Design, synthesis, and docking studies of novel benzopyrone derivatives as H(1)-antihistaminic agents.

Two new series of 2H-1-benzopyran-2-one derivatives substituted at C-6 and/or C-7 with propanolamines, and/or piperazine propanol derivatives have been synthesized and assayed for the H(1)-histamine antagonist. Twelve of the 20 newly synthesized 4- substituted benzopyrones have shown potent antihistaminic H(1) activity. In addition, molecular modeling and docking of the tested compounds into high affinity histamine binding protein (HBP) and histamine N-methyltranseferase (HNMT) active site in complex with its bound inhibitor (diphenhydramine) was performed in order to predict the affinity and orientation of these compounds at the active sites. The ICM score values show good agreement with predicted binding affinities obtained by molecular docking studies as verified by pharmacological screening. The results showed similar orientation of the target compounds at HBP, and HNMT active sites compared with reported histamine H(1) antagonist. Also, it was concluded that in order for the compounds to be active, they must bind with both active sites of HNMT enzyme (two pockets) to inhibit it. Compounds 8c, 8i, 11g, 11i, and 11k; observe the maximum activities.

[1]  T. B. Lee,et al.  Antagonists of slow reacting substance of anaphylaxis. Synthesis of a series of chromone-2-carboxylic acids. , 1977, Journal of medicinal chemistry.

[2]  D. Buckle,et al.  N-benzylpiperazino derivatives of 3-nitro-4-hydroxycoumarin with H1 antihistamine and mast cell stabilizing properties. , 1984, Journal of medicinal chemistry.

[3]  J. Shire Growth Hormone and Premature Ageing , 1973, Nature.

[4]  S. Snyder,et al.  Histamine methyltransferase: inhibition and potentiation by antihistamines. , 1972, Molecular pharmacology.

[5]  R. Smith,et al.  Aryloxyalkyloxy- and aralkyloxy-4-hydroxy-3-nitrocoumarins which inhibit histamine release in the rat and also antagonize the effects of a slow reacting substance of anaphylaxis. , 1979, Journal of medicinal chemistry.

[6]  Claudio N. Cavasotto,et al.  Protein flexibility in ligand docking and virtual screening to protein kinases. , 2004, Journal of molecular biology.

[7]  A. Coleoni Effects of the administration of catecholamine-depleting drugs on the thyroid function of the rat. , 1972, Pharmacology.

[8]  A Anderson,et al.  VRDD: applying virtual reality visualization to protein docking and design. , 1999, Journal of molecular graphics & modelling.

[9]  P. Prathipati,et al.  Synthesis of some substituted pyrazinopyridoindoles and 3D QSAR studies along with related compounds: piperazines, piperidines, pyrazinoisoquinolines, and diphenhydramine, and its semi-rigid analogs as antihistamines (H1). , 2006, Bioorganic & medicinal chemistry.

[10]  Ruth Nussinov,et al.  Principles of docking: An overview of search algorithms and a guide to scoring functions , 2002, Proteins.

[11]  D. Henry,et al.  Histamine N -Methyltransferase , 1986 .

[12]  D. Buckle,et al.  Antiallergic activity of 4-hydroxy-3-nitrocoumarins. , 1975, Journal of medicinal chemistry.

[13]  S. Sultana,et al.  Inhibition of two stage renal carcinogenesis, oxidative damage and hyperproliferative response by Nigella sativa , 2005, European journal of cancer prevention : the official journal of the European Cancer Prevention Organisation.

[14]  M. Nishibori,et al.  Two polymorphic forms of human histamine methyltransferase: structural, thermal, and kinetic comparisons. , 2001, Structure.

[15]  Xiaodong Cheng,et al.  Structural basis for inhibition of histamine N-methyltransferase by diverse drugs. , 2005, Journal of molecular biology.

[16]  D I Stuart,et al.  Tick histamine-binding proteins: isolation, cloning, and three-dimensional structure. , 1999, Molecular cell.

[17]  R. Kroemer Molecular modelling probes: docking and scoring. , 2003, Biochemical Society transactions.

[18]  Holger Stark,et al.  Development of a new class of nonimidazole histamine H(3) receptor ligands with combined inhibitory histamine N-methyltransferase activity. , 2002, Journal of medicinal chemistry.