Structure–activity relationship of human glutaminyl cyclase inhibitors having an N-(5-methyl-1H-imidazol-1-yl)propyl thiourea template

Trà̂n, Phương Thảo; Hoàng, Văn Hải; Thorat, Shivaji A.; Kim, Sung Eun; Ann, Jihyae; Chang, Yu Jin; Nam, Dong Woo; Song, Hyundong; Mook-Jung, Inhee; Lee, Jiyoun; Lee, Jeewoo

Structure–activity relationship of human glutaminyl cyclase inhibitors having an N-(5-methyl-1H-imidazol-1-yl)propyl thiourea template

2013

In an effort to design inhibitors of human glutaminyl cyclase (QC), we have synthesized a library of N-aryl N-(5-methyl-1H-imidazol-1-yl)propyl thioureas and investigated the contribution of the aryl region of these compounds to their structure–activity relationships as cyclase inhibitors. Our design was guided by the proposed binding mode of the preferred substrate for the cyclase. In this series, compound 52 was identified as the most potent QC inhibitor with an IC₅₀ value of 58nM, which was two-fold more potent than the previously reported lead 2. Compound 52 is a most promising candidate for future evaluation to monitor its ability to reduce the formation of pGlu-Aβ and Aβ plaques in cells and transgenic animals.

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AGROVOC Keywords

chemistry drug therapy enzyme inhibitors humans humans metabolism pharmacology thiourea thiourea transgenic animals

Bibliographic information

Published in

Bioorganic & medicinal chemistry

Volume 21 Issue 13 Pagination 3821 - 3830 ISSN 0968-0896

Publisher

Elsevier Ltd

Other Subjects

Drug design; Inhibitory concentration 50; Antagonists & inhibitors; Aminoacyltransferases; Inhibitory concentration 50; Alzheimer disease; Analogs & derivatives; Hek293 cells; Structure-activity relationships

Language

English

Type

Journal Article; Text

In AGRIS since: 2024-02-28

Format: MODS

Data Provider

This bibliographic record has been provided by National Agricultural Library

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Links

DOI http://dx.doi.org/10.1016/j.bmc.2013.04.005

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