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Inhibitor screening for volume-sensitive LRRC8A chloride channel

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journal contribution
posted on 2023-10-30, 14:40 authored by Chao Liu, Wenqiang Cui, Kongfu Zhu, Shuguang Yuan, Liang Sun, Yujie Liang, Jianping Lu, Da Li, Zhiqin Deng, Li Duan, Weiming Zhang, Xiaohai Yu, Daping Wang, Huawei Zhang

Leucine-rich repeat-containing protein 8 A (LRRC8A) protein is a critical member of volume-regulated anion channels. It plays a critical roles in the regulation of cellular volume and involves in the development of diseases like osteoarthritis. Screening of lead compounds to modulate its function may provide potential therapeutics of related diseases. Here, we employ virtual screening techniques and molecular dynamics (MD) simulation to screen potential inhibitors against LRRC8A. LRRC8A was regarded as the drug target to investigate potential compounds from the ZINC15 database via molecular docking. The final compound was selected among the top 10 Autodock Vina score (–8.8 Kcal/mol) with the ZINC ID ZINC000018195627 after druggability prediction. The docked complex from the virtual screening was subjected to MD simulation to analyze the stability of the LRRC8A protein–ligand complex, with parameters including root mean square deviation, root mean square fluctuation and radius of gyration. Molecular Mechanics/Poisson–Boltzmann Surface Area (MM/PBSA) method was further employed to predict the binding free energies from MD simulation trajectory. Our study provides insightful analysis for the potential compound to modulate LRRC8A and lay the foundation of therapeutics development against osteoarthritis.

Communicated by Ramaswamy H. Sarma

Funding

This work is supported by National Natural Science Foundation of China (No. 31900046 to H.W.Z., No. 81972085 and No. 82172465 to D.P.W.), Guangdong Provincial Key Laboratory of Advanced Biomaterials (2022B1212010003 to H.W.Z.) and Center for Computational Science and Engineering at Southern University of Science and Technology.

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