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完整IgG的Fc部分可阻断抗T3对人外周血单核细胞的刺激。

The Fc portion of intact IgG blocks stimulation of human PBMC by anti-T3.

作者信息

Looney R J, Abraham G N

出版信息

J Immunol. 1984 Jul;133(1):154-6.

PMID:6609973
Abstract

The means by which normal human serum inhibits the activation of PBMC by OKT3 has been investigated. The Fc portion of intact IgG is shown to be the major inhibitor in human serum of this OKT3-induced stimulation. Furthermore, inhibition by IgG subclasses correlated with their ability to bind to the monocyte Fc receptor, i.e., IgG1 and IgG3 produced greater inhibition than IgG2 and IgG4, and this inhibition was competitive. In contrast, hypogammaglobulinemic serum, IgA, IgM, and F(ab')2 of IgG were not inhibitory relative to intact IgG or Fc of IgG. Because of the similarities between T3 and the idiotype-defined T cell receptor for antigen, these investigations suggest that IgG might modulate the interactions between the T cell recognition complex and anti-idiotype antibody, thus regulating the idiotype network.

摘要

已经研究了正常人血清抑制OKT3激活外周血单个核细胞(PBMC)的方式。完整IgG的Fc部分被证明是人类血清中这种OKT3诱导刺激的主要抑制剂。此外,IgG亚类的抑制作用与其结合单核细胞Fc受体的能力相关,即IgG1和IgG3产生的抑制作用大于IgG2和IgG4,并且这种抑制是竞争性的。相比之下,低丙种球蛋白血症血清、IgA、IgM以及IgG的F(ab')2相对于完整IgG或IgG的Fc没有抑制作用。由于T3与抗原的独特型定义的T细胞受体之间存在相似性,这些研究表明IgG可能调节T细胞识别复合物与抗独特型抗体之间的相互作用,从而调节独特型网络。

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