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使用抗原四聚体对稀有记忆 B 细胞进行体外表型鉴定和分离。

Ex vivo characterization and isolation of rare memory B cells with antigen tetramers.

机构信息

Department of Cancer Immunology & AIDS, Dana-Farber Cancer Institute, Boston, MA 02215-5450, USA.

出版信息

Blood. 2011 Jul 14;118(2):348-57. doi: 10.1182/blood-2011-03-341917. Epub 2011 May 6.

Abstract

Studying human antigen-specific memory B cells has been challenging because of low frequencies in peripheral blood, slow proliferation, and lack of antibody secretion. Therefore, most studies have relied on conversion of memory B cells into antibody-secreting cells by in vitro culture. To facilitate direct ex vivo isolation, we generated fluorescent antigen tetramers for characterization of memory B cells by using tetanus toxoid as a model antigen. Brightly labeled memory B cells were identified even 4 years after last immunization, despite low frequencies ranging from 0.01% to 0.11% of class-switched memory B cells. A direct comparison of monomeric to tetrameric antigen labeling demonstrated that a substantial fraction of the B-cell repertoire can be missed when monomeric antigens are used. The specificity of the method was confirmed by antibody reconstruction from single-cell sorted tetramer(+) B cells with single-cell RT-PCR of the B-cell receptor. All antibodies bound to tetanus antigen with high affinity, ranging from 0.23 to 2.2 nM. Furthermore, sequence analysis identified related memory B cell and plasmablast clones isolated more than a year apart. Therefore, antigen tetramers enable specific and sensitive ex vivo characterization of rare memory B cells as well as the production of fully human antibodies.

摘要

研究人类抗原特异性记忆 B 细胞一直具有挑战性,因为其在外周血中的频率较低、增殖缓慢且缺乏抗体分泌。因此,大多数研究依赖于将记忆 B 细胞体外培养转化为分泌抗体的细胞。为了便于直接在体外分离,我们使用破伤风类毒素作为模型抗原,生成了荧光抗原四聚体来对记忆 B 细胞进行特征分析。即使在最后一次免疫后 4 年,仍能识别到标记的记忆 B 细胞,尽管其频率较低,在转换的记忆 B 细胞中为 0.01%至 0.11%。单体抗原与四聚体抗原标记的直接比较表明,当使用单体抗原时,B 细胞库的很大一部分可能会被遗漏。该方法的特异性通过从单细胞分选的四聚体(+)B 细胞中进行单细胞 RT-PCR 重建抗体进行了确认。所有抗体与破伤风抗原的结合亲和力很高,范围为 0.23 至 2.2 nM。此外,序列分析鉴定出相隔一年以上分离的相关记忆 B 细胞和浆母细胞克隆。因此,抗原四聚体可特异性和敏感地对稀有记忆 B 细胞进行体外特征分析,并产生完全人源抗体。

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