首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Cytokine production and surface marker expression in acute and stable multiple sclerosis: altered IL-12 production and augmented signaling lymphocytic activation molecule (SLAM)-expressing lymphocytes in acute multiple sclerosis.
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Cytokine production and surface marker expression in acute and stable multiple sclerosis: altered IL-12 production and augmented signaling lymphocytic activation molecule (SLAM)-expressing lymphocytes in acute multiple sclerosis.

机译:急性和稳定多发性硬化症中细胞因子的产生和表面标志物的表达:急性多发性硬化症中IL-12产生的改变和表达信号的淋巴细胞激活分子(SLAM)的表达增加。

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Ag-stimulated IL-2 production and mitogen-stimulated type 1 and type 2 cytokine production by PBMC, as well as expression of Th1- and Th2-associated phenotypical markers, of B7-1, B7-2, and CD95 (Fas) on the surface of immune cells, and the serum concentration of soluble Apo-1/Fas were evaluated in multiple sclerosis (MS) patients with either acute (AMS) or stable (SMS) disease and in healthy controls (HC). Results showed that 1) Ag-stimulated IL-2 production is reduced in MS patients compared with that in HC; 2) mitogen-stimulated type 1 cytokine production is increased, and IL-10 production is reduced in MS patients compared with those in HC, and in AMS patients compared with those in SMS; 3) whereas production of the metabolically active p70 heterodimers is comparable in SMS, AMS, and HC, production of the p70 heterodimer and the p40 chains (total IL-12) is increased in SMS compared with that in AMS and HC; 4) CD4+, CD4+ SLAM+, and CD4+ CD7+ lymphocytes (preferentially type 1 cytokine-producing lymphocytes) are increased in MS compared with levels in HC; 5) B7-2- as well as Fas+-expressing monocytes are augmented in MS compared with those in HC, and serum soluble Apo-1/Fas is augmented in AMS compared with SMS and HC. These results confirm that a complex imbalance in both cytokine production and the Fas system is present in MS and indicate that different cytokine profiles may be observed in patients with acute or stable disease. The data also suggest that peculiar phenotypic populations are over-represented in MS patients, and for the first time show that SLAM expression is correlated with dysregulation of type 1 and type 2 cytokine production in human pathology.
机译:PBMC对Ag刺激的IL-2产生和有丝分裂原刺激的1型和2型细胞因子产生以及B7-1,B7-2和CD95(Fas)的Th1-和Th2-相关表型标记的表达在患有急性(AMS)或稳定(SMS)疾病的多发性硬化症(MS)患者和健康对照(HC)中,评估免疫细胞表面和可溶性Apo-1 / Fas的血清浓度。结果显示:1)与HC相比,MS患者中Ag刺激的IL-2产生减少; 2)与HC相比,MS患者和AMS患者与SMS患者相比,丝裂原刺激的1型细胞因子产量增加,IL-10产量降低; 3)虽然在SMS,AMS和HC中具有代谢活性的p70异二聚体的产量相当,但与AMS和HC中相比,SMS中p70异二聚体和p40链(总IL-12)的产量增加了; 4)与HC水平相比,MS中的CD4 +,CD4 + SLAM +和CD4 + CD7 +淋巴细胞(优先产生1型细胞因子的淋巴细胞)增加; 5)与HC相比,MS中B7-2-以及Fas +表达单核细胞增加,与SMS和HC相比,AMS中血清可溶性Apo-1 / Fas增加。这些结果证实MS中存在细胞因子产生和Fas系统的复杂失衡,并且表明在患有急性或稳定疾病的患者中可以观察到不同的细胞因子谱。数据还表明,MS患者中独特的表型种群过多,并且首次表明SLAM表达与人类病理学中1型和2型细胞因子生成失调有关。

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