De Rienzo F, Fanelli F, Menziani M C, De Benedetti P G
Dipartimento di Chimica, Università di Modena e Reggio Emilia, Italy.
J Comput Aided Mol Des. 2000 Jan;14(1):93-116. doi: 10.1023/a:1008187802746.
Three-dimensional models of the cytochromes P450 IA2, P450 IID6 and P450 IIIA4 were built by means of comparative modeling using the X-ray crystallographic structures of P450 CAM, P450 BM-3, P450 TERP and P450 ERYF as templates. The three cytochromes were analyzed both in their intrinsic structural features and in their interaction properties with fifty specific and non-specific substrates. Substrate/enzyme complexes were obtained by means of both automated rigid and flexible body docking. The comparative analysis of the three cytochromes and the selected substrates, in their free and bound forms, allowed for the building of semi-quantitative models of substrate specificity based on both molecular and intermolecular interaction descriptors. The results of this study provide new insights into the molecular determinants of substrate specificity for the three different eukaryotic P450 isozymes and constitute a useful tool for predicting the specificity of new compounds.
以细胞色素P450 CAM、P450 BM - 3、P450 TERP和P450 ERYF的X射线晶体结构为模板,通过比较建模构建了细胞色素P450 IA2、P450 IID6和P450 IIIA4的三维模型。对这三种细胞色素的内在结构特征以及它们与五十种特异性和非特异性底物的相互作用特性进行了分析。通过自动刚性和柔性对接获得了底物/酶复合物。对这三种细胞色素以及所选底物的游离和结合形式进行比较分析,基于分子和分子间相互作用描述符建立了底物特异性的半定量模型。本研究结果为三种不同真核生物P450同工酶底物特异性的分子决定因素提供了新的见解,并构成了预测新化合物特异性的有用工具。