Potent dual inhibitors of Plasmodium falciparum M1 and M17 aminopeptidases through optimization of S1 pocket interactions

Nyssa Drinkwater; Natalie B Vinh; Shailesh N Mistry; Rebecca S Bamert; Chiara Ruggeri; John P Holleran; Sasdekumar Loganathan; Alessandro Paiardini; Susan A Charman; Andrew K Powell; Vicky M Avery; Sheena McGowan; Peter J Scammells

doi:10.1016/j.ejmech.2016.01.015

Potent dual inhibitors of Plasmodium falciparum M1 and M17 aminopeptidases through optimization of S1 pocket interactions

Eur J Med Chem. 2016 Mar 3:110:43-64. doi: 10.1016/j.ejmech.2016.01.015. Epub 2016 Jan 13.

Affiliations

¹ Biomedicine Discovery Institute and Department of Microbiology, Melbourne, VIC 3800, Australia; Department of Biochemistry and Molecular Biology Monash University (Clayton Campus), Melbourne, VIC 3800, Australia.
² Medicinal Chemistry, Monash Institute of Pharmaceutical Sciences, Monash University (Parkville Campus), Parkville, VIC 3052, Australia.
³ Dipartmento di Biologia e Biotecnologie "Charles Darwin", Sapienza Universita di Roma, 00185 Roma, Italy.
⁴ Discovery Biology, Eskitis Institute for Drug Discovery, Griffith University, Nathan, Queensland 4111, Australia.
⁵ Dipartimento di Scienze Biochimiche "A. Rossi Fanelli", Sapienza Università di Roma, 00185 Roma, Italy.
⁶ Centre for Drug Candidate Optimisation, Monash Institute of Pharmaceutical Sciences, Monash University (Parkville Campus), Parkville, VIC 3052, Australia.
⁷ Biomedicine Discovery Institute and Department of Microbiology, Melbourne, VIC 3800, Australia; Department of Biochemistry and Molecular Biology Monash University (Clayton Campus), Melbourne, VIC 3800, Australia. Electronic address: Sheena.McGowan@monash.edu.
⁸ Medicinal Chemistry, Monash Institute of Pharmaceutical Sciences, Monash University (Parkville Campus), Parkville, VIC 3052, Australia. Electronic address: Peter.Scammells@monash.edu.

PMID: 26807544
DOI: 10.1016/j.ejmech.2016.01.015

Abstract

Malaria remains a global health problem, and though international efforts for treatment and eradication have made some headway, the emergence of drug-resistant parasites threatens this progress. Antimalarial therapeutics acting via novel mechanisms are urgently required. Plasmodium falciparum M1 and M17 are neutral aminopeptidases which are essential for parasite growth and development. Previous work in our group has identified inhibitors capable of dual inhibition of PfA-M1 and PfA-M17, and revealed further regions within the protease S1 pockets that could be exploited in the development of ligands with improved inhibitory activity. Herein, we report the structure-based design and synthesis of novel hydroxamic acid analogues that are capable of potent inhibition of both PfA-M1 and PfA-M17. Furthermore, the developed compounds potently inhibit Pf growth in culture, including the multi-drug resistant strain Dd2. The ongoing development of dual PfA-M1/PfA-M17 inhibitors continues to be an attractive strategy for the design of novel antimalarial therapeutics.

Keywords: Aminopeptidase inhibitors; Hydroxamic acid; Malaria; Plasmodium falciparum; Zinc-binding group.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Aminopeptidases / antagonists & inhibitors*
Aminopeptidases / chemistry
Aminopeptidases / metabolism
Antimalarials / chemistry
Antimalarials / pharmacology*
HEK293 Cells
Humans
Hydroxamic Acids / chemistry
Hydroxamic Acids / pharmacology*
Malaria, Falciparum / drug therapy
Models, Molecular
Plasmodium falciparum / drug effects*
Protease Inhibitors / chemistry
Protease Inhibitors / pharmacology*
Protozoan Proteins / antagonists & inhibitors*
Protozoan Proteins / chemistry
Protozoan Proteins / metabolism
Structure-Activity Relationship
Zinc / metabolism

Substances

Antimalarials
Hydroxamic Acids
Protease Inhibitors
Protozoan Proteins
Aminopeptidases
Zinc