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FcRγ缺陷小鼠效应细胞功能的多重丧失

Multiple loss of effector cell functions in FcR gamma-deficient mice.

作者信息

Takai T

机构信息

Department of Biotechnology, Faculty of Engineering, Okayama University, Japan.

出版信息

Int Rev Immunol. 1996;13(4):369-81. doi: 10.3109/08830189609061759.

DOI:10.3109/08830189609061759
PMID:8884432
Abstract

Immunoglobulin Fc receptor (FcR) gamma subunit is a component of low affinity receptor for IgG, Fc gamma RIII, as well as high affinity receptor for IgE, Fc epsilon RI. This subunit is required for efficient surface expression of these FcRs on various cells in immune system. The FcR gamma-deficient mice, generated by gene targeting in embryonic stem cells, exhibit multiple defects in FcR-mediated effector cell responses, including absence of phagocytic activity against opsonized red blood cells by activated macrophages, loss of antibody-dependent cell-mediated cytotoxicity manifested by IL-2-induced splenic NK cells, and unresponsiveness of mast cells to crosslinking of IgE on these cells. These results demonstrate an indispensable role of FcR gamma for functional expression of FcRs, and clearly indicate the importance of Fc gamma RIII as well as Fc epsilon RI for these effector functions. Since FcR gamma-deficient mice is unable to mount the type II and type III hypersensitivity reactions, it is suggested that FcRs play pivotal roles in initiating these reaction cascades. The mutant mice should prove to be useful in evaluating FcRs in various humoral and cellular immune responses, and in developing new strategies for treatment of immunodeficiency as well as autoimmune disorders.

摘要

免疫球蛋白Fc受体(FcR)γ亚基是IgG低亲和力受体FcγRIII以及IgE高亲和力受体FcεRI的一个组成部分。该亚基是这些FcR在免疫系统各种细胞上高效表面表达所必需的。通过在胚胎干细胞中进行基因打靶产生的FcRγ缺陷小鼠,在FcR介导的效应细胞反应中表现出多种缺陷,包括活化的巨噬细胞对调理的红细胞缺乏吞噬活性、IL-2诱导的脾NK细胞表现出的抗体依赖性细胞介导的细胞毒性丧失,以及肥大细胞对这些细胞上IgE交联无反应。这些结果证明了FcRγ对FcR功能表达的不可或缺的作用,并清楚地表明FcγRIII以及FcεRI对这些效应功能的重要性。由于FcRγ缺陷小鼠无法引发II型和III型超敏反应,提示FcR在启动这些反应级联中起关键作用。这些突变小鼠应被证明在评估各种体液和细胞免疫反应中的FcR以及开发治疗免疫缺陷和自身免疫性疾病的新策略方面是有用的。

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