Class-Switching of B Lymphocytes by DNA and Cell Immunization for Stereospecific Monoclonal Antibodies against Native GPCR

Yushi Isozaki, K. Tsumoto, M. Tomita
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引用次数: 1

Abstract

To develop efficient applications of monoclonal antibodies for therapeutic purposes, stereospecific recognition of the target antigens is needed. DNA immunization is one of the best methods for sensitizing B lymphocytes that can produce conformation-specific antibodies. Here we verified the class-switching of monoclonal antibodies by DNA immunization followed by cell immunization for the generation of stereospecific monoclonal antibodies against native G protein-coupled receptor (GPCR) using the optimized stereospecific targeting (SST) technique. This technology facilitates the efficient selection of sensitized B lymphocytes through specific interaction with the intact antigen via B-cell receptors (BCRs). We demonstrate that multiple DNA immunizations followed by a single cell immunization in combination with a longer sensitization period (three to four months) are an appropriate sensitizing strategy for the generation of IgG-type stereospecific monoclonal antibodies by class-switching, and the characteristics of antibody production could be transferred to hybridoma cells provided by the optimized SST technique.
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B淋巴细胞的DNA转换和抗GPCR立体特异性单克隆抗体的细胞免疫
为了开发有效的单克隆抗体用于治疗目的,需要对靶抗原进行立体特异性识别。DNA免疫是致敏B淋巴细胞的最佳方法之一,可以产生构象特异性抗体。本研究利用优化的立体特异性靶向(SST)技术,通过DNA免疫和细胞免疫,验证了单克隆抗体的类别转换,生成了针对天然G蛋白偶联受体(GPCR)的立体特异性单克隆抗体。该技术通过B细胞受体(BCRs)与完整抗原特异性相互作用,促进了致敏B淋巴细胞的高效选择。我们证明,多次DNA免疫后再进行单细胞免疫,并结合较长的致敏期(3至4个月),是通过类别转换产生igg型立体特异性单克隆抗体的合适的致敏策略,并且优化的SST技术可以将抗体产生的特性转移到杂交瘤细胞中。
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来源期刊
Immuno-Analyse & Biologie Specialisee
Immuno-Analyse & Biologie Specialisee 医学-医学实验技术
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审稿时长
6-12 weeks
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