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无T细胞的生发中心。

Germinal centers without T cells.

作者信息

de Vinuesa C G, Cook M C, Ball J, Drew M, Sunners Y, Cascalho M, Wabl M, Klaus G G, MacLennan I C

机构信息

Medical Research Council Centre for Immune Regulation, University of Birmingham, Birmingham B15 2TT, United Kingdom.

出版信息

J Exp Med. 2000 Feb 7;191(3):485-94. doi: 10.1084/jem.191.3.485.

Abstract

Germinal centers are critical for affinity maturation of antibody (Ab) responses. This process allows the production of high-efficiency neutralizing Ab that protects against virus infection and bacterial exotoxins. In germinal centers, responding B cells selectively mutate the genes that encode their receptors for antigen. This process can change Ab affinity and specificity. The mutated cells that produce high-affinity Ab are selected to become Ab-forming or memory B cells, whereas cells that have lost affinity or acquired autoreactivity are eliminated. Normally, T cells are critical for germinal center formation and subsequent B cell selection. Both processes involve engagement of CD40 on B cells by T cells. This report describes how high-affinity B cells can be induced to form large germinal centers in response to (4-hydroxy-3-nitrophenyl) acetyl (NP)-Ficoll in the absence of T cells or signaling through CD40 or CD28. This requires extensive cross-linking of the B cell receptors, and a frequency of antigen-specific B cells of at least 1 in 1,000. These germinal centers abort dramatically at the time when mutated high-affinity B cells are normally selected by T cells. Thus, there is a fail-safe mechanism against autoreactivity, even in the event of thymus-independent germinal center formation.

摘要

生发中心对于抗体(Ab)应答的亲和力成熟至关重要。这一过程使得高效中和抗体得以产生,从而抵御病毒感染和细菌外毒素。在生发中心,应答性B细胞会选择性地突变编码其抗原受体的基因。这一过程能够改变抗体的亲和力和特异性。产生高亲和力抗体的突变细胞会被选择成为抗体形成细胞或记忆B细胞,而失去亲和力或获得自身反应性的细胞则会被清除。正常情况下,T细胞对于生发中心的形成以及随后的B细胞选择至关重要。这两个过程都涉及T细胞与B细胞上CD40的结合。本报告描述了在没有T细胞或通过CD40或CD28进行信号传导的情况下,高亲和力B细胞如何能够被诱导形成大型生发中心以响应(4-羟基-3-硝基苯基)乙酰(NP)- 聚蔗糖。这需要B细胞受体的广泛交联,以及抗原特异性B细胞的频率至少为千分之一。这些生发中心在通常由T细胞选择突变的高亲和力B细胞的时间点会急剧衰退。因此,即使在非胸腺依赖性生发中心形成的情况下,也存在一种防止自身反应性的安全机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8c67/2195827/b0b564a006f0/JEM991778.f3.jpg

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