Modeling Steroid 5alpha-reductase and Characterizing Its Potential Active Sites

Modeling Steroid 5alpha-reductase and Characterizing Its Potential Active Sites

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摘要 Steroid 5alpha-reductase of human is an enzyme in the biosynthetic pathway from testosterone （T） to dihydrotestosterone （DHT）. Up to now, no crystal structure of this enzyme has been reported. However, knowledge of the tertiary structure and possible active sites is essential for understanding the catalysis mechanism and for the design of inhibitors. A model with putative active sites has been created and evaluated by using homology modeling and molecular docking techniques based on the bioinformatics knowledge. The homology model is optimized in Swiss PDB Viewer with MM method and substrate structures before docking are also optimized on HF/6-31G. The active site for the docking of NADP, T, DHT and Finasteride is located near the N-terminus of enzyme. Four active amino acids in the active site are identified as Ala26, Arg53, Arg176 and Lys177. Reaction procedure, binding pattern of active sites, the types of weak interaction and so on are also discussed. Steroid 5alpha-reductase of human is an enzyme in the biosynthetic pathway from testosterone （T） to dihydrotestosterone （DHT）. Up to now, no crystal structure of this enzyme has been reported. However, knowledge of the tertiary structure and possible active sites is essential for understanding the catalysis mechanism and for the design of inhibitors. A model with putative active sites has been created and evaluated by using homology modeling and molecular docking techniques based on the bioinformatics knowledge. The homology model is optimized in Swiss PDB Viewer with MM method and substrate structures before docking are also optimized on HF/6-31G. The active site for the docking of NADP, T, DHT and Finasteride is located near the N-terminus of enzyme. Four active amino acids in the active site are identified as Ala26, Arg53, Arg176 and Lys177. Reaction procedure, binding pattern of active sites, the types of weak interaction and so on are also discussed.

作者欧敏锐李俊篯

机构地区 College of Chemistry and Chemical Engineering

出处《Chinese Journal of Structural Chemistry》 SCIE CAS CSCD 2012年第11期1618-1626,共9页 结构化学（英文）

基金 Supported by the National Natural Science Foundation of China(No.21073034) the State Key Laboratory of Structural Chemistry(No.20090060) the Natural Science Foundation of Fujian Province(X0650070) the Science and Technology Development Foundation of Fuzhou University(2010-XY-9)

关键词 5aipha-reductase homology modeling benign prostatic hyperplasia 5aipha-reductase, homology modeling, benign prostatic hyperplasia

分类号 O629.8 [理学—有机化学]

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Chinese Journal of Structural Chemistry

2012年第11期

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Modeling Steroid 5alpha-reductase and Characterizing Its Potential Active Sites

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