Synthesis, α-glucosidase inhibition, and molecular docking studies of novel N-substituted hydrazide derivatives of atranorin as antidiabetic agents

Thuc-Huy Duong; Asshaima Paramita Devi; Nguyen-Minh-An Tran; Hoang-Vinh-Truong Phan; Ngoc-Vinh Huynh; Jirapast Sichaem; Hoai-Duc Tran; Mahboob Alam; Thi-Phuong Nguyen; Huu-Hung Nguyen; Warinthorn Chavasiri; Tien-Cong Nguyen

Synthesis, α-glucosidase inhibition, and molecular docking studies of novel N-substituted hydrazide derivatives of atranorin as antidiabetic agents

Journal

Bioorganic & Medicinal Chemistry Letters

ISSN

0960-894X

Date Issued

2020

Author(s)

Thuc-Huy Duong

Asshaima Paramita Devi

Nguyen-Minh-An Tran

Hoang-Vinh-Truong Phan

Ngoc-Vinh Huynh

Jirapast Sichaem

Hoai-Duc Tran

Mahboob Alam

Thi-Phuong Nguyen

Huu-Hung Nguyen

Warinthorn Chavasiri

Tien-Cong Nguyen

DOI

10.1016/j.bmcl.2020.127359

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.

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Synthesis, α-glucosidase inhibition, and molecular docking studies of novel N-substituted hydrazide derivatives of atranorin as antidiabetic agents