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特定系统中抗体介导的细胞毒性:受抗原、抗体和补体的调节。

Antibody-mediated cell cytotoxicity in a defined system: regulation by antigen, antibody, and complement.

作者信息

Lustig H J, Bianco C

出版信息

J Immunol. 1976 Jan;116(1):253-60.

PMID:1245741
Abstract

The use of a serum-free environment and target cells carrying defined amounts of radiolabeled antigen allowed a quantitative study of the role of antigen, antibody, and complement on antibody-mediated cell cytotoxicity (AbMC). For lysis to occure, a minimum number of antigen molecules must be present on the target cell. 51Cr release from target cells with lower antigen density requires larger concentration of effector cells and antibodies. Target cell-bound complement, itself unable to mediate cytotoxicity, reduces the number of IgG molecules required for lysis. The antibody and complement, however, have to be bound to the same target cell. Bystander complement-coated erythrocytes, present in the same reaction mixture with IgG-coated targets, are not lysed. Blocking of AbMC is effected only by antigen, either soluble or in immune complexes prepared in antigen excess. Antigen competes at the level of the target cell. Blocking at the level of the effector cell, by use of immune complexes prepared at equivalence or in antibody excess, is difficult to achieve. The large number of cells with Fc receptors contained in mouse spleens may explain this finding. Arming of effector cells by passive binding of immune complexes is poorly effective as a means of obtaining lysis of the target cells. In all situations, the outcome of the reaction is determined by the presence of free antibody-combining sites, alone, or in immune complexes, that are able to combine with the target cell membrane antigen. The requirements for lysis are rather stringent.

摘要

使用无血清环境以及携带特定量放射性标记抗原的靶细胞,能够对抗原、抗体和补体在抗体介导的细胞毒性(AbMC)中的作用进行定量研究。为了发生裂解,靶细胞上必须存在最少数量的抗原分子。抗原密度较低的靶细胞释放(^{51}Cr)需要更高浓度的效应细胞和抗体。靶细胞结合的补体本身无法介导细胞毒性,但能减少裂解所需的IgG分子数量。然而,抗体和补体必须结合在同一靶细胞上。与IgG包被的靶细胞存在于同一反应混合物中的旁观者补体包被红细胞不会被裂解。AbMC的阻断仅由抗原实现,抗原可以是可溶性的,也可以是在抗原过量时制备的免疫复合物中的抗原。抗原在靶细胞水平上进行竞争。通过使用在等价或抗体过量时制备的免疫复合物在效应细胞水平上进行阻断很难实现。小鼠脾脏中含有大量具有Fc受体的细胞可能解释了这一发现。通过免疫复合物的被动结合来武装效应细胞作为获得靶细胞裂解的一种手段效果不佳。在所有情况下,反应的结果仅由游离的抗体结合位点决定,这些位点单独存在或存在于免疫复合物中,能够与靶细胞膜抗原结合。裂解的要求相当严格。

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