Fiedler Walter, Freisleben Fabian, Wellbrock Jasmin, Kirschner Karl N
Department of Oncology, Hematology and Bone Marrow Transplantation with Section Pneumology, Hubertus Wald University Cancer Center, University Medical Center Hamburg-Eppendorf, 20251 Hamburg, Germany.
Department of Computer Science, University of Applied Sciences Bonn-Rhein-Sieg, 53757 Sankt Augustin, Germany.
J Chem Inf Model. 2022 Aug 8;62(15):3604-3617. doi: 10.1021/acs.jcim.2c00290. Epub 2022 Jul 22.
Recent experimental evidence suggests that mebendazole, a popular antiparasitic drug, binds to heat shock protein 90 (Hsp90) and inhibits acute myeloid leukemia cell growth. In this study we use quantum mechanics (QM), molecular similarity, and molecular dynamics (MD) calculations to predict possible binding poses of mebendazole to the adenosine triphosphate (ATP) binding site of Hsp90. Extensive conformational searches and minimization of the five mebendazole tautomers using the MP2/aug-cc-pVTZ theory level resulted in 152 minima. Mebendazole-Hsp90 complex models were subsequently created using the QM optimized conformations and protein coordinates obtained from experimental crystal structures that were chosen through similarity calculations. Nine different poses were identified from a total of 600 ns of explicit solvent, all-atom MD simulations using two different force fields. All simulations support the hypothesis that mebendazole is able to bind to the ATP binding site of Hsp90.
近期的实验证据表明,常用抗寄生虫药物甲苯咪唑可与热休克蛋白90(Hsp90)结合,并抑制急性髓系白血病细胞的生长。在本研究中,我们运用量子力学(QM)、分子相似性和分子动力学(MD)计算来预测甲苯咪唑与Hsp90的三磷酸腺苷(ATP)结合位点的可能结合构象。使用MP2/aug-cc-pVTZ理论水平对甲苯咪唑的五个互变异构体进行广泛的构象搜索和最小化处理,得到了152个极小值。随后,利用通过相似性计算选择的实验晶体结构获得的QM优化构象和蛋白质坐标,创建了甲苯咪唑-Hsp90复合物模型。使用两种不同的力场,通过总共600 ns的显式溶剂全原子MD模拟,确定了九种不同的构象。所有模拟均支持甲苯咪唑能够与Hsp90的ATP结合位点结合这一假设。
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