| Literature DB >> 32761423 |
Yan Wang1,2,3, Haiqing Ni4, Shuaixiang Zhou4, Kaijie He4, Yarong Gao4, Weiwei Wu4, Min Wu4, Zhihai Wu4, Xuan Qiu4, Ying Zhou4, Bingliang Chen4, Donghui Pan2, Chenrong Huang1,3, Mingzhu Li2, Yicong Bian1,3, Min Yang5, Liyan Miao6,7, Junjian Liu8.
Abstract
CD47, an immune checkpoint receptor frequently unregulated in various blood and solid tumors, interacts with ligand SIPRα on innate immune cells, and conveys a "do not eat me" signal to inhibit macrophage-mediated tumor phagocytosis. This makes CD47 a valuable target for cancer immunotherapy. However, the therapeutic utility of CD47-SIRPα blockade monoclonal antibodies is largely compromised due to significant red blood cell (RBCs) toxicities and fast target-mediated clearance as a result of extensive expression of CD47 on normal cells. To overcome these limitations and further improve therapeutic efficacy, we designed IBI322, a CD47/PD-L1 bispecific antibody which attenuated CD47 activity in monovalent binding and blocked PD-L1 activity in bivalent binding. IBI322 selectively bound to CD47+PD-L1+ tumor cells, effectively inhibited CD47-SIRPα signal and triggered strong tumor cell phagocytosis in vitro, but only with minimal impact on CD47 single positive cells such as human RBCs. In addition, as a dual blocker of innate and adaptive immune checkpoints, IBI322 effectively accumulated in PD-L1-positive tumors and demonstrated synergistic activity in inducing complete tumor regression in vivo. Furthermore, IBI322 showed only marginal RBCs depletion and was well tolerated in non-human primates (NHP) after repeated weekly injections, suggesting a sufficient therapeutic window in future clinical development of IBI322 for cancer treatment.Entities:
Keywords: Adaptive immunity; Bispecific antibody; IBI322; Immunotherapy; Innate immunity; Phagocytosis
Year: 2020 PMID: 32761423 DOI: 10.1007/s00262-020-02679-5
Source DB: PubMed Journal: Cancer Immunol Immunother ISSN: 0340-7004 Impact factor: 6.968