Picomolar Inhibition of Plasmepsin V, an Essential Malaria Protease, Achieved Exploiting the Prime Region

Malaria is an infectious disease caused by Plasmodium parasites. It results in an annual death-toll of ~ 600,000. Resistance to all medications currently in use exists, and novel antimalarial drugs are urgently needed. Plasmepsin V (PmV) is an essential Plasmodium protease and a highly promising ant...

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Autores principales: Gambini, Luca, Rizzi, Luca, Pedretti, Alessandro, Taglialatela-Scafati, Orazio, Carucci, Mario, Pancotti, Andrea, Galli, Corinna, Read, Martin, Giurisato, Emanuele, Romeo, Sergio, Russo, Ilaria
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4643876/
https://www.ncbi.nlm.nih.gov/pubmed/26566224
http://dx.doi.org/10.1371/journal.pone.0142509
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author Gambini, Luca
Rizzi, Luca
Pedretti, Alessandro
Taglialatela-Scafati, Orazio
Carucci, Mario
Pancotti, Andrea
Galli, Corinna
Read, Martin
Giurisato, Emanuele
Romeo, Sergio
Russo, Ilaria
author_facet Gambini, Luca
Rizzi, Luca
Pedretti, Alessandro
Taglialatela-Scafati, Orazio
Carucci, Mario
Pancotti, Andrea
Galli, Corinna
Read, Martin
Giurisato, Emanuele
Romeo, Sergio
Russo, Ilaria
author_sort Gambini, Luca
collection PubMed
description Malaria is an infectious disease caused by Plasmodium parasites. It results in an annual death-toll of ~ 600,000. Resistance to all medications currently in use exists, and novel antimalarial drugs are urgently needed. Plasmepsin V (PmV) is an essential Plasmodium protease and a highly promising antimalarial target, which still lacks molecular characterization and drug-like inhibitors. PmV, cleaving the PExEl motif, is the key enzyme for PExEl-secretion, an indispensable parasitic process for virulence and infection. Here, we describe the accessibility of PmV catalytic pockets to inhibitors and propose a novel strategy for PmV inhibition. We also provide molecular and structural data suitable for future drug development. Using high-throughput platforms, we identified a novel scaffold that interferes with PmV in-vitro at picomolar ranges (~ 1,000-fold more active than available compounds). Via systematic replacement of P and P' regions, we assayed the physico-chemical requirements for PmV inhibition, achieving an unprecedented IC(50) of ~20 pM. The hydroxyethylamine moiety, the hydrogen acceptor group in P(2)', the lipophilic groups upstream to P(3), the arginine and other possible substitutions in position P(3) proved to be critically important elements in achieving potent inhibition. In-silico analyses provided essential QSAR information and model validation. Our inhibitors act ‘on-target’, confirmed by cellular interference of PmV function and biochemical interaction with inhibitors. Our inhibitors are poorly performing against parasite growth, possibly due to poor stability of their peptidic component and trans-membrane permeability. The lowest IC(50) for parasite growth inhibition was ~ 15μM. Analysis of inhibitor internalization revealed important pharmacokinetic features for PExEl-based molecules. Our work disclosed novel pursuable drug design strategies for highly efficient PmV inhibition highlighting novel molecular elements necessary for picomolar activity against PmV. All the presented data are discussed in respect to human aspartic proteases and previously reported inhibitors, highlighting differences and proposing new strategies for drug development.
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spelling pubmed-46438762015-11-18 Picomolar Inhibition of Plasmepsin V, an Essential Malaria Protease, Achieved Exploiting the Prime Region Gambini, Luca Rizzi, Luca Pedretti, Alessandro Taglialatela-Scafati, Orazio Carucci, Mario Pancotti, Andrea Galli, Corinna Read, Martin Giurisato, Emanuele Romeo, Sergio Russo, Ilaria PLoS One Research Article Malaria is an infectious disease caused by Plasmodium parasites. It results in an annual death-toll of ~ 600,000. Resistance to all medications currently in use exists, and novel antimalarial drugs are urgently needed. Plasmepsin V (PmV) is an essential Plasmodium protease and a highly promising antimalarial target, which still lacks molecular characterization and drug-like inhibitors. PmV, cleaving the PExEl motif, is the key enzyme for PExEl-secretion, an indispensable parasitic process for virulence and infection. Here, we describe the accessibility of PmV catalytic pockets to inhibitors and propose a novel strategy for PmV inhibition. We also provide molecular and structural data suitable for future drug development. Using high-throughput platforms, we identified a novel scaffold that interferes with PmV in-vitro at picomolar ranges (~ 1,000-fold more active than available compounds). Via systematic replacement of P and P' regions, we assayed the physico-chemical requirements for PmV inhibition, achieving an unprecedented IC(50) of ~20 pM. The hydroxyethylamine moiety, the hydrogen acceptor group in P(2)', the lipophilic groups upstream to P(3), the arginine and other possible substitutions in position P(3) proved to be critically important elements in achieving potent inhibition. In-silico analyses provided essential QSAR information and model validation. Our inhibitors act ‘on-target’, confirmed by cellular interference of PmV function and biochemical interaction with inhibitors. Our inhibitors are poorly performing against parasite growth, possibly due to poor stability of their peptidic component and trans-membrane permeability. The lowest IC(50) for parasite growth inhibition was ~ 15μM. Analysis of inhibitor internalization revealed important pharmacokinetic features for PExEl-based molecules. Our work disclosed novel pursuable drug design strategies for highly efficient PmV inhibition highlighting novel molecular elements necessary for picomolar activity against PmV. All the presented data are discussed in respect to human aspartic proteases and previously reported inhibitors, highlighting differences and proposing new strategies for drug development. Public Library of Science 2015-11-13 /pmc/articles/PMC4643876/ /pubmed/26566224 http://dx.doi.org/10.1371/journal.pone.0142509 Text en © 2015 Gambini et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Gambini, Luca
Rizzi, Luca
Pedretti, Alessandro
Taglialatela-Scafati, Orazio
Carucci, Mario
Pancotti, Andrea
Galli, Corinna
Read, Martin
Giurisato, Emanuele
Romeo, Sergio
Russo, Ilaria
Picomolar Inhibition of Plasmepsin V, an Essential Malaria Protease, Achieved Exploiting the Prime Region
title Picomolar Inhibition of Plasmepsin V, an Essential Malaria Protease, Achieved Exploiting the Prime Region
title_full Picomolar Inhibition of Plasmepsin V, an Essential Malaria Protease, Achieved Exploiting the Prime Region
title_fullStr Picomolar Inhibition of Plasmepsin V, an Essential Malaria Protease, Achieved Exploiting the Prime Region
title_full_unstemmed Picomolar Inhibition of Plasmepsin V, an Essential Malaria Protease, Achieved Exploiting the Prime Region
title_short Picomolar Inhibition of Plasmepsin V, an Essential Malaria Protease, Achieved Exploiting the Prime Region
title_sort picomolar inhibition of plasmepsin v, an essential malaria protease, achieved exploiting the prime region
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4643876/
https://www.ncbi.nlm.nih.gov/pubmed/26566224
http://dx.doi.org/10.1371/journal.pone.0142509
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