| Literature DB >> 27262204 |
Guoying Jiang1, Christopher Yu2, Daniela B Yadav3, Zhilan Hu4, Annamarie Amurao5, Eileen Duenas5, Marc Wong5, Mark Iverson5, Kai Zheng6, Xanthe Lam6, Jia Chen2, Roxanne Vega7, Sheila Ulufatu7, Cecilia Leddy7, Helen Davis7, Amy Shen4, Pin Y Wong8, Reed Harris2, Y John Wang6, Dongwei Li3.
Abstract
Due to their potential influence on stability, pharmacokinetics, and product consistency, antibody charge variants have attracted considerable attention in the biotechnology industry. Subtle to significant differences in the level of charge variants and new charge variants under various cell culture conditions are often observed during routine manufacturing or process changes and pose a challenge when demonstrating product comparability. To explore potential solutions to control charge heterogeneity, monoclonal antibodies (mAbs) with native, wild-type C-termini, and mutants with C-terminal deletions of either lysine or lysine and glycine were constructed, expressed, purified, and characterized in vitro and in vivo. Analytical and physiological characterization demonstrated that the mAb mutants had greatly reduced levels of basic variants without decreasing antibody biologic activity, structural stability, pharmacokinetics, or subcutaneous bioavailability in rats. This study provides a possible solution to mitigate mAb heterogeneity in C-terminal processing, improve batch-to-batch consistency, and facilitate the comparability study during process changes. Published by Elsevier Inc.Entities:
Keywords: C-terminal Lys deletion; Lys and Gly deletion; bioavailability; charge heterogeneity; mAb; pharmacokinetics
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Year: 2016 PMID: 27262204 DOI: 10.1016/j.xphs.2016.04.027
Source DB: PubMed Journal: J Pharm Sci ISSN: 0022-3549 Impact factor: 3.534