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在对三硝基苯基 - 聚蔗糖的抗体应答中T细胞对免疫球蛋白类别表达的调节。T细胞增强免疫球蛋白类别转换的证据。

T cell regulation of immunoglobulin class expression in the antibody response to trinitrophenyl-ficoll. Evidence for T cell enhancement of the immunoglobulin class switch.

作者信息

Mongini P K, Paul W E, Metcalf E S

出版信息

J Exp Med. 1982 Mar 1;155(3):884-902. doi: 10.1084/jem.155.3.884.

Abstract

In the absence of T cells, B cells were found to respond to the type 2 T-independent (TI-2) antigen, trinitrophenyl (TNP)-Ficoll, with a characteristic hierarchy of IgM and IgG subclass Ab production which directly correlated with 5' to 3' Igh-C gene order, i.e., IgM greater tha IgG3 greater than IgG1 greater than IgG2b greater than IgG2a. This was evident when immune serum Ab titers were analyzed, when in vitro secretion of antibody from immune cells was measured and when TNP-Ficoll-stimulated clones in a splenic focus assay were analyzed for isotype production. T cells were found to cause a preferential relative increase in the amount of IgG2a antibody produced to TNP-Ficoll. The T cell responsible was present in anti-IgM neonatally suppressed mice and was needed early in the response, i.e., on the day of immunization or earlier. T cells were found to increase the frequency of TNP-Ficoll-responsive B cell clones that produced IgG2a in the splenic focus assay. The great majority of these IgG2a-positive clones also produced IgM and all or nearly all of the IgG isotypes whose genes are encoded 5' to the Igh-gamma 2a gene. The data are discussed in terms to T cell enhancement of IgG2a Ab synthesis being mediated through T cell enhancement of the Igh-C gene switching mechanism within TNP-Ficoll-responsive B cell clones. Thus, isotypes encoded by genes on the 3' end of the Igh-gamma gene complex, which in the absence of T cells have a low probability of being switched to, are the most influenced by T cell help.

摘要

在缺乏T细胞的情况下,发现B细胞对2型非T细胞依赖性(TI-2)抗原三硝基苯基(TNP)-Ficoll有反应,产生具有特征性的IgM和IgG亚类抗体生成层次结构,这与5'至3'Igh-C基因顺序直接相关,即IgM>IgG3>IgG1>IgG2b>IgG2a。当分析免疫血清抗体滴度、测量免疫细胞体外抗体分泌以及在脾灶试验中分析TNP-Ficoll刺激的克隆的同种型产生时,这一点很明显。发现T细胞会使针对TNP-Ficoll产生的IgG2a抗体量相对优先增加。起作用的T细胞存在于新生期经抗IgM抑制的小鼠中,并且在反应早期即免疫当天或更早时是必需的。在脾灶试验中,发现T细胞增加了产生IgG2a的TNP-Ficoll反应性B细胞克隆的频率。这些IgG2a阳性克隆中的绝大多数也产生IgM以及其基因在Igh-γ2a基因5'端编码的所有或几乎所有IgG同种型。从T细胞增强IgG2a抗体合成是通过T细胞增强TNP-Ficoll反应性B细胞克隆内的Igh-C基因转换机制介导的角度对数据进行了讨论。因此,由Igh-γ基因复合体3'端基因编码的同种型,在没有T细胞的情况下转换的可能性较低,受T细胞辅助的影响最大。

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