iScience (Dec 2021)

Next generation Fc scaffold for multispecific antibodies

  • Bram Estes,
  • Athena Sudom,
  • Danyang Gong,
  • Douglas A. Whittington,
  • Vivian Li,
  • Christopher Mohr,
  • Danqing Li,
  • Timothy P. Riley,
  • Stone D.-H. Shi,
  • Jun Zhang,
  • Fernando Garces,
  • Zhulun Wang

Journal volume & issue
Vol. 24, no. 12
p. 103447

Abstract

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Summary: Bispecific antibodies (Bispecifics) demonstrate exceptional clinical potential to address some of the most complex diseases. However, Bispecific production in a single cell often requires the correct pairing of multiple polypeptide chains for desired assembly. This is a considerable hurdle that hinders the development of many immunoglobulin G (IgG)-like bispecific formats. Our approach focuses on the rational engineering of charged residues to facilitate the chain pairing of distinct heavy chains (HC). Here, we deploy structure-guided protein design to engineer charge pair mutations (CPMs) placed in the CH3-CH3′ interface of the fragment crystallizable (Fc) region of an antibody (Ab) to correctly steer heavy chain pairing. When used in combination with our stable effector functionless 2 (SEFL2.2) technology, we observed high pairing efficiency without significant losses in expression yields. Furthermore, we investigate the relationship between CPMs and the sequence diversity in the parental antibodies, proposing a rational strategy to deploy these engineering technologies.

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