| Literature DB >> 30442944 |
Marta Compte1, Seandean Lykke Harwood2, Ines G Muñoz3, Rocio Navarro4, Manuela Zonca1, Gema Perez-Chacon5,6, Ainhoa Erce-Llamazares1, Nekane Merino7, Antonio Tapia-Galisteo4, Angel M Cuesta4, Kasper Mikkelsen2, Eduardo Caleiras8, Natalia Nuñez-Prado4, M Angela Aznar9, Simon Lykkemark2, Jorge Martínez-Torrecuadrada3, Ignacio Melero9,10,11,12, Francisco J Blanco7,13, Jorge Bernardino de la Serna14,15, Juan M Zapata5,6, Laura Sanz4, Luis Alvarez-Vallina16,17,18.
Abstract
The costimulation of immune cells using first-generation anti-4-1BB monoclonal antibodies (mAbs) has demonstrated anti-tumor activity in human trials. Further clinical development, however, is restricted by significant off-tumor toxicities associated with FcγR interactions. Here, we have designed an Fc-free tumor-targeted 4-1BB-agonistic trimerbody, 1D8N/CEGa1, consisting of three anti-4-1BB single-chain variable fragments and three anti-EGFR single-domain antibodies positioned in an extended hexagonal conformation around the collagen XVIII homotrimerization domain. The1D8N/CEGa1 trimerbody demonstrated high-avidity binding to 4-1BB and EGFR and a potent in vitro costimulatory capacity in the presence of EGFR. The trimerbody rapidly accumulates in EGFR-positive tumors and exhibits anti-tumor activity similar to IgG-based 4-1BB-agonistic mAbs. Importantly, treatment with 1D8N/CEGa1 does not induce systemic inflammatory cytokine production or hepatotoxicity associated with IgG-based 4-1BB agonists. These results implicate FcγR interactions in the 4-1BB-agonist-associated immune abnormalities, and promote the use of the non-canonical antibody presented in this work for safe and effective costimulatory strategies in cancer immunotherapy.Entities:
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Year: 2018 PMID: 30442944 PMCID: PMC6237851 DOI: 10.1038/s41467-018-07195-w
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919