Abstract:The interactions of Toll‐like receptor 4 (TLR4) with competitive inhibitors were investigated by a combined ligand‐based and target‐based approach. Firstly, the ligand‐based pharmacophore model of the reported TLR4 inhibitors was constructed by utilizing the common feature method, which included three hydrophobic groups and a hydrogen bond receptor. The Schrödinger software suite glide module was used to dock inhibitors with proteins and verify the importance of these four interaction points from the target le… Show more
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