Author: Rangel, Mauricio Aguilar; Bedwell, Alice; Costanzi, Elisa; Ricagno, Stefano; Frydman, Judith; Vendruscolo, Michele; Sormanni, Pietro
                    Title: Fragment-based computational design of antibodies targeting structured epitopes  Cord-id: sl6bxf9j  Document date: 2021_3_2
                    ID: sl6bxf9j
                    
                    Snippet: De novo design methods hold the promise of reducing the time and cost of antibody discovery, while enabling the facile and precise targeting of specific epitopes. Here we describe a fragment-based method for the combinatorial design of antibody binding loops and their grafting onto antibody scaffolds. We designed and tested six single-domain antibodies targeting different epitopes on three antigens, including the receptor-binding domain of the SARS-CoV-2 spike protein. Biophysical characterisati
                    
                    
                    
                     
                    
                    
                    
                    
                        
                            
                                Document: De novo design methods hold the promise of reducing the time and cost of antibody discovery, while enabling the facile and precise targeting of specific epitopes. Here we describe a fragment-based method for the combinatorial design of antibody binding loops and their grafting onto antibody scaffolds. We designed and tested six single-domain antibodies targeting different epitopes on three antigens, including the receptor-binding domain of the SARS-CoV-2 spike protein. Biophysical characterisation showed that all designs are highly stable, and bind their intended targets with affinities in the nanomolar range without any in vitro affinity maturation. We further show that a high-resolution input antigen structure is not required, as our method yields similar predictions when the input is a crystal structure or a computer-generated model. This computational procedure, which readily runs on a laptop, provides the starting point for the rapid generation of lead antibodies binding to pre-selected epitopes.
 
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