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Identification of covalent active site inhibitors of dengue virus protease.

Drug Des Devel Ther.. 2015-12; 
Koh-Stenta X, Joy J, Wang SF, Kwek PZ, Wee JL, Wan KF, Gayen S, Chen AS, Kang C, Lee MA, Poulsen A, Vasudevan SG, Hill J, Nacro K.
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Gene Synthesis ... Materials and methods. Expression and purification of DENV2 and WNV proteases. A WNV fusion construct encoding fragments from NS2B and NS3, fused by a G4-S-G3 linker, was codon optimized for expression in Escherichia coli and synthesized (GenScript). ... Get A Quote

摘要

Dengue virus (DENV) protease is an attractive target for drug development; however, no compounds have reached clinical development to date. In this study, we utilized a potent West Nile virus protease inhibitor of the pyrazole ester derivative class as a chemical starting point for DENV protease drug development. Compound potency and selectivity for DENV protease were improved through structure-guided small molecule optimization, and protease-inhibitor binding interactions were validated biophysically using nuclear magnetic resonance. Our work strongly suggests that this class of compounds inhibits flavivirus protease through targeted covalent modification of active site serine, contrary to an allosteric bindin... More

关键词

active site binding; covalent inhibitor; flavivirus protease; pyrazole ester derivatives; small molecule optimization