| Literature DB >> 33488625 |
Marta Compte1, Seandean L Harwood2, Jorge Martínez-Torrecuadrada3, Gema Perez-Chacon4,5, Patricia González-García3, Antonio Tapia-Galisteo6, Paul M P Van Bergen En Henegouwen7, Aránzazu Sánchez8, Isabel Fabregat9, Laura Sanz6, Juan M Zapata4,5, Luis Alvarez-Vallina10,11.
Abstract
Agonistic monoclonal antibodies (mAbs) targeting the co-stimulatory receptor 4-1BB are among the most effective immunotherapeutic agents across pre-clinical cancer models. However, clinical development of full-length 4-1BB agonistic mAbs, has been hampered by dose-limiting liver toxicity. We have previously developed an EGFR-targeted 4-1BB-agonistic trimerbody (1D8N/CEGa1) that induces potent anti-tumor immunity without systemic toxicity, in immunocompetent mice bearing murine colorectal carcinoma cells expressing human EGFR. Here, we study the impact of human EGFR expression on mouse liver in the toxicity profile of 1D8N/CEGa1. Systemic administration of IgG-based anti-4-1BB agonist resulted in nonspecific immune stimulation and hepatotoxicity in a liver-specific human EGFR-transgenic immunocompetent mouse, whereas in 1D8N/CEGa1-treated mice no such immune-related adverse effects were observed. Collectively, these data support the role of FcγR interactions in the major off-tumor toxicities associated with IgG-based 4-1BB agonists and further validate the safety profile of EGFR-targeted Fc-less 4-1BB-agonistic trimerbodies in systemic cancer immunotherapy protocols.Entities:
Keywords: 4-1BB agonists; EGFR; EGFR-targeted 4-1BB agonists; cancer immunotherapy; hepatotoxicity; immunostimulatory antibodies; trimerbodies
Year: 2021 PMID: 33488625 PMCID: PMC7817978 DOI: 10.3389/fimmu.2020.614363
Source DB: PubMed Journal: Front Immunol ISSN: 1664-3224 Impact factor: 7.561