Krämer Andreas, Horn Hans W, Rice Julia E
IBM Almaden Research Center, 650 Harry Road, San Jose, CA 95120, USA.
J Comput Aided Mol Des. 2003 Jan;17(1):13-38. doi: 10.1023/a:1024503712135.
We present a new method (fFLASH) for the virtual screening of compound databases that is based on explicit three-dimensional molecular superpositions. fFLASH takes the torsional flexibility of the database molecules fully into account, and can deal with an arbitrary number of conformation-dependent molecular features. The method utilizes a fragmentation-reassembly approach which allows for an efficient sampling of the conformational space. A fast clique-based pattern matching algorithm generates alignments of pairs of adjacent molecular fragments on the rigid query molecule that are subsequently reassembled to complete database molecules. Using conventional molecular features (hydrogen bond donors and acceptors, charges, and hydrophobic groups) we show that fFLASH is able to rapidly produce accurate alignments of medium-sized drug-like molecules. Experiments with a test database containing a diverse set of 1780 drug-like molecules (including all conformers) have shown that average query processing times of the order of 0.1 seconds per molecule can be achieved on a PC.
我们提出了一种基于显式三维分子叠加的用于化合物数据库虚拟筛选的新方法(fFLASH)。fFLASH充分考虑了数据库分子的扭转灵活性,并且能够处理任意数量的构象相关分子特征。该方法采用碎片重组方法,允许对构象空间进行高效采样。一种基于快速团的模式匹配算法生成刚性查询分子上相邻分子片段对的比对,随后将这些比对重新组合以完成数据库分子。使用常规分子特征(氢键供体和受体、电荷以及疏水基团),我们表明fFLASH能够快速生成中等大小类药物分子的准确比对。对包含1780个不同类药物分子(包括所有构象异构体)的测试数据库进行的实验表明,在个人电脑上每个分子的平均查询处理时间可达0.1秒左右。
