Agrafiotis Andreas, Neumeier Daniel, Hong Kai-Lin, Chowdhury Tasnia, Ehling Roy, Kuhn Raphael, Sandu Ioana, Kreiner Victor, Cotet Tudor-Stefan, Shlesinger Danielle, Laslo Daria, Anzböck Stine, Starkie Dale, Lightwood Daniel J, Oxenius Annette, Reddy Sai T, Yermanos Alexander
Department of Biosystems Science and Engineering, ETH Zurich, Basel, Switzerland.
Institute of Microbiology, ETH Zurich, Zurich, Switzerland.
iScience. 2023 Jan 25;26(3):106055. doi: 10.1016/j.isci.2023.106055. eCollection 2023 Mar 17.
Although new genomics-based pipelines have potential to augment antibody discovery, these methods remain in their infancy due to an incomplete understanding of the selection process that governs B cell clonal selection, expansion, and antigen specificity. Furthermore, it remains unknown how factors such as aging and reduction of tolerance influence B cell selection. Here we perform single-cell sequencing of antibody repertoires and transcriptomes of murine B cells following immunizations with a model therapeutic antigen target. We determine the relationship between antibody repertoires, gene expression signatures, and antigen specificity across 100,000 B cells. Recombinant expression and characterization of 227 monoclonal antibodies revealed the existence of clonally expanded and class-switched antigen-specific B cells that were more frequent in young mice. Although integrating multiple repertoire features such as germline gene usage and transcriptional signatures failed to distinguish antigen-specific from nonspecific B cells, other features such as immunoglobulin G (IgG) subtype and sequence composition correlated with antigen specificity.
尽管基于新基因组学的流程有增强抗体发现的潜力,但由于对控制B细胞克隆选择、扩增和抗原特异性的选择过程理解不完整,这些方法仍处于起步阶段。此外,衰老和耐受性降低等因素如何影响B细胞选择仍不清楚。在这里,我们对用一种模型治疗性抗原靶点免疫后的小鼠B细胞抗体库和转录组进行了单细胞测序。我们确定了100,000个B细胞中抗体库、基因表达特征和抗原特异性之间的关系。227种单克隆抗体的重组表达和表征揭示了克隆扩增和类别转换的抗原特异性B细胞的存在,这些细胞在年轻小鼠中更为常见。尽管整合多个库特征(如种系基因使用和转录特征)未能区分抗原特异性B细胞和非特异性B细胞,但其他特征(如免疫球蛋白G(IgG)亚型和序列组成)与抗原特异性相关。
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