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Dual epitope targeting and enhanced hexamerization by DR5 antibodies as a novel approach to induce potent antitumor activity through DR5 agonism
Weak fragment crystallizable (Fc) domain interactions drive the dynamic assembly of IgG oligomers upon antigen recognition
CD20 and CD37 antibodies synergize to activate complement by Fc-mediated clustering
Structures of C1-IgG1 provide insights into how danger pattern recognition activates complement
Structures of C1-IgG1 provide insights into how danger pattern recognition activates complement
Human IgG is produced in a pro-form that requires clipping of C-terminal lysines for maximal complement activation