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用阻断Fc受体功能的单克隆抗体B73.1分析人自然杀伤细胞。II. B73.1抗体与淋巴细胞膜上抗原相互作用的研究。

Human natural killer cells analyzed by B73.1, a monoclonal antibody blocking Fc receptor functions. II. Studies of B73.1 antibody-antigen interaction on the lymphocyte membrane.

作者信息

Perussia B, Acuto O, Terhorst C, Faust J, Lazarus R, Fanning V, Trinchieri G

出版信息

J Immunol. 1983 May;130(5):2142-8.

PMID:6339622
Abstract

In this paper, we characterize the antigen recognized by the monoclonal antibody B73.1 and the modification occurring at the membrane of the positive cells after interaction with the antibody. The B73.1-defined antigen is a protein of 50,000 to 72,000 daltons that is sensitive to pronase but not to trypsin treatment. B73.1 antibody, and its F(ab')2 fragment, directly block, at high concentrations, the binding of IgG antibody-sensitized erythrocytes to the Fc receptors (FcR) of a subpopulation of lymphocytes and neutrophils. B73.1 antibody dissociates rapidly from the positive cells, but concomitant modulation of both B73.1 antigen and FcR is induced when cells are incubated in the continuous presence of antibody or when B73.1 antibody is cross-linked at the cell membrane with an anti-mouse immunoglobulin antiserum. Reaction of lymphocytes with immune complexes also induces modulation of both FcR and B73.1 antigen, without affecting the expression of other antigens on the positive cells. The possibility that the antigen is internalized and digested by the cell after reaction with the antibody is discussed. B73.1 antibody inhibits antibody-dependent cytotoxicity mediated by lymphocytes (K cells) and neutrophils, whereas it does not affect spontaneous cytotoxicity of NK cells. These results suggest the B73.1-defined antigen might be the FcR or a structure closely related to it on K/NK cells.

摘要

在本文中,我们鉴定了单克隆抗体B73.1所识别的抗原,以及阳性细胞与该抗体相互作用后细胞膜上发生的修饰。B73.1所定义的抗原是一种分子量为50,000至72,000道尔顿的蛋白质,对链霉蛋白酶敏感,但对胰蛋白酶处理不敏感。B73.1抗体及其F(ab')2片段在高浓度时可直接阻断IgG抗体致敏的红细胞与淋巴细胞和中性粒细胞亚群的Fc受体(FcR)的结合。B73.1抗体可迅速从阳性细胞上解离,但当细胞在抗体持续存在的情况下孵育,或当B73.1抗体在细胞膜上与抗小鼠免疫球蛋白抗血清交联时,会诱导B73.1抗原和FcR的同时调节。淋巴细胞与免疫复合物的反应也会诱导FcR和B73.1抗原的调节,而不影响阳性细胞上其他抗原的表达。本文还讨论了抗原与抗体反应后被细胞内化和消化的可能性。B73.1抗体可抑制淋巴细胞(K细胞)和中性粒细胞介导的抗体依赖性细胞毒性,而不影响NK细胞的自发细胞毒性。这些结果表明,B73.1所定义的抗原可能是K/NK细胞上的FcR或与其密切相关的结构。

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