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Th1和Th2细胞因子对人单核细胞上刺激性和抑制性Fcγ受体的差异性调节

Differential modulation of stimulatory and inhibitory Fc gamma receptors on human monocytes by Th1 and Th2 cytokines.

作者信息

Pricop L, Redecha P, Teillaud J L, Frey J, Fridman W H, Sautès-Fridman C, Salmon J E

机构信息

Department of Medicine, Hospital for Special Surgery and Weill Medical College of Cornell University, New York, NY 10021, USA.

出版信息

J Immunol. 2001 Jan 1;166(1):531-7. doi: 10.4049/jimmunol.166.1.531.

Abstract

Immune complex-mediated inflammatory responses are initiated by Fc gamma R on phagocytes. We report in this study that an inhibitory receptor, Fc gamma RIIb2, is expressed on circulating human monocytes, and when co-cross-linked with stimulatory Fc gamma R it down-regulates effector function. Fc gamma RIIb2 expression is increased by IL-4 and decreased by IFN-gamma, in contrast to the activating receptor, Fc gamma RIIa, which is increased by IFN-gamma and decreased by IL-4. Thus, Th1 and Th2 cytokines differentially regulate the opposing Fc gamma R systems, altering the balance of activating and inhibiting Fc gamma R. The detection and cytokine modulation of Fc gamma RIIb2 in human myeloid cells provide evidence of a negative regulator of immune complex-mediated responses in human phagocytes and offer a new approach to limit Ab-triggered inflammation in autoimmune disease.

摘要

免疫复合物介导的炎症反应由吞噬细胞上的FcγR启动。我们在本研究中报告,一种抑制性受体FcγRIIb2在循环中的人单核细胞上表达,当与刺激性FcγR共同交联时,它会下调效应功能。与激活受体FcγRIIa相反,FcγRIIb2的表达被IL-4上调而被IFN-γ下调,FcγRIIa被IFN-γ上调而被IL-4下调。因此,Th1和Th2细胞因子以不同方式调节相反的FcγR系统,改变激活和抑制性FcγR的平衡。人髓样细胞中FcγRIIb2的检测和细胞因子调节为人类吞噬细胞中免疫复合物介导反应的负调节因子提供了证据,并为限制自身免疫疾病中抗体触发的炎症提供了新方法。

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