Scientific Reports (Sep 2021)

A new approach to produce IgG4-like bispecific antibodies

  • Caizhi Zhao,
  • Wei Zhang,
  • Guihua Gong,
  • Liping Xie,
  • Ming-Wei Wang,
  • Youjia Hu

DOI
https://doi.org/10.1038/s41598-021-97393-2
Journal volume & issue
Vol. 11, no. 1
pp. 1 – 12

Abstract

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Abstract While achieving rapid developments in recent years, bispecific antibodies are still difficult to design and manufacture, due to mispair of both heavy and light chains. Here we report a novel technology to make bispecific molecules. The knob-into-hole method was used to pair two distinct heavy chains as a heterodimer. IgG4 S228P CH1-CL interface was then partially replaced by T-cell receptor α/β constant domain to increase the efficiency of cognate heavy and light chain pairing. Following expression and purification, the bispecific antibody interface exchange was confirmed by Western blotting and LC–MS/MS. To ensure its validity, we combined a monovalent bispecific antibody against PD-1 (sequence from Pembrolizumab) and LAG3 (sequence from Relatlimab). The results showed that the molecule could be assembled correctly at a ratio of 95% in cells. In vitro functional assay demonstrated that the purified bispecific antibody exhibits an enhanced agonist activity compared to that of the parental antibodies. Low immunogenicity was predicted by an open-access software and ADA test.