Structural Elucidation of Recombinant Trichomonas Vaginalis 20S Proteasome Bound to Covalent Inhibitors

Overview

Journal Nat Commun

Specialty Biology

Date 2024 Oct 4

PMID 39366995

Authors

Jan Silhan

Pavla Fajtova

Jitka Bartosova

Brianna M Hurysz

Jehad Almaliti

Yukiko Miyamoto

Lars Eckmann

William H Gerwick

Anthony J ODonoghue

Evzen Boura

Affiliations

Soon will be listed here.

Abstract

The proteasome is a proteolytic enzyme complex essential for protein homeostasis in mammalian cells and protozoan parasites like Trichomonas vaginalis (Tv), the cause of the most common, non-viral sexually transmitted disease. Tv and other protozoan 20S proteasomes have been validated as druggable targets for antimicrobials. However, low yields and purity of the native proteasome have hindered studies of the Tv 20S proteasome (Tv20S). We address this challenge by creating a recombinant protozoan proteasome by expressing all seven α and seven β subunits of Tv20S alongside the Ump-1 chaperone in insect cells. The recombinant Tv20S displays biochemical equivalence to its native counterpart, confirmed by various assays. Notably, the marizomib (MZB) inhibits all catalytic subunits of Tv20S, while the peptide inhibitor carmaphycin-17 (CP-17) specifically targets β2 and β5. Cryo-electron microscopy (cryo-EM) unveils the structures of Tv20S bound to MZB and CP-17 at 2.8 Å. These findings explain MZB's low specificity for Tv20S compared to the human proteasome and demonstrate CP-17's higher specificity. Overall, these data provide a structure-based strategy for the development of specific Tv20S inhibitors to treat trichomoniasis.

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