Caflisch A, Miranker A, Karplus M
Department of Chemistry, Harvard University, Cambridge, Massachusetts 02138.
J Med Chem. 1993 Jul 23;36(15):2142-67. doi: 10.1021/jm00067a013.
Rational ligand design is a complex problem that can be divided into three parts: the search for optimal positions and orientations of functional groups in the binding site, the connection of such positions to form candidate ligands, and the estimation of their binding constants. Approaches for addressing the first two parts of the problem are described in the present work. They are applied to the construction of peptide ligands in the binding site of the human immunodeficiency virus 1 (HIV-1) proteinase. The primary objective is to test the method by comparison of the results with the MVT-101 complex structure for which coordinates are available; the results obtained with the liganded and unliganded proteinase structure are used to examine the utility of the latter for binding studies. A secondary objective is to show how to find new inhibitor candidates. The multiple copy simultaneous search (MCSS) method is utilized to search for optimal positions and orientations of a set of functional groups. For peptide ligands, functional groups corresponding to the protein main chain (N-methylacetamide) and to protein side chains (e.g., methanol, ethyl guanidinium) are used. The resulting N-methylacetamide minima are connected to form hexapeptide main chains with a simple pseudoenergy function that permits a complete search of all possible ways of connecting the minima. Side chains are added to the main-chain candidates by application of the same pseudoenergy function to the appropriate functional group minima. A set of 15 hexapeptides with the sequence of MVT-101 is then minimized by a Monte Carlo scheme, which allows for escape from local minima. Comparison of the MCSS results with the structure of MVT-101 in the HIV-1 binding site showed that all of its functional group positions correspond (within 2.4 A) to some (usually more than one) MCSS minima. There were also many other low-energy MCSS minima which do not appear in any known inhibitors, e.g., methyl ammonium minima in the neighborhood of the catalytic aspartates. Among the 15 lowest minima are seven hexapeptides with the same main-chain orientation as the one found by X-ray crystallography for the inhibitor MVT-101 in the binding site and eight with the main chain oriented in the opposite direction; the latter tend to be more stable. [Addendum: These results are in agreement with recent high-resolution crystallographic data provided after the study was completed.(ABSTRACT TRUNCATED AT 400 WORDS)
合理的配体设计是一个复杂的问题,可分为三个部分:寻找结合位点中官能团的最佳位置和取向、连接这些位置以形成候选配体以及估计它们的结合常数。本文描述了解决该问题前两部分的方法。这些方法应用于构建人类免疫缺陷病毒1(HIV-1)蛋白酶结合位点中的肽配体。主要目的是通过将结果与可获得坐标的MVT-101复合物结构进行比较来测试该方法;使用结合配体和未结合配体的蛋白酶结构获得的结果来检验后者在结合研究中的效用。第二个目的是展示如何找到新的抑制剂候选物。利用多重复制同时搜索(MCSS)方法来搜索一组官能团的最佳位置和取向。对于肽配体,使用与蛋白质主链(N-甲基乙酰胺)和蛋白质侧链(例如甲醇、乙基胍)相对应的官能团。通过一个简单的伪能量函数将得到的N-甲基乙酰胺极小值连接起来,形成六肽主链,该函数允许对连接极小值的所有可能方式进行全面搜索。通过将相同的伪能量函数应用于适当的官能团极小值,将侧链添加到主链候选物上。然后通过蒙特卡罗方案对一组15个具有MVT-101序列的六肽进行最小化,该方案允许逃离局部极小值。将MCSS结果与HIV-1结合位点中MVT-101的结构进行比较表明,其所有官能团位置(在2.4埃范围内)与一些(通常不止一个)MCSS极小值相对应。也有许多其他低能量的MCSS极小值未出现在任何已知抑制剂中,例如催化天冬氨酸附近的甲基铵极小值。在15个最低极小值中,有7个六肽的主链取向与通过X射线晶体学在结合位点发现的抑制剂MVT-101相同,8个主链取向相反;后者往往更稳定。[附录:这些结果与研究完成后提供的最新高分辨率晶体学数据一致。(摘要截断于400字)
