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Merck

Efficient tumor killing and minimal cytokine release with novel T-cell agonist bispecific antibodies.

mAbs (2019-01-31)
Nathan D Trinklein, Duy Pham, Ute Schellenberger, Ben Buelow, Andrew Boudreau, Priya Choudhry, Starlynn C Clarke, Kevin Dang, Katherine E Harris, Suhasini Iyer, Brett Jorgensen, Payal P Pratap, Udaya S Rangaswamy, Harshad S Ugamraj, Omid Vafa, Arun P Wiita, Wim van Schooten, Roland Buelow, Shelley Force Aldred
RÉSUMÉ

T-cell-recruiting bispecific antibodies (T-BsAbs) have shown potent tumor killing activity in humans, but cytokine release-related toxicities have affected their clinical utility. The use of novel anti-CD3 binding domains with more favorable properties could aid in the creation of T-BsAbs with improved therapeutic windows. Using a sequence-based discovery platform, we identified new anti-CD3 antibodies from humanized rats that bind to multiple epitopes and elicit varying levels of T-cell activation. In T-BsAb format, 12 different anti-CD3 arms induce equivalent levels of tumor cell lysis by primary T-cells, but potency varies by a thousand-fold. Our lead CD3-targeting arm stimulates very low levels of cytokine release, but drives robust tumor antigen-specific killing in vitro and in a mouse xenograft model. This new CD3-targeting antibody underpins a next-generation T-BsAb platform in which potent cytotoxicity is uncoupled from high levels of cytokine release, which may lead to a wider therapeutic window in the clinic.