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Chiral‐Substrate‐Assisted Stereoselective Epoxidation Catalyzed by H2O2‐Dependent Cytochrome P450SPα |
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| Authors: | Dr. Takashi Fujishiro Dr. Osami Shoji Dr. Norifumi Kawakami Takahiro Watanabe Dr. Hiroshi Sugimoto Dr. Yoshitsugu Shiro Prof. Dr. Yoshihito Watanabe |
| Affiliation: | 1. Department of Chemistry, Graduate School of Science, Nagoya University, Furo‐cho, Chikusa‐ku, Nagoya 464‐8602 (Japan), Fax: (+81)?52‐789‐3557;2. RIKEN SPring‐8 Center Harima Institute, 1‐1‐1 Kouto, Mikazuki‐cho, Sayo, Hyogo 679‐5148 (Japan);3. Research Center for Materials Science, Nagoya University, Furo‐cho, Chikusa‐ku, Nagoya 464‐8602 (Japan) |
| Abstract: | The stereoselective epoxidation of styrene was catalyzed by H2O2‐dependent cytochrome P450SPα in the presence of carboxylic acids as decoy molecules. The stereoselectivity of styrene oxide could be altered by the nature of the decoy molecules. In particular, the chirality at the α‐positions of the decoy molecules induced a clear difference in the chirality of the product: (R)‐ibuprofen enhanced the formation of (S)‐styrene oxide, whereas (S)‐ibuprofen preferentially afforded (R)‐styrene oxide. The crystal structure of an (R)‐ibuprofen‐bound cytochrome P450SPα (resolution 1.9 Å) revealed that the carboxylate group of (R)‐ibuprofen served as an acid–base catalyst to initiate the epoxidation. A docking simulation of the binding of styrene in the active site of the (R)‐ibuprofen‐bound form suggested that the orientation of the vinyl group of styrene in the active site agreed with the formation of (S)‐styrene oxide. |
| Keywords: | carboxylic acids chirality decoy molecules epoxidation hydrogen peroxide |