Discovery of sultam-containing small-molecule disruptors of the huntingtin–calmodulin protein–protein interaction

被引:0
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作者
Nicholas J. Klus
Khushboo Kapadia
Peter McDonald
Anuradha Roy
Kevin J. Frankowski
Nancy A. Muma
Jeffrey Aubé
机构
[1] UNC Eshelman School of Pharmacy,Division of Chemical Biology and Medicinal Chemistry, Center for Integrative Chemical Biology and Drug Discovery
[2] University of Kansas,Department of Pharmacology and Toxicology
[3] University of Kansas High-Throughput Screening Laboratory,undefined
[4] University of Kansas,undefined
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Huntington’s disease; High-throughput screening; Neurodegeneration; Structure–activity relationship studies;
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摘要
The aberrant protein–protein interaction between calmodulin and mutant huntingtin protein in Huntington’s disease patients has been found to contribute to Huntington’s disease progression. A high-throughput screen for small molecules capable of disrupting this interaction revealed a sultam series as potent small-molecule disruptors. Diversification of the sultam scaffold afforded a set of 24 analogs or further evaluation. Several structure–activity trends within the analog set were found, most notably a negligible effect of absolute stereochemistry and a strong beneficial correlation with electron-withdrawing aromatic substituents. The most promising analogs were profiled for off-target effects at relevant kinases and, ultimately, one candidate molecule was evaluated for neuroprotection in a neuronal cell model of Huntington’s disease.
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页码:1187 / 1198
页数:11
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