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利用机器学习和分子对接方法发现新型抗乙酰胆碱酯酶肽
Authors Xiao W, Chen LZ, Chang J, Xiao YW
Received 12 March 2025
Accepted for publication 28 May 2025
Published 14 June 2025 Volume 2025:19 Pages 5085—5098
DOI https://doi.org/10.2147/DDDT.S523769
Checked for plagiarism Yes
Review by Single anonymous peer review
Peer reviewer comments 2
Editor who approved publication: Professor Tamer Ibrahim
Wei Xiao, Liu-Zhen Chen, Jun Chang, Yi-Wen Xiao
School of Life Science, Jiangxi Science & Technology Normal University, Nanchang, Jiangxi, People’s Republic of China
Correspondence: Jun Chang, School of Life Science, Jiangxi Science & Technology Normal University, Nanchang, Jiangxi, People’s Republic of China, Email changjun@jxstnu.edu.cn
Objective: Alzheimer’s disease poses a significant threat to human health. Currenttherapeutic medicines, while alleviate symptoms, fail to reverse the disease progression or reduce its harmful effects, and exhibit toxicity and side effects such as gastrointestinal discomfort and cardiovascular disorders. The major challenge in developing machine learning models for anti-acetylcholinesterase peptides discovery is the limited availability of active peptide data in public databases. This study primarily aims to address this challenge and secondarily to discover novel, safer, and less toxic anti-acetylcholinesterase peptides for better Alzheimer’s disease treatment.
Methods: A Random Forest Classifier model was constructed from a hybrid dataset of non-peptide small molecules and peptides. It was applied to screen a custom peptide library. The binding affinities of the predicted peptides to acetylcholinesterase were assessed via molecular docking, and top ranked peptides were selected for experimental assay.
Results: The top six peptides (IFLSMC, WCWIYN, WIGCWD, LHTMELL, WHLCVLF, and VWIIGFEHM) were selected for experimental validation. Their inhibitiory effects on acetylcholinesterase were determined to be 0.007, 3.4, 1.9, 10.6, 1.5, and 3.9 μmol/L, respectively.
Discussion: Predicting anti-acetylcholinesterase peptides is challenging due to the absence of a comprehensive, publicly accessible peptide database. Traditional approaches using only non-peptide small molecules for model construction often have poor performance on predicting active peptides. Here, we developed a machine-learning model from a hybrid dataset of non-peptide small molecules and peptides, which find six potent peptides. This model was as/superior accuracy compared to small-molecule-only models reported before, but has a significant higher capability of discriminating active peptides. Our work shows that hybrid datasets can boost machine-learning model prediction in peptide drug discovery.
Keywords: Alzheimer’s disease, acetylcholinesterase, machine learning, random forest classifier, Peptides