Issue 30, 2014

Exploring dual electrophiles in peptide-based proteasome inhibitors: carbonyls and epoxides

Abstract

Peptide epoxyketones are potent and selective proteasome inhibitors. Selectivity is governed by the epoxyketone dual electrophilic warhead, which reacts with the N-terminal threonine 1,2-amino alcohol uniquely present in proteasome active sites. We studied a series of C-terminally modified oligopeptides featuring adjacent electrophiles based on the epoxyketone warhead. We found that the carbonyl moiety in the natural warhead is essential, but that the adjacent epoxide can be replaced by a carbonyl, though with considerable loss of activity.

Graphical abstract: Exploring dual electrophiles in peptide-based proteasome inhibitors: carbonyls and epoxides

Supplementary files

Article information

Article type
Paper
Submitted
01 May 2014
Accepted
18 Jun 2014
First published
20 Jun 2014

Org. Biomol. Chem., 2014,12, 5710-5718

Author version available

Exploring dual electrophiles in peptide-based proteasome inhibitors: carbonyls and epoxides

B. Xin, G. de Bruin, M. Verdoes, D. V. Filippov, G. A. van der Marel and H. S. Overkleeft, Org. Biomol. Chem., 2014, 12, 5710 DOI: 10.1039/C4OB00893F

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