Christopher A. Beaudoin* and Tom L. Blundell
Antibodies are an essential component of the adaptive immune system that function to neutralize foreign invaders, such as bacterial and parasitic pathogens. However, B-cell epitopes remain difficult to predict due to their general indistinguishability from other protein regions. Epitope prediction tools in the past have largely relied on amino acid sequence similarity; however, implementing three-dimensional protein structure analyses into the epitope prediction algorithms has been shown to increase detection accuracy. Furthermore, structural comparisons between antigenic proteins for their potential to bind cross-reactive antibodies have not been explored extensively in the literature. Recent studies have pointed to the utility of looking at shared epitope structures in predicting antibody crossreactivity, which may shed light on cross-immunity between infectious pathogens and autoimmune diseases induced after infection. Thus, herein, the potential impact of including structural similarity comparisons in detecting shared epitopes is discussed. With the large amount of structural information being determined by three-dimensional computational protein modelling methods, the ability to perform these analyses is becoming more feasible.
Published Date: 2021-09-10; Received Date: 2021-08-20