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首页> 外文期刊>Journal of Inclusion Phenomena and Macrocyclic Chemistry >Inclusion complexes of pantoprazole with beta-cyclodextrin and cucurbit[7]uril: experimental and molecular modeling study
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Inclusion complexes of pantoprazole with beta-cyclodextrin and cucurbit[7]uril: experimental and molecular modeling study

机译:用β-环糊精和葫芦(葫芦)包络合物[7] URIL:实验和分子造型研究

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摘要

The inclusion complexes of the proton pump inhibitor (PPI) pantoprazole sodium (PNZ(Na)) with beta-cyclodextrin (beta CD) and cucurbit[7]uril (CB[7]) have been investigated. Fluorescence spectroscopy and electrospray ionization mass spectrometry (ESI-MS) were used to characterize these complexes. The fluorescence intensity of PNZ(Na) was remarkably enhanced by both hosts, indicating the formation of the complexes. Nevertheless, the two hosts are of comparable cavity size their effect on the fluorescence of PNZ(Na) was quite different. The ESI-MS data on the other hand confirmed the formation of a 1:1 PNZ(Na): host inclusion complexes for the two hosts. We further utilized molecular dynamics to shed more light on the mechanism of complexation and on the stability of these complexes in aqueous media. The complexes were stabilized over the 20 ns of simulation time mainly via hydrogen bonding interactions in addition to hydrophobic effects and van der Waals interactions. Snapshots collected during the simulations for both complexes have clearly shown that the mode of insertion of PNZ into the two host's cavities are different which explain the difference in fluorescence enhancement of PNZ obtained in presence of each of these hosts.
机译:已经研究了质子泵抑制剂(PPI)泮托拉唑(PNZ(NA))与β-环糊精(βCD)和葫芦[7] URIN(CB [7])的包合物的包合物。荧光光谱和电喷雾电离质谱(ESI-MS)用于表征这些配合物。两个宿主显着增强了PNZ(NA)的荧光强度,表明复合物的形成。然而,这两个宿主具有可比的腔体大小它们对PNZ(NA)的荧光的影响非常不同。另一方面,ESI-MS数据确认了两个主机的1:1 PNZ(NA):主机包装复合物。我们进一步利用了分子动力学在络合机理和含水介质中的这些配合物的稳定性上进行了更多的光。除了疏水效应和范德华相互作用之外,主要通过氢键相互作用主要通过氢键相互作用稳定在20ns模拟时间上。在两种复合物的模拟期间收集的快照已经清楚地表明,PNZ的插入模式进入两个宿主的腔的模式是不同的,这对这些宿主的每个宿主存在的PNZ的荧光增强差异不同。

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