Prokopcová, H., Dallinger, D., Uray, G., Kaan, H.Y.K., Ulaganathan, V., Kozielski, F., Laggner, C. and Kappe, C.O. (2010) Structure-Activity Relationships and Molecular Docking of Novel Dihydropyrimidine-Based Mitotic Eg5 Inhibitors. ChemMedChem, 5(10), pp. 1760-1769. (doi: 10.1002/cmdc.201000252)
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Publisher's URL: http://dx.doi.org/10.1002/cmdc.201000252
Abstract
Dihydropyrimidine-based compounds belong to the first discovered inhibitors of the human mitotic kinesin Eg5. Although they are used by many research groups as model compounds for chemical genetics, considerably less emphasis has been placed on the improvement of this type of inhibitor, with the exception of two recent studies. Dihydropyrimidines can be divided into class I (analogues that bind in the S configuration) and class II type inhibitors, which bind in the R configuration. Herein we report the synthesis and optimization of novel class II type dihydropyrimidines using a combination of in vitro and docking techniques
Item Type: | Articles |
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Status: | Published |
Refereed: | Yes |
Glasgow Author(s) Enlighten ID: | Kozielski, Professor Frank and Ulaganathan, Dr Venkat |
Authors: | Prokopcová, H., Dallinger, D., Uray, G., Kaan, H.Y.K., Ulaganathan, V., Kozielski, F., Laggner, C., and Kappe, C.O. |
College/School: | College of Medical Veterinary and Life Sciences > School of Cancer Sciences |
Journal Name: | ChemMedChem |
ISSN: | 1860-7179 |
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