus

机译:白细胞介素10和白细胞介素12对系统性红斑狼疮患者体外产生抗双链DNA抗体的影响

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摘要

IL-10 and IL-12 are cytokines which are important in regulating immune responses. Plasma levels of IL-10 and autoantibodies against double-stranded DNA (dsDNA) often mirror disease activity in patients with SLE. IL-12 secretion from SLE patients' blood mononuclear cells also correlates with disease activity, but has an inverse relationship. The aim of this study was to measure the effect of IL-10 and of IL-12 on the production of IgG autoantibodies from patients with SLE, both cross-sectionally and longitudinally.Peripheral blood mononuclear cells (PBMC) were cultured with IL-10 (at 20 ng/ml or 2 ng/ml) or IL-12 (at 2 ng/ml or 0·2 ng/ml) or without cytokine and the supernatanants tested for the production of double-stranded DNA antibodies (dsDNA abs), single-stranded DNA antibodies (ssDNA abs) and total IgG antibodies (IgG abs) by ELISA. The BILAG disease activity index was recorded at each patient visit (a global score of six or more is regarded as active disease).In general, treatment with IL-10 caused PBMCs from patients with inactive disease to increase their antissDNA and dsDNA ab production (by upto 354% and 186%, respectively) while patients with active disease decreased their antibody production (by upto 91% and 97%, respectively). Overall there was a correlation between disease activity and change in antissDNA and dsDNA ab production (r = − 0·51; P = 0·03 and r = − 0·48; P = 0·042, respectively). Treatment with IL-12 at 0·2 ng/ml inhibited antissDNA and dsDNA antibody production, having the greatest effect on patients with active disease (decreasing antissDNA and dsDNA antibody production by upto 75% and 73%, respectively). This resulted in a significant correlation between disease activity and change in antissDNA antibody production (r = − 0·76; P = 0·03), but significance was not reached with antidsDNA antibody production (P = 0·06). Together these data suggest that the effect of these cytokines on antibody production by SLE PBMCs involves several factors; one of which is disease activity.
机译:IL-10和IL-12是在调节免疫反应中很重要的细胞因子。 SLE患者的血浆IL-10水平和针对双链DNA(dsDNA)的自身抗体通常反映出疾病活动。 SLE患者血液单核细胞中的IL-12分泌也与疾病活动相关,但具有相反的关系。这项研究的目的是测量IL-10和IL-12对SLE患者横断面和纵向产生IgG自身抗体的影响.IL-10培养外周血单个核细胞(PBMC) (浓度为20 ng / ml或2 ng / ml)或IL-12(浓度为2 ng / ml或0·2 ng / ml)或无细胞因子,并且上清液经测试可产生双链DNA抗体(dsDNA abs) ,ELISA检测单链DNA抗体(ssDNA abs)和总IgG抗体(IgG abs)。每次患者就诊时记录BILAG疾病活动指数(总体得分为6或更高被认为是活动性疾病)。一般而言,用IL-10治疗导致非活动性疾病患者的PBMC增加其抗DNA和dsDNA抗体的产生(活跃疾病患者的抗体产量分别下降了354%和186%)(分别下降了91%和97%)。总体而言,疾病活动性与antissDNA和dsDNA ab产生的变化之间存在相关性(分别为r = − 0·51; P = 0·03和r = − 0·48; P = 0·042)。以0·2 ng / ml的IL-12进行治疗可抑制antissDNA和dsDNA抗体的产生,对活动性疾病患者的影响最大(将antissDNA和dsDNA抗体的产生分别降低75%和73%)。这导致疾病活性和抗ssDNA抗体产生的变化之间具有显着的相关性(r = − 0·76; P = 0·03),但抗dsDNA抗体的产生没有达到显着性(P = 0·06)。这些数据加在一起表明,这些细胞因子对SLE PBMC产生抗体的影响涉及多个因素。其中之一是疾病活动。

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