| Literature DB >> 32738998 |
Thuc-Huy Duong1, Asshaima Paramita Devi2, Nguyen-Minh-An Tran3, Hoang-Vinh-Truong Phan4, Ngoc-Vinh Huynh5, Jirapast Sichaem6, Hoai-Duc Tran3, Mahboob Alam7, Thi-Phuong Nguyen8, Huu-Hung Nguyen9, Warinthorn Chavasiri2, Tien-Cong Nguyen10.
Abstract
A series of novel N-substituted hydrazide derivatives were synthesized by reacting atranorin, a compound with a natural depside structure (1), with a range of hydrazines. The natural product and 12 new analogues (2-13) were investigated for inhibition of α-glucosidase. The N-substituted hydrazide derivatives showed more potent inhibition than the original. The experimental results were confirmed by docking analysis. This study suggests that these compounds are promising molecules for diabetes therapy. Molecular dynamics simulations were carried out with compound 2 demonstrating the best docking model using Gromac during simulation up to 20 ns to explore the stability of the complex ligand-protein. Furthermore, the activity of all synthetic compounds 2-13 against a normal cell line HEK293, used for assessing their cytotoxicity, was evaluated.Entities:
Keywords: Atranorin; Cytotoxicity; N-substituted hydrazide derivatives; Parmotrema tsavoense; α-Glucosidase inhibition
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Year: 2020 PMID: 32738998 DOI: 10.1016/j.bmcl.2020.127359
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823