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Discovery of Novel IDH1 Inhibitor Through Comparative Structure-Based Virtual Screening

Yuwei Wang, Shuai Tang, Huanling Lai, Ruyi Jin, Long Xu, Na Li, Yuping Tang, Hui Guo, Xiaojun Yao, Elaine Lai‐Han Leung

2020Frontiers in Pharmacology33 citationsDOIOpen Access PDF

Abstract

IDH1 mutation occurs in 20–30% of gliomas and is a promising target for the cancer therapy. In present study, the performances of the different IDH1R132H were verified by using glide-docking-based virtual screening. Based on the two crystal structures (5TQH and 6B0Z) with the best capability to distinguish IDH1 inhibitors from decoys, a docking-based virtual screening was employed for identified novel IDH1R132H inhibitors. A total of 57 structurally diverse compounds were reserved and evaluated with experimental testing, and 10 of them exhibited substantial activity against the IDH1R132H (IC50 < 50 μM). Molecular docking technology showed that L806-0255, V015-1671 and AQ-714/41674992 could bind to the binding pocket composed of hydrophobic residues. These findings indicate that L806-0255, V015-1671 and AQ-714/41674992 have the potential for further optimization as a lead compound for the treatment of IDH1 mutated gliomas.

Topics & Concepts

Virtual screeningDrug discoveryPharmacologyComputational biologyMedicineComputer scienceChemistryBiologyBiochemistryCancer, Hypoxia, and MetabolismComputational Drug Discovery MethodsHistone Deacetylase Inhibitors Research
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