将 PCSK9 抑制剂作为治疗动脉粥样硬化性心血管疾病 (ASCVD) 的更安全疗法:药理设计和分子动力学分析。

IF 3 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Journal of cellular biochemistry Pub Date : 2024-05-15 DOI:10.1002/jcb.30581
Ibrahim O. Kehinde, Oluwole Akawa, Adeniyi T. Adewumi, Ali H. Rabbad, Mahmoud E. S. Soliman
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引用次数: 0

摘要

心血管疾病仍然具有挑战性,是致命疾病之一。作为动脉粥样硬化性心血管疾病的主要危险因素,血脂异常,尤其是高低密度脂蛋白胆固醇,可以通过降脂药物进行一级和二级预防。因此,我们仍需深入了解如何设计副作用最小的新药。Proprotein convertase subtilisin/kexin 9(PCSK9)酶能催化蛋白质与低密度脂蛋白之间的相互作用,因此与他汀类药物相比,它是设计有前景的抑制剂的关键靶点。因此,我们利用重新设计的 PCSK9 构象行为筛选潜在化合物,以寻找一个范围广泛的化学库,并利用综合计算方法研究最终化合物的抑制机制,包括配体基本官能团筛选、全原子 MD 模拟和基于 MMGBSA 的结合自由能。所筛选化合物的抑制机制与标准抑制剂进行了比较。K31和K34分子与PCSK9的相互作用更强,其结合能(kcal/mol)分别为-33.39和-63.51,而对照组为-27.97。最终的分子显示出合适的药物亲和性、非致突变性、渗透性和高溶解度值。与apo PCSK9相比,结合型PCSK9复合物的C-α原子均方根偏差和均方根波动显示出稳定和较低的波动。这些发现提出了一个模型,揭示了最终分子抑制 PCSK9 功能的机制,可进一步改进心血管疾病新药的设计。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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PCSK9 inhibitors as safer therapeutics for atherosclerotic cardiovascular disease (ASCVD): Pharmacophore design and molecular dynamics analysis

Cardiovascular disorders are still challenging and are among the deadly diseases. As a major risk factor for atherosclerotic cardiovascular disease, dyslipidemia, and high low-density lipoprotein cholesterol in particular, can be prevented primary and secondary by lipid-lowering medications. Therefore, insights are still needed into designing new drugs with minimal side effects. Proprotein convertase subtilisin/kexin 9 (PCSK9) enzyme catalyses protein-protein interactions with low-density lipoprotein, making it a critical target for designing promising inhibitors compared to statins. Therefore, we screened for potential compounds using a redesigned PCSK9 conformational behaviour to search for a significantly extensive chemical library and investigated the inhibitory mechanisms of the final compounds using integrated computational methods, from ligand essential functional group screening to all-atoms MD simulations and MMGBSA-based binding free energy. The inhibitory mechanisms of the screened compounds compared with the standard inhibitor. K31 and K34 molecules showed stronger interactions for PCSK9, having binding energy (kcal/mol) of −33.39 and −63.51, respectively, against −27.97 of control. The final molecules showed suitable drug-likeness, non-mutagenesis, permeability, and high solubility values. The C-α atoms root mean square deviation and root mean square fluctuation of the bound-PCSK9 complexes showed stable and lower fluctuations compared to apo PCSK9. The findings present a model that unravels the mechanism by which the final molecules proposedly inhibit the PCSK9 function and could further improve the design of novel drugs against cardiovascular diseases.

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来源期刊
Journal of cellular biochemistry
Journal of cellular biochemistry 生物-生化与分子生物学
CiteScore
9.90
自引率
0.00%
发文量
164
审稿时长
1 months
期刊介绍: The Journal of Cellular Biochemistry publishes descriptions of original research in which complex cellular, pathogenic, clinical, or animal model systems are studied by biochemical, molecular, genetic, epigenetic or quantitative ultrastructural approaches. Submission of papers reporting genomic, proteomic, bioinformatics and systems biology approaches to identify and characterize parameters of biological control in a cellular context are encouraged. The areas covered include, but are not restricted to, conditions, agents, regulatory networks, or differentiation states that influence structure, cell cycle & growth control, structure-function relationships.
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