Role of IgE-VH in FcεRIα and superantigen binding in allergy and immunotherapy

Abstract Background VH family frameworks have been reported to affect antibody receptor and superantigen binding, however such effects in IgE remains largely unknown. Given that VH family biases have been previously reported in IgE of certain allergies, there is a need to investigate this phenomenon for biotechnological and therapeutic purposes. Objective We sought to investigate the effects of VH families on IgE interaction with FceRIα, anti-IgE Omalizumab, antigen, and superantigen spA using the Pertuzumab and Trastuzumab IgE models. Methods Pertuzumab VH1–VH7 family variants of IgE with the same CDRs were investigated with regards to their binding interactions to FceRIα, Her2, Omalizumab, and spA. Notable FceRIα-IgE observations were cross-checked against appropriate Trastuzumab IgE VH variants. Computational structural modeling and simulations were also performed for insights into the mechanism of interactions with various VH FWRs. Results The Pertuzumab VH5 IgE variant but not the Trastuzumab VH5 IgE was found to interact with FceRIα significantly longer than the respective VH family variants within each model antibody. No significant differences in interaction were found between IgE and Omalizumab for the Pertuzumab VH variants. Although Trastuzumab VH3 interacted with spA, all our Pertuzumab VH variants including VH3 did not associate with spA. Conclusion We found unexpected varying allosteric communications caused by the VH family frameworks to the FceRIα, Her2, and spA binding regions of Pertuzumab IgE, with implications on the use of IgE/anti-IgE therapeutics to treat allergy and IgE therapeutics in allergooncology.