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记忆祖B细胞的沉默发育

Silent development of memory progenitor B cells.

作者信息

Aviszus Katja, Zhang Xianghua, Wysocki Lawrence J

机构信息

Integrated Department of Immunology, National Jewish Medical and Research Center, University of Colorado School of Medicine, Denver, CO 80206, USA.

出版信息

J Immunol. 2007 Oct 15;179(8):5181-90. doi: 10.4049/jimmunol.179.8.5181.

Abstract

T cell-dependent immune responses generate long-lived plasma cells and memory B cells, both of which express hypermutated Ab genes. The relationship between these cell types is not entirely understood. Both appear to emanate from the germinal center reaction, but it is unclear whether memory cells evolve while obligatorily generating plasma cells by siblings under all circumstances. In the experiments we report, plasma cell development was functionally segregated from memory cell development by a series of closely spaced injections of Ag delivered during the period of germinal center development. The injection series elevated serum Ab of low affinity, supporting the idea that a strong Ag signal drives plasma cell development. At the same time, the injection series produced a distinct population of affinity/specificity matured memory B cells that were functionally silent, as manifested by an absence of corresponding serum Ab. These cells could be driven by a final booster injection to develop into Ab-forming cells. This recall response required that a rest period precede the final booster injection, but a pause of only 4 days was sufficient. Our results support a model of memory B cell development in which extensive affinity/specificity maturation can take place within a B cell clone under some circumstances in which a concomitant generation of Ab-forming cells by siblings does not take place.

摘要

T细胞依赖性免疫反应产生长寿浆细胞和记忆B细胞,二者均表达超突变的抗体基因。这些细胞类型之间的关系尚未完全明确。二者似乎均源自生发中心反应,但尚不清楚记忆细胞在所有情况下是否在由同胞细胞产生浆细胞的同时必然发生演化。在我们报道的实验中,通过在生发中心发育期间进行一系列间隔紧密的抗原注射,浆细胞发育在功能上与记忆细胞发育相分离。注射系列提高了低亲和力血清抗体水平,支持了强抗原信号驱动浆细胞发育这一观点。与此同时,注射系列产生了一群亲和力/特异性成熟的记忆B细胞,这些细胞在功能上处于静止状态,表现为相应血清抗体的缺失。这些细胞可由最后一次加强注射驱动而发育为抗体形成细胞。这种回忆反应要求在最后一次加强注射之前有一个休息期,但仅4天的停顿就足够了。我们的结果支持一种记忆B细胞发育模型,即在某些情况下,B细胞克隆内可发生广泛的亲和力/特异性成熟,而同胞细胞不会同时产生抗体形成细胞。

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