Enhancing thermal stability in the CH2 domain to suppress aggregation through the introduction of simultaneous disulfide bonds in Pichia pastoris

Author:

Oyama Kosuke1ORCID,Nakakido Makoto2ORCID,Ohkuri Takatoshi3ORCID,Nakamura Hitomi3,Tsumoto Kouhei2,Ueda Tadashi1

Affiliation:

1. Graduate School of Pharmaceutical Sciences Kyushu University Fukuoka Japan

2. Graduate School of Engineering The University of Tokyo Tokyo Japan

3. Faculty of Pharmaceutical Sciences Sojo University Kumamoto Japan

Abstract

AbstractProtein aggregations decrease production yields and impair the efficacy of therapeutics. The CH2 domain is a crucial part of the constant region of human IgG. But, it is also the least stable domain in IgG, which can result in antibody instability and aggregation problems. We created a novel mutant of the CH2 domain (T250C/L314C, mut10) by introducing a disulfide bond and expressed it using Pichia pastoris. The mut10 variant exhibited enhanced thermal stability, resistance to enzymatic degradation, and reduced aggregation in comparison to the original CH2 domain. However, it was less stable than mut20 (L242C/K334C), which is the variant prepared in a previous study (Gong et al., J. Biol. Chem., 2009). A more advanced mutant, mut25, was created by combining mut10 and mut20. Mut25 artificially contains two disulfide bonds. The new mutant, mut25, showed enhanced thermal stability, increased resistance to enzymatic digestion, and reduced aggregation in comparison to mut20. According to our knowledge, mut25 achieves an unprecedented level of stability among the humanized whole CH2 domains that have been reported so far. Mut25 has the potential to serve as a new platform for antibody therapeutics due to its ability to reduce immunogenicity by decreasing aggregation.

Publisher

Wiley

Subject

Molecular Biology,Biochemistry

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