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皮质类固醇对人单核细胞免疫球蛋白G及补体受体的作用。

Effect of corticosteroids on the human monocyte IgG and complement receptors.

作者信息

Schreiber A D, Parsons J, McDermott P, Cooper R A

出版信息

J Clin Invest. 1975 Nov;56(5):1189-97. doi: 10.1172/JCI108196.

Abstract

A quantitative in vitro assay was employed to directly assess the effect of corticosteroids on the IgG and complement receptor function of human mononuclear phagocytic cells. In this system corticosteroids were solubilized with cholesterol-phospholipid sonicated dispersions before exposure to mononuclear cells. Solubilized corticosteroids at concentrations between 10(-4) and 10(-3) M inhibited both IgG and complement receptor activity in a dose-response fashion. Inhibition was dependent upon the time of interaction of the mononuclear cells with corticosteroids and was half-maximal by 15 min. The inhibitory effect at all concentrations of hydrocortisone was partially overcome by increasing the number of IgG molecules per erythrocyte. Hydrocortisone also inhibited the binding of erythrocytes coated with both IgG and C3, despite the fact that when both were on the erythrocyte surface a synergistic effect on binding to mononuclear cells was observed. At the steroid concentrations employed, the capacity of mononuclear cells to exclude trypan blue and to take up latex particles and neutral red was unaffected. Mineralocorticoids also inhibited receptor activity, but the sex hormones were less effective. These studies demonstrate an effect of steroid hormones on cell membrane receptor function, and they suggest that an inhibition of the recognition system for IgG and C3 in vivo may explain, in part, the effect of corticosteroids in man.

摘要

采用定量体外试验直接评估皮质类固醇对人单核吞噬细胞IgG和补体受体功能的影响。在该系统中,皮质类固醇在暴露于单核细胞之前先用胆固醇-磷脂超声分散体溶解。浓度在10^(-4)至10^(-3) M之间的溶解皮质类固醇以剂量反应方式抑制IgG和补体受体活性。抑制作用取决于单核细胞与皮质类固醇的相互作用时间,15分钟时达到半数最大抑制。通过增加每个红细胞上IgG分子的数量,可部分克服所有浓度氢化可的松的抑制作用。尽管当IgG和C3都在红细胞表面时观察到对与单核细胞结合有协同作用,但氢化可的松也抑制了同时包被有IgG和C3的红细胞的结合。在所采用的类固醇浓度下,单核细胞排除台盼蓝、摄取乳胶颗粒和中性红的能力未受影响。盐皮质激素也抑制受体活性,但性激素的作用较小。这些研究证明了类固醇激素对细胞膜受体功能的影响,并表明体内对IgG和C3识别系统的抑制可能部分解释了皮质类固醇在人体中的作用。

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