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The anti-tumor efficacy of 3C23K, a glyco-engineered humanized anti-MISRII antibody, in an ovarian cancer model is mainly mediated by engagement of immune effector cells.

Research Paper. 2017-06; 
Pauline Estupina,,,, Alexandre Fontayne, Jean-Marc Barret, Nathalie Kersual,,,, Olivier Dubreuil, Marion Le Blay,,,, Alexandre Pichard,,,, Marta Jarlier, Martine Pugnière,,,, Maëva Chauvin,,,, Thierry Chardès,,,, JeanPierre Pouget,,,, Emmanuel Deshayes, Alexis Rossignol, Toufik Abache, Christophe de Romeuf, Aurélie Terrier, Lucie Verhaeghe, Christine Gaucher, Jean-François Prost, André Pèlegrin,,,,*, Isabelle Navarro-Teulon,,,,*
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摘要

Ovarian cancer is the leading cause of death in women with gynecological cancers and despite recent advances, new and more efficient therapies are crucially needed. Müllerian Inhibiting Substance type II Receptor (MISRII, also named AMHRII) is expressed in most ovarian cancer subtypes and is a novel potential target for ovarian cancer immunotherapy. We previously developed and tested 12G4, the first murine monoclonal antibody (MAb) against human MISRII. Here, we report the humanization, affinity maturation and glyco-engineering steps of 12G4 to generate the Fc-optimized 3C23K MAb, and the evaluation of its in vivo anti-tumor activity. The epitopes of 3C23K and 12G4 were strictly identical and 3C23K affinity fo... More

关键词

immunotherapy, therapeutic antibody, ovarian cancer, GCT, MISRII