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IgG1和IgG2b在小鼠巨噬细胞上共享Fc受体。

IgG1 and IgG2b share the Fc receptor on mouse macrophages.

作者信息

Diamond B, Scharff M D

出版信息

J Immunol. 1980 Aug;125(2):631-3.

PMID:7391572
Abstract

Monoclonal IgG1 anti-SRBC has been used to study the binding of monomeric and aggregated IgG1 to Fc receptors on mouse macrophages. Aggregated IgG1 was found to bind to Fc receptors on two macrophage cell lines and on primary macrophages. It competes for binding with IgG2b and not IgG2a. Like the binding of IgG2b, the binding of IgG1 is unaltered at 4 degrees C and is insensitive to trypsin or cytochalasin B. Antigen-bound IgG1, like IgG2b and IgG2a, mediates phagocytosis. Variant macrophage cell lines selected for the loss of phagocytosis through the IgG2b receptor no longer phagocytize IgG1 bearing SRBC. Monomeric IgG1 did not bind to either macrophage lines or primary macrophages. We conclude from these experiments that antigen-activated IgG1 binds to the same receptor as IgG2b.

摘要

单克隆IgG1抗绵羊红细胞已被用于研究单体和聚集的IgG1与小鼠巨噬细胞上Fc受体的结合。发现聚集的IgG1可与两种巨噬细胞系和原代巨噬细胞上的Fc受体结合。它与IgG2b竞争结合,而不与IgG2a竞争。与IgG2b的结合一样,IgG1在4℃时结合不变,对胰蛋白酶或细胞松弛素B不敏感。与IgG2b和IgG2a一样,抗原结合的IgG1介导吞噬作用。通过IgG2b受体选择失去吞噬作用的变异巨噬细胞系不再吞噬携带IgG1的绵羊红细胞。单体IgG1既不与巨噬细胞系结合,也不与原代巨噬细胞结合。我们从这些实验得出结论,抗原激活的IgG1与IgG2b结合到相同的受体上。

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