Structure of the human histamine H1 receptor complex with doxepin

Abstract

The biogenic amine histamine is an important pharmacological mediator involved in pathophysiological processes such as allergies and inflammations. Histamine H₁ receptor (H₁R) antagonists are very effective drugs alleviating the symptoms of allergic reactions. Here we show the crystal structure of the H₁R complex with doxepin, a first-generation H₁R antagonist. Doxepin sits deep in the ligand-binding pocket and directly interacts with Trp 428^6.48, a highly conserved key residue in G-protein-coupled-receptor activation. This well-conserved pocket with mostly hydrophobic nature contributes to the low selectivity of the first-generation compounds. The pocket is associated with an anion-binding region occupied by a phosphate ion. Docking of various second-generation H₁R antagonists reveals that the unique carboxyl group present in this class of compounds interacts with Lys 191^5.39 and/or Lys 179^ECL2, both of which form part of the anion-binding region. This region is not conserved in other aminergic receptors, demonstrating how minor differences in receptors lead to pronounced selectivity differences with small molecules. Our study sheds light on the molecular basis of H₁R antagonist specificity against H₁R.