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一种疟疾多克隆B细胞激活剂可提高B细胞存活率并优先激活记忆细胞区室。

Increased B cell survival and preferential activation of the memory compartment by a malaria polyclonal B cell activator.

作者信息

Donati Daria, Mok Bobo, Chêne Arnaud, Xu Hong, Thangarajh Mathula, Glas Rickard, Chen Qijun, Wahlgren Mats, Bejarano Maria Teresa

机构信息

Center for Infectious Medicine, Department of Medicine, Karolinska Institutet, Karolinska University Hospital Huddinge, Stockholm, Sweden.

出版信息

J Immunol. 2006 Sep 1;177(5):3035-44. doi: 10.4049/jimmunol.177.5.3035.

DOI:10.4049/jimmunol.177.5.3035
PMID:16920940
Abstract

Chronic malaria infection is characterized by polyclonal B cell activation, hyperglobulinemia, and elevated titers of autoantibodies. We have recently identified the cysteine-rich interdomain region 1alpha (CIDR1alpha) of the Plasmodium falciparum erythrocyte membrane protein 1 as a T cell-independent polyclonal B cell activator and Ig binding protein. Here, we show that, although the binding affinity of CIDR1alpha to human IgM and IgG is relatively low, B cell activation still proceeds. CIDR1alpha rescues tonsillar B cells from apoptosis, and increases the proportion of cycling cells. Comparison of the impact on naive and memory B cell compartment indicated that CIDR1alpha preferentially activates memory B lymphocytes. Analysis of the gene expression profiles induced by CIDR1alpha and anti-Ig activation using a cDNA microarray demonstrated a low degree of homology in the signatures imposed by both stimuli. The microarray data correlate with the functional analysis demonstrating that CIDR1alpha activates various immunological pathways and protects B cells from apoptosis. Together, the results provide evidence for a role of malaria in preferentially activating the memory B cell compartment. The polyclonal B cell activation and augmented survival induced by CIDR1alpha is of relevance for understanding the mechanisms behind the increased risk of Burkitt's lymphoma in malaria endemic areas.

摘要

慢性疟疾感染的特征是多克隆B细胞活化、高球蛋白血症和自身抗体滴度升高。我们最近已确定恶性疟原虫红细胞膜蛋白1富含半胱氨酸的结构域间区域1α(CIDR1α)是一种不依赖T细胞的多克隆B细胞激活剂和Ig结合蛋白。在此,我们表明,尽管CIDR1α与人IgM和IgG的结合亲和力相对较低,但B细胞活化仍会发生。CIDR1α可挽救扁桃体B细胞免于凋亡,并增加循环细胞的比例。对幼稚和记忆B细胞区室影响的比较表明,CIDR1α优先激活记忆B淋巴细胞。使用cDNA微阵列分析由CIDR1α和抗Ig激活诱导的基因表达谱,结果显示两种刺激所产生的特征具有低度同源性。微阵列数据与功能分析相关,表明CIDR1α激活各种免疫途径并保护B细胞免于凋亡。总之,这些结果为疟疾在优先激活记忆B细胞区室中所起的作用提供了证据。CIDR1α诱导的多克隆B细胞活化和增强的存活与理解疟疾流行地区伯基特淋巴瘤风险增加背后的机制有关。

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