%0 Journal Article
%T 肿瘤蛋白MDMX与抑制剂PMI作用机制的分子动力学研究<br>Molecular Dynamics Insight into the Interaction Mechanism of Inhibitor PMI with MDMX
%A 程伟渊
%A 梁志强
%A 王伟
%A 伊长虹
%A 王克彦
%A 李洪云
%A 陈建中
%J Hans Journal of Computational Biology
%P 27-33
%@ 2164-5434
%D 2012
%I Hans Publishing
%R 10.12677/hjcb.2012.23003
%X <span style=\"font-family:宋体;font-size:10pt;\">恢复抑癌蛋白</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">p53</span><span style=\"font-family:宋体;font-size:10pt;\">的功能已经成为一种治疗癌症的新途径。本文采用分子动力学模拟和</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">MM-PBSA</span><span style=\"font-family:宋体;font-size:10pt;\">方法计算了抑制剂</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">PMI</span><span style=\"font-family:宋体;font-size:10pt;\">与肿瘤蛋白</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">MDMX</span><span style=\"font-family:宋体;font-size:10pt;\">的结合自由能。结果表明范德华相互作用驱动了</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">PMI</span><span style=\"font-family:宋体;font-size:10pt;\">与</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">MDMX</span><span style=\"font-family:宋体;font-size:10pt;\">的结合。同时也使用基于残基对的自由能分解方法计算了残基</span><span style=\"font-family:宋体;font-size:10pt;\">–</span><span style=\"font-family:宋体;font-size:10pt;\">残基相互作用，结果不仅表明</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">PMI</span><span style=\"font-family:宋体;font-size:10pt;\">的</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">5</span><span style=\"font-family:宋体;font-size:10pt;\">个残基能与</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">MDMX</span><span style=\"font-family:宋体;font-size:10pt;\">产生强烈的相互作用，而且也表明</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">CH-CH</span><span style=\"font-family:宋体;font-size:10pt;\">，</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">CH-π</span><span style=\"font-family:宋体;font-size:10pt;\">，</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">π-π</span><span style=\"font-family:宋体;font-size:10pt;\">相互作用主导了</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">PMI</span><span style=\"font-family:宋体;font-size:10pt;\">在</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">MDMX</span><span style=\"font-family:宋体;font-size:10pt;\">疏水性裂缝中的结合。我们期望这个研究能为抑制</span><span style=\"font-family:'Times New Roman','serif';font-size:10pt;\">p53-MDMX</span><span style=\"font-family:宋体;font-size:10pt;\">相互作用药物的研发提供理论上的启示。<br />
<span style=\"font-size:10pt;\"><span style=\"font-family:Times New Roman;\">Restoration of p53 function is considered to be a new therapeutic strategy for anti-cancers. Molecular Dynamics (MD) simulations coupled with Molecular
%K p53-MDMX相互作用；分子动力学；MM-PBSA；结合自由能<br>p53-MDMX Interaction
%K Molecular Dynamics
%K MM-PBSA
%K Binding Free Energy
%U http://www.hanspub.org/journal/PaperInformation.aspx?PaperID=2953