Molecular Landscape of Anti-Drug Antibodies Reveals the Mechanism of the Immune Response Following Treatment With TNFα Antagonists

抗药物抗体的分子图谱揭示了TNFα拮抗剂治疗后免疫反应的机制

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作者:Anna Vaisman-Mentesh ,Shai Rosenstein ,Miri Yavzori ,Yael Dror ,Ella Fudim ,Bella Ungar ,Uri Kopylov ,Orit Picard ,Aya Kigel ,Shomron Ben-Horin ,Itai Benhar ,Yariv Wine

Abstract

Drugs formulated from monoclonal antibodies (mAbs) are clinically effective in various diseases. Repeated administration of mAbs, however, elicits an immune response in the form of anti-drug-antibodies (ADA), thereby reducing the drug's efficacy. Notwithstanding their importance, the molecular landscape of ADA and the mechanisms involved in their formation are not fully understood. Using a newly developed quantitative bio-immunoassay, we found that ADA concentrations specific to TNFα antagonists can exceed extreme concentrations of 1 mg/ml with a wide range of neutralization capacity. Our data further suggest a preferential use of the λ light chain in a subset of neutralizing ADA. Moreover, we show that administration of TNFα antagonists result in a vaccine-like response whereby ADA formation is governed by the extrafollicular T cell-independent immune response. Our bio-immunoassay coupled with insights on the nature of the immune response can be leveraged to improve mAb immunogenicity assessment and facilitate improvement in therapeutic intervention strategies. Keywords: anti-drug antibodies; antibody repertoire; biologics; high-throughput sequencing; immunogenicity; monoclonal antibody; next generation sequencing; proteomics.

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