Bilastine, a zwitterionic second-generation antihistamine containing a carboxyl group, has higher selectivity for H receptors than first-generation antihistamines. Ligand-receptor docking simulations have suggested that the electrostatic interaction between the carboxyl group of second-generation antihistamines and the amino group of Lys179 and Lys191 of human H receptors might contribute to increased affinity of these antihistamines to H receptors. In this study, we evaluated the roles of Lys179 and Lys191 in regulating the electrostatic and hydrophobic binding of bilastine to H receptors by thermodynamic analyses. The binding enthalpy and entropy of bilastine were estimated from the van 't Hoff equation using the dissociation constants. These constants were obtained from the displacement curves against the binding of [H] mepyramine to membrane preparations of Chinese hamster ovary cells expressing wild-type human H receptors and their Lys179 or Lys191 mutants to alanine at various temperatures. We found that the binding of bilastine to wild-type H receptors occurred by enthalpy-dependent binding forces and, more dominantly, entropy-dependent binding forces. The mutation of Lys179 and Lys191 to alanine reduced the affinity of bilastine to H receptors by reducing enthalpy- and entropy-dependent binding forces, respectively. These results suggest that Lys179 and Lys191 differentially contribute to the increased binding affinity to bilastine via electrostatic and hydrophobic binding forces.
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Differential Regulation of Bilastine Affinity for Human Histamine H Receptors by Lys 179 and Lys 191 via Its Binding Enthalpy and Entropy.
Int J Mol Sci
February 2021
Department of Pharmacodynamics, Meiji Pharmaceutical University, 2-522-1 Noshio, Kiyose, Tokyo 204-8588, Japan.
Bilastine, a zwitterionic second-generation antihistamine containing a carboxyl group, has higher selectivity for H receptors than first-generation antihistamines. Ligand-receptor docking simulations have suggested that the electrostatic interaction between the carboxyl group of second-generation antihistamines and the amino group of Lys179 and Lys191 of human H receptors might contribute to increased affinity of these antihistamines to H receptors. In this study, we evaluated the roles of Lys179 and Lys191 in regulating the electrostatic and hydrophobic binding of bilastine to H receptors by thermodynamic analyses.
View Article and Find Full Text PDFRoles of Lys191 and Lys179 in regulating thermodynamic binding forces of ligands to determine their binding affinity for human histamine H receptors.
Biochem Pharmacol
October 2020
Department of Pharmacodynamics, Meiji Pharmaceutical University, 2-522-1 Kiyose, Tokyo 204-8588, Japan. Electronic address:
Docking simulations based on the crystal structure of human histamine H receptors have predicted crucial roles of Lys191 and Lys179, which exist at the entrance of the ligand-binding pocket, in increasing the H-receptor selectivity for carboxylated second-generation antihistamines via electrostatic interaction. In this study, we evaluated the roles of Lys191 and Lys179 in regulating the thermodynamic binding forces of non-carboxylated and carboxylated antihistamines that determine their binding affinity for human H receptors. The binding enthalpy and entropy of the 3 sets of non-carboxylated and corresponding carboxylated antihistamines (doxepin and olopatadine, desloratadine and loratadine, and terfenadine and fexofenadine, respectively) were estimated using the van't Hoff equation with the dissociation constants obtained from the displacement curves of the non-carboxylated and carboxylated antihistamines against the binding of [H]mepyramine to the membrane preparations of Chinese hamster ovary cells expressing human H receptors at various temperatures, ranging from 4 °C to 37 °C.
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Bioinformation
June 2013
Department of Pharmacology and Clinical Pharmacy, Faculty of Pharmacy, Universitas Gadjah Mada Yogyakarta Indonesia.
Unlabelled: The aim of this study is to determine the affinity of six active compounds of Aegle Marmelos Correa, they are (E, R)-Marmin, skimmianine, (S)-aegeline, aurapten, zeorin, and dustanin as antihistamines in histamine H1 receptor in comparison to cetirizin, diphenhydramine and chlorpheniramine as ligands comparison. Previously, in the in vitro study marmin obviously antagonized the histamine H1 receptor in a competitive manner.
Methods: molecular docking to determine the interaction of ligand binding to its receptor.
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