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用新型隐球菌葡糖醛酸木糖甘露聚糖荚膜多糖疫苗接种引发的人单克隆抗体分析。

Analysis of human monoclonal antibodies elicited by vaccination with a Cryptococcus neoformans glucuronoxylomannan capsular polysaccharide vaccine.

作者信息

Pirofski L, Lui R, DeShaw M, Kressel A B, Zhong Z

机构信息

Department of Microbiology, Albert Einstein College of Medicine, Bronx, New York 10461, USA.

出版信息

Infect Immun. 1995 Aug;63(8):3005-14. doi: 10.1128/iai.63.8.3005-3014.1995.

Abstract

The Cryptococcus neoformans capsular polysaccharide glucuronoxylomannan (GXM) has been conjugated to tetanus toxoid (GXM-TT) as an investigational vaccine. GXM-TT elicits antibodies that are protective in C. neoformans-infected mice. In an effort to characterize the fine specificity and molecular structure of human GXM-TT-elicited antibodies, we generated two GXM monoclonal antibodies (MAbs) from peripheral blood lymphocytes of a volunteer GXM-TT recipient and studied serum GXM antibody idiotype expression in 10 additional vaccinees. The MAbs, 2E9 and 3B6, are the immunoglobulin M(lambda) isotype and bind capsular polysaccharides of C. neoformans serotypes other than the serotype A that was used for immunization. Neither antibody competes with murine GXM MAbs for antigen binding, suggesting that the human MAbs recognize a different epitope. The B-cell superantigen staphylococcal protein A binds both MAbs, and human immunodeficiency virus gp120 binds 2E9. MAb nucleic acid sequence analysis revealed that both antibodies use an identical V lambda 1a-J lambda genetic element with different, somatically mutated, members of the VH3 gene family and different DH and JH gene elements. The gene elements used by both MAbs occur in fetal B-lymphocyte repertoires, autoantibodies, and other polysaccharide antibodies. Post-GXM-TT vaccination GXM antibodies from 10 additional vaccinees expressed a shared idiotype defined by rabbit antiserum raised against MAb 2E9. Our data suggest that the human GXM antibody response is restricted and raise questions regarding the importance of specific variable-region elements and superantigens in the generation of human antibody responses to encapsulated pathogens.

摘要

新型隐球菌荚膜多糖葡糖醛酸木甘露聚糖(GXM)已与破伤风类毒素偶联(GXM-TT)作为一种研究性疫苗。GXM-TT能诱导产生对新型隐球菌感染小鼠具有保护作用的抗体。为了表征人源GXM-TT诱导抗体的精细特异性和分子结构,我们从一名GXM-TT志愿者接受者的外周血淋巴细胞中产生了两种GXM单克隆抗体(MAb),并研究了另外10名疫苗接种者血清中GXM抗体独特型的表达。单克隆抗体2E9和3B6属于免疫球蛋白M(λ)同种型,可结合除用于免疫的A型血清型以外的新型隐球菌血清型的荚膜多糖。两种抗体均不与鼠源GXM单克隆抗体竞争抗原结合,这表明人源单克隆抗体识别不同的表位。B细胞超抗原葡萄球菌蛋白A可结合这两种单克隆抗体,而人类免疫缺陷病毒gp120可结合2E9。单克隆抗体核酸序列分析表明,两种抗体均使用相同的Vλ1a-Jλ基因元件,与VH3基因家族中不同的、体细胞突变的成员以及不同的DH和JH基因元件结合。两种单克隆抗体使用的基因元件存在于胎儿B淋巴细胞库、自身抗体和其他多糖抗体中。在另外10名疫苗接种者接种GXM-TT后,其GXM抗体表达了一种由针对单克隆抗体2E9产生的兔抗血清所定义的共同独特型。我们的数据表明,人源GXM抗体反应受到限制,并引发了关于特定可变区元件和超抗原在人类对包膜病原体抗体反应产生中的重要性的问题。

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