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CD23b 同种型表达鉴定人类血吸虫病中新型活化 B 细胞亚群。

CD23b isoform expression in human schistosomiasis identifies a novel subset of activated B cells.

机构信息

Center for Global Health Research, Kenya Medical Research Institute, Kisumu, Kenya.

出版信息

Infect Immun. 2011 Sep;79(9):3770-7. doi: 10.1128/IAI.05094-11. Epub 2011 Jun 27.

Abstract

Resistance to schistosomiasis is associated with increased levels of serum parasite-specific IgE. IgE exerts its functions through its cellular receptors, FcεRI and FcεRII/CD23; however, its functional significance in humans requires further characterization. We previously reported that increased levels of CD23(+) B cells correlate with resistance to schistosomiasis in hyperexposed populations and sought to define their potential function and relationship with IgE. We found that CD23(+) B cells are a heterogeneous cell population with functional and phenotypic differences. Circulating CD23(+) B cells are uniquely activated in schistosomiasis and express the CD23b isoform and CXCR5, the homing receptor for lymphoid follicles. High CXCR5 expression by CD23(+) B cells was associated with the capacity to home to the cognate ligand CXCL13. CD23-bound IgE cross-linking increased surface expression of CXCR5, suggesting that CD23(+) B cells home directly into the lymphoid follicles upon antigen capture. As human schistosomiasis is an intravascular parasitic infection associated with a high antigenic burden in the blood, circulating CD23(+) B cells may play a role in the capture and shuttling of antigens directly to splenic follicles, highlighting a new role for circulating B cells. This function likely plays an important role in the development of protective immunity to infection with schistosomes.

摘要

对血吸虫病的抵抗力与血清寄生虫特异性 IgE 水平升高有关。IgE 通过其细胞受体 FcεRI 和 FcεRII/CD23 发挥作用;然而,其在人类中的功能意义需要进一步表征。我们之前报道过,在高暴露人群中,CD23(+)B 细胞水平升高与对血吸虫病的抵抗力相关,并试图确定其潜在功能及其与 IgE 的关系。我们发现 CD23(+)B 细胞是一个具有功能和表型差异的异质细胞群体。循环中的 CD23(+)B 细胞在血吸虫病中被独特地激活,并表达 CD23b 同工型和 CXCR5,这是淋巴滤泡的归巢受体。CD23(+)B 细胞高表达 CXCR5 与归巢到同源配体 CXCL13 的能力相关。CD23 结合的 IgE 交联增加了 CXCR5 的表面表达,表明 CD23(+)B 细胞在抗原捕获后直接归巢到淋巴滤泡中。由于人类血吸虫病是一种与血液中高抗原负荷相关的血管内寄生虫感染,循环中的 CD23(+)B 细胞可能在将抗原直接捕获并转运到脾脏滤泡中发挥作用,突出了循环 B 细胞的新作用。该功能可能在感染血吸虫病时产生保护性免疫的发展中发挥重要作用。

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