Proteomic Profiling of Antimalarial Plasmodione Using 3‐Benz(o)ylmenadione Affinity‐Based Probes

Author:

Iacobucci Ilaria1234,Monaco Vittoria1234,Hovasse Agnès23,Dupouy Baptiste1,Keumoe Rodrigue5,Cichocki Bogdan1,Elhabiri Mourad1,Meunier Brigitte6,Strub Jean‐Marc23,Monti Maria4,Cianférani Sarah23,Blandin Stéphanie A.5,Schaeffer‐Reiss Christine23,Davioud‐Charvet Elisabeth1ORCID

Affiliation:

1. Laboratoire d'Innovation Moléculaire et Applications (LIMA) Team Bio(IN)organic & Medicinal Chemistry UMR7042 CNRS-Université de Strasbourg-Université Haute-Alsace European School of Chemistry Polymers and Materials (ECPM), 25 rue Becquerel, 25, rue Becquerel F-67087 Strasbourg France

2. Laboratoire de Spectrométrie de Masse BioOrganique IPHC UMR 7178 CNRS Université de Strasbourg 67087 Strasbourg France

3. Infrastructure Nationale de Protéomique ProFI – FR2048 F-67087 Strasbourg France

4. Department of Chemical Sciences University of Naples Federico II Complesso Universitario di Monte Sant' Angelo Via Cintia 26 I-80126 Napoli Italy

5. Institut de Biologie Moléculaire et Cellulaire INSERM U1257 – CNRS UPR9022 – Université de Strasbourg 2, Allée Konrad Roentgen -67084 Strasbourg France

6. Institute for Integrative Biology of the Cell (I2BC) CEA CNRS Univ. Paris-Sud, Université Paris-Saclay 91198 Gif-Sur-Yvette Cedex France

Abstract

AbstractUnderstanding the mechanisms of drug action in malarial parasites is crucial for the development of new drugs to combat infection and to counteract drug resistance. Proteomics is a widely used approach to study host‐pathogen systems and to identify drug protein targets. Plasmodione is an antiplasmodial early‐lead drug exerting potent activities against young asexual and sexual blood stages in vitro with low toxicity to host cells. To elucidate its molecular mechanisms, an affinity‐based protein profiling (AfBPP) approach was applied to yeast and P. falciparum proteomes. New (pro‐) AfBPP probes based on the 3‐benz(o)yl‐6‐fluoro‐menadione scaffold were synthesized. With optimized conditions of both photoaffinity labeling and click reaction steps, the AfBPP protocol was then applied to a yeast proteome, yielding 11 putative drug‐protein targets. Among these, we found four proteins associated with oxidoreductase activities, the hypothesized type of targets for plasmodione and its metabolites, and other proteins associated with the mitochondria. In Plasmodium parasites, the MS analysis revealed 44 potential plasmodione targets that need to be validated in further studies. Finally, the localization of a 3‐benzyl‐6‐fluoromenadione AfBPP probe was studied in the subcellular structures of the parasite at the trophozoite stage.

Funder

European Cooperation in Science and Technology

International Business Machines Corporation

Université de Strasbourg

Publisher

Wiley

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