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• W3048900135 abstract "Herpes virus entry mediator (HVEM) regulates positive and negative signals for T cell activation through co-signaling pathways. Dysfunction of the HVEM co-signaling network is associated with multiple pathologies related to autoimmunity, infectious disease, and cancer, making the associated molecules biologically and therapeutically attractive targets. HVEM interacts with three ligands from two different superfamilies using two different binding interfaces. The engagement with ligands CD160 and B- and T-lymphocyte attenuator (BTLA), members of immunoglobulin superfamily, is associated with inhibitory signals, whereas inflammatory responses are regulated through the interaction with LIGHT from the TNF superfamily. We computationally redesigned the HVEM recognition interfaces using a residue-specific pharmacophore approach, ProtLID, to achieve switchable-binding specificity. In subsequent cell-based binding assays the new interfaces, designed with only single or double mutations, exhibited selective binding to only one or two out of the three cognate ligands." @default.
• W3048900135 created "2020-08-18" @default.
• W3048900135 creator A5006013523 @default.
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• W3048900135 date "2020-11-01" @default.
• W3048900135 modified "2023-10-16" @default.
• W3048900135 title "Redesigning HVEM Interface for Selective Binding to LIGHT, BTLA, and CD160" @default.
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• W3048900135 doi "https://doi.org/10.1016/j.str.2020.07.013" @default.
• W3048900135 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/7642093" @default.
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• W3048900135 hasPublicationYear "2020" @default.
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