Article

Chitinase inhibitors: extraction of the active framework from natural argifin and use of in situ click chemistry

The Kitasato Institute and Kitasato Institute for Life Science and Graduate School of Infection Control Sciences, Kitasato University, Tokyo, Japan.
The Journal of Antibiotics (impact factor: 1.65). 03/2009; 62(5):277-282. DOI:10.1038/ja.2009.28 pp.277-282

ABSTRACT In situ click chemistry is a target-guided synthesis technique for discovering potent protein ligands by assembling azides and alkynes into triazoles inside the affinity site of a target protein. We report the rapid discovery of a new and potent inhibitor of bacterial chitinases by the use of in situ click chemistry. We observed a target-templated formation of a potent triazole inhibitor of the chitinase-catalyzed chitin hydrolysis, through in situ click chemistry between a biologically active azide-containing scaffold and structurally unrelated alkyne fragments. Chitinase inhibitors have chemotherapeutic potential as fungicides, pesticides and antiasthmatics. Argifin, which has been isolated and characterized as a cyclopentapeptide natural product by our research group, shows strong inhibitory activity against chitinases. As a result of our efforts at developing a chitinase inhibitor from an azide-bearing argifin fragment and the application of the chitinase template and a library of alkynes, we rapidly obtained a very potent and new 1,5-disubstituted triazole inhibitor against Serratia marcescens chitinase (SmChi) B. The new inhibitor expressed 300-fold increase in the inhibitory activity against SmChiB compared with that of argifin. To the best of our knowledge, our finding of an enzyme-made 1,5-disubstituted triazole, using in situ click chemistry is the second example reported in the literature.Keywords: argifin, chitinase, in situ click chemistry, target-guided synthesis, triazole

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Keywords

azide-bearing argifin fragment
 
bacterial chitinases
 
biologically active azide-containing scaffold
 
chitinase inhibitor
 
Chitinase inhibitors
 
chitinase template
 
chitinase-catalyzed chitin hydrolysis
 
cyclopentapeptide natural product
 
discovering potent protein ligands
 
enzyme-made 1,5-disubstituted triazole
 
new 1,5-disubstituted triazole inhibitor
 
new inhibitor
 
potent inhibitor
 
potent triazole inhibitor
 
research group
 
Serratia marcescens chitinase
 
situ click chemistry
 
strong inhibitory activity
 
target-guided synthesis
 
target-guided synthesis technique
 

Tomoyasu Hirose