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由人IgG Fc受体介导的细胞毒性。

Cytotoxicity mediated by human Fc receptors for IgG.

作者信息

Fanger M W, Shen L, Graziano R F, Guyre P M

出版信息

Immunol Today. 1989 Mar;10(3):92-9. doi: 10.1016/0167-5699(89)90234-X.

Abstract

The Fc receptors for IgG(Fc gamma R) play a major role in the removal of antibody-coated infectious agents and may be important molecules for triggering cytotoxicity of tumor cells; they may also serve as an entry for infection of Fc gamma R-bearing cells by viral (including HIV and Dengue), and perhaps other infectious agents. Although central to immune defense, an understanding of the role of these Fc gamma R in cytotoxicity has been complicated in part by the presence of several biochemically distinct types of receptor that have different distributions, specificities, affinities and modes of activation for killing. The development of monoclonal antibodies specific for Fc gamma R on human leukocytes has established the existence of three distinct Fc gamma R and furthermore has helped clarify the function of each of these receptors. In this review, Michael Fanger and colleagues discuss the use of Fc gamma R-specific mAb and the hybridoma cell lines that produce them in examining the ability of each of these unique receptors to mediate killing of tumor and red cell targets. In particular, the use of self-directed hybridoma cells as a model of tumor-cell killing and of bi-specific antibodies to link target cells to effector cells through the different Fc gamma R is discussed. The results of these studies suggest that the ability of a given Fc gamma R to trigger killing is sometimes dependent on the type of Fc gamma R, but is also markedly influenced by the type of target cell and by the nature and state of activation of the effector cell.

摘要

IgG的Fc受体(FcγR)在清除抗体包被的感染因子中起主要作用,可能是触发肿瘤细胞细胞毒性的重要分子;它们也可能是病毒(包括HIV和登革热)以及其他可能的感染因子感染携带FcγR细胞的入口。尽管FcγR对免疫防御至关重要,但由于存在几种生化特性不同、分布、特异性、亲和力及激活杀伤模式各异的受体,对其在细胞毒性中作用的理解变得复杂。针对人白细胞上FcγR的单克隆抗体的研制确定了三种不同的FcγR的存在,而且有助于阐明每种受体的功能。在这篇综述中,迈克尔·范格及其同事讨论了利用针对FcγR的单克隆抗体以及产生这些抗体的杂交瘤细胞系来研究每种独特受体介导杀伤肿瘤细胞和红细胞靶标的能力。特别讨论了利用自身导向的杂交瘤细胞作为肿瘤细胞杀伤模型,以及利用双特异性抗体通过不同的FcγR将靶细胞与效应细胞连接起来的情况。这些研究结果表明,特定FcγR触发杀伤的能力有时取决于FcγR的类型,但也明显受靶细胞类型以及效应细胞激活的性质和状态的影响。

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