Comprehensive Stress Stability Studies Reveal the Prominent Stability of the Liquid-Formulated Biotherapeutic Asymmetric Monovalent Bispecific IgG1 Monoclonal Antibody Format

去酰胺 单克隆抗体 化学 糖基化 表位 异构化 抗体 生物化学 二硫键 生物物理学 免疫学 催化作用 受体 生物
作者
Praveen Kallamvalliillam Sankaran,Ryte Poskute,Lydia Dewis,Yasunori Watanabe,Vanessa Wong,Laura Pascual Fernandez,Richard Shannon,Lisa Wong,Rebecca Shrubsall,Lee Carman,Alexander Holt,Giordana Lepore,Rahul Mishra,Laura Sewell,Matt Gothard,Matthew Cheeks,Viv Lindo
出处
期刊:Journal of Pharmaceutical Sciences [Elsevier BV]
卷期号:113 (8): 2101-2113 被引量:2
标识
DOI:10.1016/j.xphs.2024.04.029
摘要

The developed asymmetric monovalent bispecific IgG1 or Duet monoclonal antibody (Duet mAb) has two distinct fragment antigen-binding region (Fab) subunits that target two different epitope specificities sequentially or simultaneously. The design features include unique engineered disulfide bridges, knob-into-hole mutations, and kappa and lambda chains to produce Duet mAbs. These make it structurally and functionally complex, so one expects challenging developability linked to instability, degradation of products and pathways, and limited reports available. Here, we have treated the product with different sources of extreme stress over a lengthy period, including varying heat, pH, photo stress, chemical oxidative stress, accelerated stress in physiological conditions, and forced glycation conditions. The effects of different stress conditions on the product were assessed using various analytical characterization tools to measure product-related substances, post-translational modifications (PTMs), structural integrity, higher-order disulfide linkages, and biological activity. The results revealed degradation products and pathways of Duet mAb. A moderate increase in size, charge, and hydrophobic variants, PTMs, including deamidation, oxidation, isomerization, and glycation were observed, with most conditions exhibiting biological activity. In addition, the characterization of fractionated charge variants, including deamidated species, showed satisfactory biological activity. This study demonstrated the prominent stability of the Duet mAb format comparable to most marketed mAbs.
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