Domain binding and isotype dictate the activity of anti-human OX40 antibodies.
Jordana GriffithsKhiyam HussainHannah L SmithTheodore SandersKerry L CoxMonika SemmrichLinda MårtenssonJinny KimTatyana InzhelevskayaChris A PenfoldAlison L TuttC Ian MockridgeHt Claude ChanVikki EnglishRuth F FrenchIngrid TeigeAymen Al-ShamkhaniMartin J GlennieBjorn L FrendeusJane E WilloughbyMark S CraggPublished in: Journal for immunotherapy of cancer (2021)
These findings highlight the significant impact of isotype and epitope on the modulation of anti-hOX40 mAb therapy, and indicate that CD8+ T-cell expansion or Treg depletion might be preferred according to the composition of different tumors. As many of the current clinical trials using OX40 antibodies are now using combination therapies, this understanding of how to manipulate therapeutic activity will be vital in directing new combinations that are more likely to improve efficacy and clinical outcomes.