The Potential of Cyclodextrins as Inhibitors for the BM2 Protein: An In Silico Investigation

Author:

Liu Aijun1,Zhang Hao1,Zheng Qingchuan2,Wang Song1

Affiliation:

1. Institute of Theoretical Chemistry, College of Chemistry, Jilin University, Changchun 130023, China

2. School of Pharmaceutical Sciences, Jilin University, Changchun, 130021, China

Abstract

The influenza BM2 transmembrane domain (BM2TM), an acid-activated proton channel, is an attractive antiviral target due to its essential roles during influenza virus replication, whereas no effective inhibitors have been reported for BM2. In this study, we draw inspiration from the properties of cyclodextrins (CDs) and hypothesize that CDs of appropriate sizes may possess the potential to act as inhibitors of the BM2TM proton channel. To explore this possibility, molecular dynamics simulations were employed to assess their inhibitory capabilities. Our findings reveal that CD4, CD5, and CD6 are capable of binding to the BM2TM proton channel, resulting in disrupted water networks and reduced hydrogen bond occupancy between H19 and the solvent within the BM2TM channel necessary for proton conduction. Notably, CD4 completely obstructs the BM2TM water channel. Based on these observations, we propose that CD4, CD5, and CD6 individually contribute to diminishing the proton transfer efficiency of the BM2 protein, and CD4 demonstrates promising potential as an inhibitor for the BM2 proton channel.

Funder

National Natural Science Foundation of China

Jilin Provincial Science and Technology Development Plan

Jilin University Graduate Innovation Research Program Project

Jilin Provincial Association for Science and Technology Domestic and Foreign Academic Exchange Project

Jilin Province Higher Education Research Project

Jilin Provincial Social Science Foundation

Jilin University Graduate Teaching Reform Project

Publisher

MDPI AG

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