iScience (Sep 2022)

Tumor targeted 4-1BB agonist antibody-albumin fusions with high affinity to FcRn induce anti-tumor immunity without toxicity

  • Oana Hangiu,
  • Marta Compte,
  • Anders Dinesen,
  • Rocio Navarro,
  • Antonio Tapia-Galisteo,
  • Ole A. Mandrup,
  • Ainhoa Erce-Llamazares,
  • Rodrigo Lázaro-Gorines,
  • Daniel Nehme-Álvarez,
  • Carmen Domínguez-Alonso,
  • Seandean L. Harwood,
  • Carlos Alfonso,
  • Belen Blanco,
  • Laura Rubio-Pérez,
  • Anaïs Jiménez-Reinoso,
  • Laura Díez-Alonso,
  • Francisco J. Blanco,
  • Laura Sanz,
  • Kenneth A. Howard,
  • Luis Álvarez-Vallina

Journal volume & issue
Vol. 25, no. 9
p. 104958

Abstract

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Summary: Costimulation of tumor-infiltrating T lymphocytes by anti-4-1BB monoclonal antibodies (mAbs) has shown anti-tumor activity in human trials, but can be associated with significant off-tumor toxicities involving FcγR interactions. Here, we introduce albumin-fused mouse and human bispecific antibodies with clinically favorable pharmacokinetics designed to confine 4-1BB costimulation to the tumor microenvironment. These Fc-free 4-1BB agonists consist of an EGFR-specific VHH antibody, a 4-1BB-specific scFv, and a human albumin sequence engineered for high FcRn binding connected in tandem (LiTCo-Albu). We demonstrate in vitro cognate target engagement, EGFR-specific costimulatory activity, and FcRn-driven cellular recycling similar to non-fused FcRn high-binding albumin. The mouse LiTCo-Albu exhibited a prolonged circulatory half-life and in vivo tumor inhibition, with no indication of 4-1BB mAb-associated toxicity. Furthermore, we show a greater therapeutic effect when used in combination with PD-1-blocking mAbs. These findings demonstrate the feasibility of tumor-specific LiTCo-Albu antibodies for safe and effective costimulatory strategies in cancer immunotherapy.

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