Author: Bournazos, Stylianos; Corti, Davide; Virgin, Herbert W.; Ravetch, Jeffrey V.
                    Title: Fc-optimized antibodies elicit CD8 immunity to viral respiratory infection  Cord-id: ybxz74a4  Document date: 2020_10_8
                    ID: ybxz74a4
                    
                    Snippet: Antibodies against viral pathogens represent promising therapeutic agents for the control of infection, and their antiviral efficacy has been shown to require the coordinated function of both the Fab and Fc domains(1). The Fc domain engages a wide spectrum of receptors on discrete cells of the immune system to trigger the clearance of viruses and subsequent killing of infected cells(1–4). Here we report that Fc engineering of anti-influenza IgG monoclonal antibodies for selective binding to th
                    
                    
                    
                     
                    
                    
                    
                    
                        
                            
                                Document: Antibodies against viral pathogens represent promising therapeutic agents for the control of infection, and their antiviral efficacy has been shown to require the coordinated function of both the Fab and Fc domains(1). The Fc domain engages a wide spectrum of receptors on discrete cells of the immune system to trigger the clearance of viruses and subsequent killing of infected cells(1–4). Here we report that Fc engineering of anti-influenza IgG monoclonal antibodies for selective binding to the activating Fcγ receptor FcγRIIa results in enhanced ability to prevent or treat lethal viral respiratory infection in mice, with increased maturation of dendritic cells and the induction of protective CD8(+) T cell responses. These findings highlight the capacity for IgG antibodies to induce protective adaptive immunity to viral infection when they selectively activate a dendritic cell and T cell pathway, with important implications for the development of therapeutic antibodies with improved antiviral efficacy against viral respiratory pathogens.
 
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