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Antitumor efficacy and reduced toxicity using an anti-CD137 Probody therapeutic

Autores: Etxeberria Uriz, Iñaki; Bolaños Mateo, Elixabet; Teijeira Sánchez, Álvaro; Garasa, S.; Yanguas Andrés, Alba; Azpilicueta Lusarreta, Arantza; Kavanaugh, W. M.; Vasiljeva, O.; Belvin, M.; Howng, B.; Irving, B.; Tipton, K.; West, J.; Mei, L.; Korman, A. J.; Sega, E.; Olivera, I.; Cirella, A.; Ochoa Nieto, Maria del Carmen; Rodríguez Ruiz, María Esperanza; Melero, A.; Fernández de Sanmamed Gutiérrez, Miguel; Engelhardt, J. J.; Melero Bermejo, Ignacio (Autor de correspondencia)
Título de la revista: PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
ISSN: 0027-8424
Volumen: 118
Número: 26
Páginas: e2025930118
Fecha de publicación: 2021
Resumen:
Costimulation via CD137 (4-1BB) enhances antitumor immunity mediated by cytotoxic T lymphocytes. Anti-CD137 agonist antibodies elicit mild liver inflammation in mice, and the maximum tolerated dose of Urelumab, an anti-human CD137 agonist monoclonal antibody, in the clinic was defined by liver inflammation-related side effects. A protease-activated prodrug form of the anti-mouse CD137 agonist antibody 1D8 (1D8 Probody therapeutic, Pb-Tx) was constructed and found to be selectively activated in the tumor microenvironment. This construct, which encompasses a protease-cleavable linker holding in place a peptide that masks the antigen binding site, exerted antitumor effects comparable to the unmodified antibody but did not result in liver inflammation. Moreover, it efficaciously synergized with both PD-1 blockade and adoptive T-cell therapy. Surprisingly, minimal active Pb-Tx reached tumor-draining lymph nodes, and regional lymphadenectomy did not abrogate antitumor efficacy. By contrast, S1P receptor-dependent recirculation of T cells was absolutely required for efficacy. The preferential cleavage of the anti-CD137 Pb-Tx by tumor proteases offers multiple therapeutic opportunities, including neoadjuvant therapy, as shown by experiments in which the Pb-Tx is given prior to surgery to avoid spontaneous metastases.