Structural changes by sulfoxidation of phenothiazine drugs |
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| Authors: | Svein G Dahl Peter A Kollman Shashidhar N Rao U Chandra Singh |
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| Institution: | (1) Department of Pharmacology, Institute of Medical Biology, University of Tromsø, N-9001 Tromsø, Norway;(2) Department of Pharmaceutical Chemistry, University of California, 94143 San Francisco, CA, U.S.A.;(3) Present address: Drug Design, Searle Research and Development, 4901 Searle Parkway, 60077 Skokie, IL, U.S.A. |
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| Abstract: | Summary The side-chain conformations of psychoactive phenothiazine drugs in crystals are different from those of biologically inactive ring sulfoxide metabolites. This study examines the potential energies, molecular conformations and electrostatic potentials in chlorpromazine, levomepromazine (methotrimeprazine), their sulfoxide metabolites and methoxypromazine. The purpose of the study was to examine the significance of the different crystal conformations of active and inactive phenothiazine derivatives, and to determine why phenothiazine drugs lose most of their biological activity by sulfoxidation. Quantum mechanics and molecular mechanics calculations demonstrated that conformations with the side chain folded over the ring structure had lowest potential energy in vacuo, both in the drugs and in the sulfoxide metabolites. In the sulfoxides, side chain conformations corresponding to the crystal structure of chlorpromazine sulfoxide were characterized by stronger negative electrostatic potentials around the ring system than in the parent drugs. This may weaken the electrostatic interaction of sulfoxide metabolites with negatively charged domains in dopamine receptors, and cause the sulfoxides to be virtually inactive in dopamine receptor binding and related pharmacological tests. |
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| Keywords: | Chlorpromazine Levomepromazine Sulfoxide metabolites Molecular structure Conformation |
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