Cystargolide-based amide and ester Pz analogues as proteasome inhibitors and anti-cancer agents

Carlos R. Viera; Bradley T. Stevens; Talysa Viera; Cameron Zielinski; Lee A. Uranga; Snezna Rogelj; Praveen L. Patidar; Rodolfo Tello-Aburto

doi:10.1098/rsos.220358

Royal Society Open Science (Sep 2022)

Cystargolide-based amide and ester Pz analogues as proteasome inhibitors and anti-cancer agents

Carlos R. Viera,
Bradley T. Stevens,
Talysa Viera,
Cameron Zielinski,
Lee A. Uranga,
Snezna Rogelj,
Praveen L. Patidar,
Rodolfo Tello-Aburto

Affiliations

Carlos R. Viera: Department of Chemistry, New Mexico Institute of Mining and Technology, Socorro, NM 87801, USA
Bradley T. Stevens: Department of Biology, New Mexico Institute of Mining and Technology, Socorro, NM 87801, USA
Talysa Viera: Department of Chemistry, New Mexico Institute of Mining and Technology, Socorro, NM 87801, USA
Cameron Zielinski: Department of Chemical Engineering, New Mexico Institute of Mining and Technology, Socorro, NM 87801, USA
Lee A. Uranga: Department of Chemistry and Biochemistry, New Mexico State University, Las Cruces, NM 88003, USA
Snezna Rogelj: Department of Biology, New Mexico Institute of Mining and Technology, Socorro, NM 87801, USA
Praveen L. Patidar: Department of Chemistry, New Mexico Institute of Mining and Technology, Socorro, NM 87801, USA
Rodolfo Tello-Aburto: Department of Chemistry and Biochemistry, New Mexico State University, Las Cruces, NM 88003, USA

DOI: https://doi.org/10.1098/rsos.220358
Journal volume & issue: Vol. 9, no. 9

Abstract

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A series of cystargolide-based β-lactone analogues containing nitrogen atoms at the Pz portion of the scaffold were prepared and evaluated as proteasome inhibitors, and for their cytotoxicity profile toward several cancer cell lines. Inclusion of one, two or even three nitrogen atoms at the Pz portion of the cystargolide scaffold is well tolerated, producing analogues with low nanomolar proteasome inhibition activity, in many cases superior to carfilzomib. Additionally, analogue 8g, containing an ester and pyrazine group at Pz, was shown to possess significant activity toward RPMI 8226 cells (IC50 = 21 nM) and to be less cytotoxic toward the normal tissue model MCF10A cells than carfilzomib.

Published in Royal Society Open Science

ISSN: 2054-5703 (Online)
Publisher: The Royal Society
Country of publisher: United Kingdom
LCC subjects: Science
Website: https://royalsocietypublishing.org/journal/rsos

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