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Evaluation of Heavy Chain C-Terminal Deletions on Productivity and Product Quality of Monoclonal Antibodies in Chinese Hamster Ovary (CHO) Cells

机译:重链C末端缺失对中国仓鼠卵巢(CHO)细胞单克隆抗体生产率和产品质量的评价

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摘要

Monoclonal antibodies (mAbs) have been well established as potent therapeutic agents and are used to treat many different diseases. During cell culture production, antibody charge variants can be generated by cleavage of heavy chain (HC) C-terminal lysine and proline amidation. Differences in levels of charge variants during manufacturing process changes make it challenging to demonstrate process comparability. In order to reduce heterogeneity and achieve consistent product quality, we generated and expressed antibodies with deletion of either HC C-terminal lysine (-K) or lysine and glycine (-GK). Interestingly, clones that express antibodies lacking HC C-terminal lysine (-K) had considerably lower specific productivities compared to clones that expressed either wild type antibodies (WT) or antibodies lacking HC glycine and lysine (-GK). While no measurable differences in antibody HC and LC mRNA levels, glycosylation and secretion were observed, our analysis suggests that the lower specific productivity of clones expressing antibody lacking HC C-terminal lysine was due to slower antibody HC synthesis and faster antibody degradation. (C) 2017 American Institute of Chemical Engineers
机译:单克隆抗体(mAbs)已得到很好地建立为有效的治疗剂,并用于治疗许多不同的疾病。在细胞培养生产期间,可以通过裂解重链(HC)C-末端赖氨酸和脯氨酸酰胺的切割产生抗体电荷变体。制造过程中电荷变体水平的差异变化使其具有挑战性地证明过程可比性。为了减少异质性并实现一致的产品质量,我们产生并表达了缺失HC C末端赖氨酸(-K)或赖氨酸和甘氨酸(-GK)的抗体。有趣的是,与表达缺乏HC甘氨酸和赖氨酸(-GK)的克隆相比,表达缺乏HC C-末端赖氨酸(-K)的克隆的克隆具有显着降低的特异性生产率。虽然未观察到抗体HC和LC mRNA水平的可测量差异,但我们的分析表明表达缺少HC C末端赖氨酸的抗体的克隆的较低比生产率是由于较慢的抗体HC合成和更快的抗体降解。 (c)2017美国化学工程师研究所

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