针对血脑屏障胆碱转运体的中枢神经系统活性分子在阿尔茨海默病治疗方面的硅学比较分析。

In silico pharmacology Pub Date : 2024-07-31 eCollection Date: 2024-01-01 DOI:10.1007/s40203-024-00245-w
Sergey Shityakov, Carola Y Förster, Ekaterina Skorb
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引用次数: 0

摘要

本研究采用全面的硅学方法研究了中枢神经系统(CNS)活性化合物多奈哌齐(DON)、蛋氨酸(MET)和美金刚(MEM)的血脑屏障(BBB)渗透性。这些化合物对阿尔茨海默病(AD)的治疗具有特别重要的意义。刚性-柔性分子对接模拟表明,所有化合物都与 BBB-ChT 具有良好的结合亲和力,其中 DON 的结合亲和力最高(ΔGbind = -10.26 kcal/mol),这主要是由显著的疏水相互作用介导的。硅学动力学分析表明,DON/BBB-ChT 复合物具有稳定性,构象变化会促使配体释放。三维分子配准证实了 DON 在其最小结合能姿势中的微小构象变化。预测结果表明,与 MET 和 MEM 相比,主动转运机制显著提高了多奈哌齐在大脑中的分布。此外,DON 和 MEM 的致突变概率较低,而 MET 则被确定为具有高度致突变性。总之,这些发现凸显了多奈哌齐主要通过主动转运机制实现良好BBB渗透的潜力,强调了通过体外和体内研究进一步验证其有效治疗AD的必要性:在线版本包含补充材料,可在 10.1007/s40203-024-00245-w.上查阅。
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Comparative in silico analysis of CNS-active molecules targeting the blood-brain barrier choline transporter for Alzheimer's disease therapy.

This study investigated the blood‒brain barrier (BBB) permeability of the central nervous system (CNS)-active compounds donepezil (DON), methionine (MET), and memantine (MEM) by employing a comprehensive in silico approach. These compounds are of particular interest for Alzheimer's disease (AD) therapy. Rigid-flexible molecular docking simulations indicated favorable binding affinities of all the compounds with BBB-ChT, with DON exhibiting the highest binding affinity (ΔGbind = -10.26 kcal/mol), predominantly mediated by significant hydrophobic interactions. In silico kinetic profiling suggested the stability of the DON/BBB-ChT complex, with ligand release prompted by conformational changes. 3D molecular alignment corroborated a minor conformational shift for DON in its minimal binding energy pose. Predictions indicated that active transport mechanisms notably enhance the brain distribution of donepezil compared to that of MET and MEM. Additionally, DON and MEM exhibited low mutagenic probabilities, while MET was identified as highly mutagenic. Overall, these findings highlight the potential of donepezil for superior BBB penetration, primarily through active transport mechanisms, underscoring the need for further validation through in vitro and in vivo studies for effective AD treatment.

Graphical abstract:

Supplementary information: The online version contains supplementary material available at 10.1007/s40203-024-00245-w.

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