PLoS Biology (Jan 2016)

A Novel Platform for the Potentiation of Therapeutic Antibodies Based on Antigen-Dependent Formation of IgG Hexamers at the Cell Surface.

  • Rob N de Jong,
  • Frank J Beurskens,
  • Sandra Verploegen,
  • Kristin Strumane,
  • Muriel D van Kampen,
  • Marleen Voorhorst,
  • Wendy Horstman,
  • Patrick J Engelberts,
  • Simone C Oostindie,
  • Guanbo Wang,
  • Albert J R Heck,
  • Janine Schuurman,
  • Paul W H I Parren

DOI
https://doi.org/10.1371/journal.pbio.1002344
Journal volume & issue
Vol. 14, no. 1
p. e1002344

Abstract

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IgG antibodies can organize into ordered hexamers on cell surfaces after binding their antigen. These hexamers bind the first component of complement C1 inducing complement-dependent target cell killing. Here, we translated this natural concept into a novel technology platform (HexaBody technology) for therapeutic antibody potentiation. We identified mutations that enhanced hexamer formation and complement activation by IgG1 antibodies against a range of targets on cells from hematological and solid tumor indications. IgG1 backbones with preferred mutations E345K or E430G conveyed a strong ability to induce conditional complement-dependent cytotoxicity (CDC) of cell lines and chronic lymphocytic leukemia (CLL) patient tumor cells, while retaining regular pharmacokinetics and biopharmaceutical developability. Both mutations potently enhanced CDC- and antibody-dependent cellular cytotoxicity (ADCC) of a type II CD20 antibody that was ineffective in complement activation, while retaining its ability to induce apoptosis. The identified IgG1 Fc backbones provide a novel platform for the generation of therapeutics with enhanced effector functions that only become activated upon binding to target cell-expressed antigen.