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Molecular Modeling of Cytochrome P450 2B1: Mode of Membrane Insertion and Substrate Specificity
Authors:Renke Dai  Matthew R Pincus and Fred K Friedman
Institution:(1) Laboratory of Molecular Carcinogenesis, National Cancer Institute, Bethesda, Maryland, 20892;(2) Department of Pathology & Laboratory Medicine, Veterans Administration Medical Center, Brooklyn, New York 11209, and Department of Pathology, SUNY Health Science Center, New York, 11239
Abstract:A molecular model of a mammalian membrane-bound cytochrome P450, rat P450 2B1, was constructed in order to elucidate its mode of attachment to the endoplasmic reticulum and the structural basis of substrate specificity. The model was primarily derived from the structure of P450BM-3, which as a class II P450 is the most functionally similar P450 of known structure. However, model development was also guided by the conserved core regions of P450cam and P450terp. To optimally align the P450 2B1 and P450BM-3 sequences, multiple alignment was performed using sequences of five P450s in the II family, followed by minor adjustments on the basis of secondary structure predictions. The resulting P450 2B1 homology model structure was refined by molecular dynamics heating, equilibration, simulation, and energy minimization. The model suggests that the F–G loop serves as both a hydrophobic membrane anchor and entrance channel for hydrophobic substrates from the membrane to the P450 active site. To assess the mode of substrate binding, benzphetamine, testosterone, and benzoa]pyrene were docked into the active site. The hydrophobic substrate-binding pocket is consistent with the preferences of this P450 toward hydrophobic substrates, while the presence of an acidic Glu-105 in this pocket is consistent with the preference of this P450 for the cationic substrate benzphetamine. This model is thus consistent with several known experimental properties of this P450, such as membrane attachment and substrate selectivity.
Keywords:Cytochrome P450  molecular modeling  membrane  substrate specificity
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