The Discovery of Potential Acetylcholinesterase Inhibitors: a Combination of Pharmacophore Modeling, Virtual Screening, and Molecular Docking Studies

Overview

Journal J Biomed Sci

Publisher Biomed Central

Specialty Biology

Date 2011 Jan 22

PMID 21251245

Citations 55

Authors

Shin-Hua Lu

Josephine W Wu

Hsuan-Liang Liu

Jian-Hua Zhao

Kung-Tien Liu

Chih-Kuang Chuang

Hsin-Yi Lin

Wei-Bor Tsai

Yih Ho

Affiliations

Soon will be listed here.

Abstract

Background: Alzheimer's disease (AD) is the most common cause of dementia characterized by progressive cognitive impairment in the elderly people. The most dramatic abnormalities are those of the cholinergic system. Acetylcholinesterase (AChE) plays a key role in the regulation of the cholinergic system, and hence, inhibition of AChE has emerged as one of the most promising strategies for the treatment of AD.

Methods: In this study, we suggest a workflow for the identification and prioritization of potential compounds targeted against AChE. In order to elucidate the essential structural features for AChE, three-dimensional pharmacophore models were constructed using Discovery Studio 2.5.5 (DS 2.5.5) program based on a set of known AChE inhibitors.

Results: The best five-features pharmacophore model, which includes one hydrogen bond donor and four hydrophobic features, was generated from a training set of 62 compounds that yielded a correlation coefficient of R = 0.851 and a high prediction of fit values for a set of 26 test molecules with a correlation of R² = 0.830. Our pharmacophore model also has a high Güner-Henry score and enrichment factor. Virtual screening performed on the NCI database obtained new inhibitors which have the potential to inhibit AChE and to protect neurons from Aβ toxicity. The hit compounds were subsequently subjected to molecular docking and evaluated by consensus scoring function, which resulted in 9 compounds with high pharmacophore fit values and predicted biological activity scores. These compounds showed interactions with important residues at the active site.

Conclusions: The information gained from this study may assist in the discovery of potential AChE inhibitors that are highly selective for its dual binding sites.

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