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单克隆IgG抗体协同补体介导大鼠红细胞溶解的机制。

The mechanism of synergistic complement-mediated lysis of rat red cells by monoclonal IgG antibodies.

作者信息

Hughes-Jones N C, Gorick B D, Howard J C

出版信息

Eur J Immunol. 1983 Aug;13(8):635-41. doi: 10.1002/eji.1830130806.

Abstract

The mechanism of synergistic complement-mediated lysis of rat red cells was investigated using rat monoclonal antibodies against class I RT1Aa antigens. The increased lytic activity when using two antibodies simultaneously is due to the increase in the number of activated C1 molecules on the cell surface and this results from (a) an increase in the number of binding sites for C1q, (b) an increase in the functional affinity constant for C1q binding and (c) an increase in the rate of activation of C1. Complete lysis of red cells was only achieved if one member of the synergistic pair was of the gamma 2b isotype, and this isotype was the only one to which binding of 125I-labeled C1q could be detected. A partial synergistic effect was seen using an F(ab')2 fragment of antibody. Increased uptake and activation of C1 probably results both from the presence of two antibodies attached to each antigen molecule and from the formation of antigen-antibody catenars.

摘要

利用抗I类RT1Aa抗原的大鼠单克隆抗体,研究了补体协同介导的大鼠红细胞溶解机制。同时使用两种抗体时裂解活性增强,这是由于细胞表面活化的C1分子数量增加,而这又源于:(a)C1q结合位点数量增加;(b)C1q结合的功能亲和常数增加;(c)C1活化速率增加。只有当协同对中的一个成员为γ2b同种型时,红细胞才能完全溶解,并且该同种型是唯一能检测到125I标记的C1q结合的同种型。使用抗体的F(ab')2片段可观察到部分协同效应。C1摄取和活化增加可能是由于每个抗原分子上附着两种抗体以及抗原-抗体链的形成。

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