STEREOSELECTIVE INTERACTION OF AN AZOLE ANTIFUNGAL AGENT WITH ITS TARGET, LANOSTEROL 14-ALPHA-DEMETHYLASE (CYTOCHROME P-45014DM) - A MODEL STUDY WITH STEREOISOMERS OF TRIADIMENOL AND PURIFIED CYTOCHROME P-45014DM FROM YEAST

被引:38
作者
YOSHIDA, Y
AOYAMA, Y
机构
[1] Faculty of Pharmaceutical Sciences, Mukogawa Women's University, Nishinomiya
关键词
antifungal activity; diniconazole; hemoprotein; structure–function relationship; substrate‐binding site;
D O I
10.1002/chir.530020103
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
The effect of the four triadimenol stereoisomers on the purified yeast lanosterol 14α‐demethylase (cytochrome P‐45014DM), the primary target of azole antifungal agents, was studied. (1S,2R)‐Triadimenol was the most potent demethylase inhibitor and bound quantitatively to the enzyme below 0.05 μM. This isomer also interfered with the chemical reduction of cytochrome P‐45014DM and the binding of CO to the cytochrome. The other isomers showed a lower inhibitory effect on the enzyme, and the order of activity was (1R,2R) > (1R,2S) ≧ (1S,2S). Based on these findings and the reported preferred conformations for the triadimenol stereoisomers (Anderson, N.H. et al., Pestic. Sci. 15:310–316, 1984), it is predicted that orientation of the hydrophobic tert‐butyl and p‐chlorophenyl groups relative to the azole nitrogen is important to fit the antifungal agent in the active site of the demethylase. Copyright © 1990 Wiley‐Liss, Inc.
引用
收藏
页码:10 / 15
页数:6
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