Non-Covalent Inhibitors of the 20S Proteasome

Carlos García-Echeverría; Patricia Imbach; Johannes Roesel; Peter Fuerst; Marc Lang; Vito Guagnano; Maria Noorani; Johann Zimmermann; Pascal Furet

doi:10.2533/000942903777679415

Non-Covalent Inhibitors of the 20S Proteasome

Authors

Carlos García-Echeverría
Patricia Imbach
Johannes Roesel
Peter Fuerst
Marc Lang
Vito Guagnano
Maria Noorani
Johann Zimmermann
Pascal Furet

DOI:

https://doi.org/10.2533/000942903777679415

Keywords:

Antitumor agents, Drug design, Enzyme inhibitors, Peptidomimetic

Abstract

Peptidomimetics have been commonly used as lead compounds to design inhibitors with high affinity and specificity for a particular enzyme. The discovery that a 2-aminobenzylstatine derivative originally designed to target an aspartyl protease was able to inhibit specifically and non-covalently the chymotrypsin-like activity of the 20S proteasome represented a unique starting point for our medicinal chemistry endeavor for this target. Utilizing a structure-based design approach, we have been able to improve the potency of this new class of proteasome inhibitors without affecting its in vitro selectivity profile.

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Published

2003-04-01

How to Cite

[1]

C. García-Echeverría, P. Imbach, J. Roesel, P. Fuerst, M. Lang, V. Guagnano, M. Noorani, J. Zimmermann, P. Furet, Chimia 2003, 57, 179, DOI: 10.2533/000942903777679415.