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糖皮质激素增强γ干扰素对人单核细胞抗原表达及抗体依赖的细胞介导的细胞毒作用的影响。

Glucocorticoid enhances gamma interferon effects on human monocyte antigen expression and ADCC.

作者信息

Shen L, Guyre P M, Ball E D, Fanger M W

出版信息

Clin Exp Immunol. 1986 Aug;65(2):387-95.

Abstract

The expression of HLA-DR antigen by highly enriched human monocytes cultured in serum free medium was found to be markedly elevated by human recombinant gamma interferon (IFN-gamma). This effect was maximal after 48 h in culture with 300 mu/ml IFN-gamma. Class I MHC antigen also increased with IFN-gamma treatment. By contrast, binding of a myeloid-specific monoclonal antibody, AML-2-23, was dramatically decreased by IFN-gamma. The augmentation of MHC antigens was not ablated by an immunosuppressive concentration (2 X 10(-7) M) of the glucocorticoid dexamethasone (DEX). In fact, both the enhancement of Class I and Class II MHC antigen expression and the suppression of AML-2-23 antigen by IFN-gamma were often more profound in the presence of DEX. IFN-gamma treatment also resulted in elevated monocyte effector function, as measured by antibody dependent cellular cytotoxicity (ADCC). This functional activation was not inhibited by DEX. On the contrary, DEX slightly augmented IFN-gamma effects on ADCC. This contrasts with other reports that glucocorticoids inhibit monocyte responsiveness to lymphokines, and suggests that the interplay between lymphokines and the glucocorticoid hormones may be more complex than previously thought.

摘要

在无血清培养基中培养的高度纯化的人单核细胞,其HLA - DR抗原的表达被发现可被人重组γ干扰素(IFN - γ)显著提高。在用300μ/ml IFN - γ培养48小时后,这种效应达到最大。I类MHC抗原也随着IFN - γ处理而增加。相比之下,一种髓系特异性单克隆抗体AML - 2 - 23的结合被IFN - γ显著降低。糖皮质激素地塞米松(DEX)的免疫抑制浓度(2×10⁻⁷M)并未消除MHC抗原的增加。事实上,在DEX存在的情况下,IFN - γ对I类和II类MHC抗原表达的增强以及对AML - 2 - 23抗原的抑制往往更显著。通过抗体依赖性细胞毒性(ADCC)测量,IFN - γ处理还导致单核细胞效应功能增强。这种功能激活未被DEX抑制。相反,DEX略微增强了IFN - γ对ADCC的作用。这与其他关于糖皮质激素抑制单核细胞对淋巴因子反应性的报道形成对比,表明淋巴因子与糖皮质激素之间的相互作用可能比以前认为的更为复杂。

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本文引用的文献

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