氟化二芳基磺酰胺:作为新型CETP抑制剂的分子建模、合成和体外验证。

Reema Abu Khalaf, Azhar Shalluf, Maha Habash
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引用次数: 0

摘要

背景:高脂血症是一种心血管疾病的危险因素,其特征是低密度脂蛋白(LDL)、甘油三酯和总胆固醇升高,高密度脂蛋白降低。胆固醇酯转移蛋白(CETP)能够将胆固醇酯从高密度脂蛋白转移到低密度脂蛋白和极低密度脂蛋白质。目的:抑制CETP是一种很有前途的预防和治疗心血管疾病的方法。通过抑制脂质转运活性,它提高了高密度脂蛋白水平,降低了低密度脂蛋白的水平。方法:制备了6a-6g和7a-7g二芳基磺酰胺,并用不同的光谱技术对其结构进行了全面测定。结果:这些化合物经过体外生物学评价,对CETP表现出不同的抑制活性;观察到化合物7a-7g具有100%的抑制活性,而化合物6a-6g在10µM浓度下的活性范围高达42.6%。药效团图谱与生物测定结果一致,其中与化合物6a-6g相比,四个芳环化合物7a-7g对Hypo4/8具有更高的拟合值,并且形状互补的Hypo4/8口袋,而化合物6a-6g错过了与氨基酸Leu206、Phe265和Phe263的这些疏水性相互作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Fluorinated Diaryl Sulfonamides: Molecular Modeling, Synthesis, and In Vitro Validation as New CETP Inhibitors.

Background: Hyperlipidemia, a cardiovascular disease risk factor, is characterized by a rise in low-density lipoprotein (LDL), triglycerides and total cholesterol, and a decrease in high-density lipoprotein (HDL). Cholesteryl ester transfer protein (CETP) enables the transfer of cholesteryl ester from HDL to LDL and very low-density lipoprotein.

Objectives: CETP inhibition is a promising approach to prevent and treat cardiovascular diseases. By inhibiting lipid transport activity, it increases HDL levels and decreases LDL levels.

Materials and method: Herein, diaryl sulfonamides 6a-6g and 7a-7g were prepared, and the structure of these compounds was fully determined using different spectroscopic techniques.

Results: These compounds underwent biological evaluation in vitro and showed different inhibitory activities against CETP; 100% inhibitory activity was observed for compounds 7a-7g, while activities of compounds 6a-6g ranged up to 42.6% at 10 μM concentration. Pharmacophore mapping agreed with the bioassay results where the four aromatic ring compounds 7a-7g possessed higher fit values against Hypo4/8 and the shape-complemented Hypo4/8 in comparison to compounds 6a-6g.

Conclusion: Docking of the synthesized compounds using libdock and ligandfit engines revealed that compounds 7a-7g formed п-п stacking and hydrophobic interactions with the binding pocket, while compounds 6a-6g missed these hydrophobic interactions with amino acids Leu206, Phe265, and Phe263.

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