A tumor-targeted trimeric 4-1BB-agonistic antibody induces potent anti-tumor immunity without systemic toxicity

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 Fc gamma R interactions. Here, we have desig...

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Autores: Compte, M. (Marta)|||/items/17255d0f-5af9-4a6c-b580-886ddbd8a7f0, Harwood, S.L. (Seandean Lykke)|||/items/55124f98-0659-45cd-a1fb-c8d69e98b475, Muñoz, I.G. (Inés G.)|||/items/9cb7c656-9a91-49bb-ae66-2c63ec7e82ad, Navarro, R. (Rocío)|||/items/81f40442-386e-4a34-8e07-d62c96180460, Zonca, M. (Manuela)|||/items/63acc310-55c0-47e4-a044-148c80783b7d, Pérez-Chacon, G. (Gema)|||/items/7f9e1301-12b7-484d-8f67-b62927926a94, Erce-Llamazares, A. (Ainhoa)|||/items/c4e9a238-1f8f-4845-ac0a-c63d82373414, Merino, N. (Nekane)|||/items/05098be7-e4a2-4bc7-ad2e-5af6daee371a, Tapia-Galisteo, A. (Alberto)|||/items/388eec7d-6be6-449c-a84c-2012e178678d, Cuesta, A.M. (Ángel M.)|||/items/b6f72fb1-3eb3-42dd-a183-48f7046a50c1, Mikkelsen, K. (Kasper)|||/items/47f850d8-62de-4879-87b8-ebaab06cf178, Caleiras, E. (Eduardo)|||/items/a50fa3bb-6348-4b3b-996d-a6bb73dcdd8c, Núñez-Prado, N. (Natalia)|||/items/b9208457-51e8-4402-9572-dd90c3532229, Aznar, M.A. (María Ángela)|||/items/8a93c205-a638-4589-8774-64166348f62c, Lykkemark, S. (Simon)|||/items/bbd62872-ae31-41ee-9711-f17a0d4511e6, Martínez-Torrecuadrada, J. (Jorge)|||/items/3b75da7b-d237-4fb4-8b89-18bf2ecd3d13, Melero, I. (Ignacio)|||/items/82113ea8-7ce1-49d5-9ee3-42cf20db1c4e, Blanco, F.J. (Francisco J.)|||/items/07383702-ffda-4145-915a-262a82d5cbd9, Serna, J.B. (Jorge Bernardino) de la|||/items/5a0de908-0d03-43ec-b86c-4be1345b3a44, Zapata, J.M. (Juan M.)|||/items/190da49d-edea-4c11-b83d-1fe615cff305, Sanz, L. (Laura)|||/items/4e0eb12b-c3e6-4132-baa9-cac2ed42a7ab, Álvarez-Vallina, L. (Luis)|||/items/6151cce7-7e07-45ee-970e-e35ca2156a90
Tipo de recurso: artículo
Fecha de publicación:2018
País:España
Institución:Universidad de Navarra
Repositorio:Dadun. Depósito Académico Digital de la Universidad de Navarra
Idioma:inglés
OAI Identifier:oai:dadun.unav.edu:10171/56004
Acceso en línea:https://hdl.handle.net/10171/56004
Access Level:acceso abierto
Palabra clave:4-1bb costimulation
Monoclonal-antibodies
In-vivo
Anti-cd137 mab
T-cells
Cancer
Immunotherapy
Cd137
Stimulation
Induction
Descripción
Sumario: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 Fc gamma R interactions. Here, we have designed an Fc-free tumor-targeted 4-1BB-agonistic trimerbody, 1D8(N)/(C)EGa1, 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. The1D8(N)/(C)EGa1 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 1D8(N)/(C)EGa1 does not induce systemic inflammatory cytokine production or hepatotoxicity associated with IgG-based 4-1BB agonists. These results implicate Fc gamma R 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.