Analysis of affinities of penicillins for a class C beta-lactamase by molecular dynamics simulations.

Drug design and discovery Pub Date : 1999-08-01
K Tsuchida, N Yamaotsu, S Hirono
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Abstract

We present a calculation for the binding free energy difference between two complexes of the class C beta-lactamase from Enterobacter cloacae with foramidocillin (FOPC) and with piperacillin (PIPC). The calculation was carried out by means of the thermodynamic integration (TI) method implemented with molecular dynamics (MD). By use of the available crystal structure of the class C beta-lactamase from E. cloacae, the structures of the beta-lactamase-FOPC (FOPC complex) and beta-lactamase-PIPC (PIPC complex) complexes were built by molecular modeling and equilibrated with MD simulations. FOPC were gradually converted into PIPC in both the solution and the enzyme system by means of MD/TI methods during the MD simulation. The structure of the PIPC complex as derived by the MD/TI simulation was similar to that of the PIPC complex obtained from molecular modeling. The calculated difference in the free energy of binding (deltadeltaGbind) was -2.2 kcal/mol. This compares well with the experimental value of -1.5 kcal/mol. The results indicate that the binding affinity of FOPC is lower than that of PIPC because of the greater difficulty of desolvation for FOPC upon binding to the enzyme. This calculation suggests that the desolvation of the ligand, as well as its interaction with the beta-lactamase, is important in understanding the relative affinity of the ligands with beta-lactamase.

用分子动力学模拟分析青霉素对C类β -内酰胺酶的亲和力。
我们计算了阴沟肠杆菌C类β -内酰胺酶与foramidocillin (FOPC)和哌拉西林(PIPC)两种配合物的结合自由能差。计算采用分子动力学的热力学积分法(TI)进行。利用阴沟肠杆菌C类β -内酰胺酶的晶体结构,通过分子模拟构建了β -内酰胺酶-FOPC (FOPC配合物)和β -内酰胺酶-PIPC (PIPC配合物)配合物的结构,并用MD模拟进行了平衡。在MD模拟过程中,通过MD/TI方法,FOPC在溶液和酶体系中逐渐转化为PIPC。通过MD/TI模拟得到的PIPC配合物的结构与分子模拟得到的PIPC配合物的结构相似。结合自由能(deltadeltaGbind)的计算差值为-2.2 kcal/mol。这与-1.5千卡/摩尔的实验值相当。结果表明,FOPC的结合亲和力比PIPC低,因为FOPC与酶结合后更难解离。这一计算表明,配体的脱溶及其与β -内酰胺酶的相互作用对于理解配体与β -内酰胺酶的相对亲和力是重要的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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