Discovery of Immunoproteasome Inhibitors Using Large-Scale Covalent Virtual Screening

Andrea Scarpino; Dávid Bajusz; Matic Proj; Martina Gobec; Izidor Sosič; Stanislav Gobec; György  G. Ferenczy; György  M. Keserű

doi:10.3390/molecules24142590

Molecules (Jul 2019)

Discovery of Immunoproteasome Inhibitors Using Large-Scale Covalent Virtual Screening

Andrea Scarpino,
Dávid Bajusz,
Matic Proj,
Martina Gobec,
Izidor Sosič,
Stanislav Gobec,
György G. Ferenczy,
György M. Keserű

Affiliations

Andrea Scarpino: Medicinal Chemistry Research Group, Research Centre for Natural Sciences, Hungarian Academy of Sciences, Magyar tudósok krt. 2, H-1117 Budapest, Hungary
Dávid Bajusz: Medicinal Chemistry Research Group, Research Centre for Natural Sciences, Hungarian Academy of Sciences, Magyar tudósok krt. 2, H-1117 Budapest, Hungary
Matic Proj: Faculty of Pharmacy, University of Ljubljana, Aškerčeva cesta 7, SI-1000 Ljubljana, Slovenia
Martina Gobec: Faculty of Pharmacy, University of Ljubljana, Aškerčeva cesta 7, SI-1000 Ljubljana, Slovenia
Izidor Sosič: Faculty of Pharmacy, University of Ljubljana, Aškerčeva cesta 7, SI-1000 Ljubljana, Slovenia
Stanislav Gobec: Faculty of Pharmacy, University of Ljubljana, Aškerčeva cesta 7, SI-1000 Ljubljana, Slovenia
György G. Ferenczy: Medicinal Chemistry Research Group, Research Centre for Natural Sciences, Hungarian Academy of Sciences, Magyar tudósok krt. 2, H-1117 Budapest, Hungary
György M. Keserű: Medicinal Chemistry Research Group, Research Centre for Natural Sciences, Hungarian Academy of Sciences, Magyar tudósok krt. 2, H-1117 Budapest, Hungary

DOI: https://doi.org/10.3390/molecules24142590
Journal volume & issue: Vol. 24, no. 14
p. 2590

Abstract

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Large-scale virtual screening of boronic acid derivatives was performed to identify nonpeptidic covalent inhibitors of the β5i subunit of the immunoproteasome. A hierarchical virtual screening cascade including noncovalent and covalent docking steps was applied to a virtual library of over 104,000 compounds. Then, 32 virtual hits were selected, out of which five were experimentally confirmed. Biophysical and biochemical tests showed micromolar binding affinity and time-dependent inhibitory potency for two compounds. These results validate the computational protocol that allows the screening of large compound collections. One of the lead-like boronic acid derivatives identified as a covalent immunoproteasome inhibitor is a suitable starting point for chemical optimization.

Published in Molecules

ISSN: 1420-3049 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Chemistry: Organic chemistry
Website: http://www.mdpi.com/journal/molecules

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