Immunogenicity Risk Assessment of Biotherapeutics Using an Ex Vivo B Cell Assay.

IF 2.7 Q3 IMMUNOLOGY

Antibodies Pub Date : 2025-07-22 DOI:10.3390/antib14030062

Kevin M Budge, Ross Blankenship, Patricia Brown-Augsburger, Lukasz K Chlewicki

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引用次数: 0

Abstract

Background/objectives: Anti-drug antibody (ADA) formation can impact the safety, pharmacokinetics, and/or efficacy of biotherapeutics, including monoclonal antibodies (mAbs). Current strategies for ADA/immunogenicity risk prediction of mAbs include in silico algorithms, T cell proliferation assays, MHC-associated peptide proteomics assays (MAPPs), and dendritic cell internalization assays. However, B cell-mediated responses are not assessed in these assays. B cells are professional antigen-presenting cells (APCs) and secrete antibodies toward immunogenic mAbs. Therefore, methods to determine B cell responses would be beneficial for immunogenicity risk prediction and may provide a more comprehensive assessment of risk.

Methods: We used a PBMC culture method with the addition of IL-4, IL-21, B cell activating factor (BAFF), and an anti-CD40 agonist mAb to support B cell survival and activation.

Results: B cells in this assay format become activated, proliferate, and secrete IgG. A panel of 51 antibodies with varying clinical immunogenicity rates were screened in this assay with IgG secretion used as a readout for immunogenicity risk. IgG secretion differed among test articles but did not correlate with the clinical immunogenicity rating.

Conclusions: This dataset highlights the challenges of developing a B cell assay for immunogenicity risk prediction and provides a framework for further refinement of a B cell-based assay for immunogenicity risk prediction of mAbs.

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利用体外B细胞试验评估生物治疗药物的免疫原性风险。

背景/目的：抗药物抗体（ADA）的形成会影响生物治疗药物的安全性、药代动力学和/或疗效，包括单克隆抗体（mab）。目前单克隆抗体的ADA/免疫原性风险预测策略包括计算机算法、T细胞增殖测定、mhc相关肽蛋白质组学测定（MAPPs）和树突状细胞内化测定。然而，在这些试验中没有评估B细胞介导的反应。B细胞是专业的抗原呈递细胞（APCs），分泌针对免疫原性单克隆抗体的抗体。因此，确定B细胞反应的方法将有利于免疫原性风险预测，并可能提供更全面的风险评估。方法：采用PBMC培养法，加入IL-4、IL-21、B细胞活化因子（BAFF）和抗cd40激动剂mAb，支持B细胞存活和活化。结果：B细胞被激活、增殖并分泌IgG。该试验筛选了51种具有不同临床免疫原性率的抗体，用IgG分泌量作为免疫原性风险的读数。IgG的分泌量在不同的试验品之间存在差异，但与临床免疫原性评级无关。结论：该数据集强调了开发用于免疫原性风险预测的B细胞检测的挑战，并为进一步完善基于B细胞的单克隆抗体免疫原性风险预测检测提供了框架。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Antibodies IMMUNOLOGY-

CiteScore

7.10

自引率

6.40%

发文量

审稿时长

11 weeks

期刊介绍： Antibodies (ISSN 2073-4468), an international, peer-reviewed open access journal which provides an advanced forum for studies related to antibodies and antigens. It publishes reviews, research articles, communications and short notes. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. There is no restriction on the length of the papers. Full experimental and/or methodical details must be provided. Electronic files or software regarding the full details of the calculation and experimental procedure - if unable to be published in a normal way - can be deposited as supplementary material. This journal covers all topics related to antibodies and antigens, topics of interest include (but are not limited to): antibody-producing cells (including B cells), antibody structure and function, antibody-antigen interactions, Fc receptors, antibody manufacturing antibody engineering, antibody therapy, immunoassays, antibody diagnosis, tissue antigens, exogenous antigens, endogenous antigens, autoantigens, monoclonal antibodies, natural antibodies, humoral immune responses, immunoregulatory molecules.