使用动态组合化学鉴定和合成选择性胆固醇酯酶抑制剂。

Identification and synthesis of selective cholesterol esterase inhibitor using dynamic combinatorial chemistry.

机构信息

School of Pharmacy, Jiangsu University, Zhenjiang, 301 Xuefu Rd., Zhenjiang, China.

出版信息

Bioorg Chem. 2022 Feb;119:105520. doi: 10.1016/j.bioorg.2021.105520. Epub 2021 Nov 27.

DOI:10.1016/j.bioorg.2021.105520

Abstract

In this study, the concept of dynamic combinatorial chemistry (DCC) was applied to explore novel cholesterol esterase (CEase) inhibitors. In the presence of enzyme, two substrates (A1H3 and A2H3) were amplified from the dynamic combinatorial library (DCL), which was generated through reversible acylhydrazone formation reaction. In the in vitro biological evaluation, compound A1H3 exhibited not only potent (IC in nanomolar range) but also selective inhibition (>120 folds of selectivity for CEase over AChE). Furthermore, the binding pattern and possible binding mechanism were investigated in the kinetic experiment and molecular docking study, respectively.

摘要

在这项研究中，动态组合化学（DCC）的概念被应用于探索新型胆固醇酯酶（CEase）抑制剂。在酶的存在下，从动态组合库（DCL）中扩增出两种底物（A1H3 和 A2H3），这是通过可逆酰腙形成反应生成的。在体外生物学评价中，化合物 A1H3 不仅表现出很强的抑制活性（IC 值在纳摩尔范围内），而且具有选择性（对 CEase 的选择性是 AChE 的 120 多倍）。此外，在动力学实验和分子对接研究中分别研究了结合模式和可能的结合机制。

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使用动态组合化学鉴定和合成选择性胆固醇酯酶抑制剂。

Identification and synthesis of selective cholesterol esterase inhibitor using dynamic combinatorial chemistry.

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