Frontiers in Immunology (Jan 2024)

Translatability of findings from cynomolgus monkey to human suggests a mechanistic role for IL-21 in promoting immunogenicity to an anti-PD-1/IL-21 mutein fusion protein

  • Mark A. Kroenke,
  • Marta Starcevic Manning,
  • Christina L. Zuch de Zafra,
  • Xinwen Zhang,
  • Kevin D. Cook,
  • Michael Archer,
  • Martijn P. Lolkema,
  • Jin Wang,
  • Sarah Hoofring,
  • Gurleen Saini,
  • Famke Aeffner,
  • Elizabeth Ahern,
  • Elena Garralda Cabanas,
  • Ramaswamy Govindan,
  • Mun Hui,
  • Shalini Gupta,
  • Daniel T. Mytych

DOI
https://doi.org/10.3389/fimmu.2024.1345473
Journal volume & issue
Vol. 15

Abstract

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AMG 256 is a bi-specific, heteroimmunoglobulin molecule with an anti-PD-1 antibody domain and a single IL-21 mutein domain on the C-terminus. Nonclinical studies in cynomolgus monkeys revealed that AMG 256 administration led to the development of immunogenicity-mediated responses and indicated that the IL-21 mutein domain of AMG 256 could enhance the anti-drug antibody response directed toward the monoclonal antibody domain. Anti-AMG 256 IgE were also observed in cynomolgus monkeys. A first-in-human (FIH) study in patients with advanced solid tumors was designed with these risks in mind. AMG 256 elicited ADA in 28 of 33 subjects (84.8%). However, ADA responses were only robust and exposure-impacting at the 2 lowest doses. At mid to high doses, ADA responses remained low magnitude and all subjects maintained exposure, despite most subjects developing ADA. Limited drug-specific IgE were also observed during the FIH study. ADA responses were not associated with any type of adverse event. The AMG 256 program represents a unique case where nonclinical studies informed on the risk of immunogenicity in humans, due to the IL-21-driven nature of the response.

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