Structural design of tetravalent T-cell engaging bispecific antibodies: improve developability by engineering disulfide bonds

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作者
Lin Yu
Nan Huang
Liangpeng Ge
Heng Sun
Yuna Fu
Chundong Liu
Jianhua Wang
机构
[1] Chongqing University,Key Laboratory of Biorheological Science and Technology (Ministry of Education)
[2] Chongqing University,College of Bioengineering
[3] Chongqing Academy of Animal Sciences,Qiuzhen College
[4] Chongqing Engineering Technology Research Center for Medical Animal Resources Development and Application,undefined
[5] Huzhou University,undefined
来源
Journal of Biological Engineering | / 15卷
关键词
Bispecific antibody; ScFv; Disulfide bond; Stability;
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摘要
Since the advances in protein engineering and manufacture, over the last 30 years, antibody-based immunotherapeutic has become a powerful strategy to treat diseases. The T-cell engaging bispecific antibody (BsAb) by combining the Fab binding domain of tumor antigens and Fab or single-chain variable fragments (scFvs) binding domain of CD3 molecules, could redirect cytotoxic T cells to kill tumor cells. The IgG-scFv format of BsAb is a dual bivalent and asymmetrical design, which adds the benefit of potent cytotoxicity and less complicated for manufacture but limits the stability and production. Here, we engineered a series of interchain disulfide bonds in the Fab region of IgG-svFv BsAbs and evaluated its biophysical and biological properties. We found that simultaneously replaced the position of VH44-VL100 and CH1126-CL121 residues with cysteine, to form two additional disulfide bonds, could markedly increase monomeric BsAb formation and yield. The thermostability and stability against aggregation and degradation also performed better than BsAbs without extra disulfide bonds introduction. Besides, the affinity of engineered BsAbs was maintained, and the h8B-BsAb antibody had a slight enhancement in an inhibitory effect on target cells.
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