Characterization of P. falciparum dipeptidyl aminopeptidase 3 specificity identifies differences in amino acid preferences between peptide‐based substrates and covalent inhibitors

Malarial dipeptidyl aminopeptidases (DPAPs) are cysteine proteases important for parasite development thus making them attractive drug targets. In order to develop inhibitors specific to the parasite enzymes, it is necessary to map the determinants of substrate specificity of the parasite enzymes an...

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Autores principales: de Vries, Laura E., Sanchez, Mateo I., Groborz, Katarzyna, Kuppens, Laurie, Poreba, Marcin, Lehmann, Christine, Nevins, Neysa, Withers‐Martinez, Chrislaine, Hirst, David J., Yuan, Fang, Arastu‐Kapur, Shirin, Horn, Martin, Mares, Michael, Bogyo, Matthew, Drag, Marcin, Deu, Edgar
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6851853/
https://www.ncbi.nlm.nih.gov/pubmed/31177613
http://dx.doi.org/10.1111/febs.14953
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author de Vries, Laura E.
Sanchez, Mateo I.
Groborz, Katarzyna
Kuppens, Laurie
Poreba, Marcin
Lehmann, Christine
Nevins, Neysa
Withers‐Martinez, Chrislaine
Hirst, David J.
Yuan, Fang
Arastu‐Kapur, Shirin
Horn, Martin
Mares, Michael
Bogyo, Matthew
Drag, Marcin
Deu, Edgar
author_facet de Vries, Laura E.
Sanchez, Mateo I.
Groborz, Katarzyna
Kuppens, Laurie
Poreba, Marcin
Lehmann, Christine
Nevins, Neysa
Withers‐Martinez, Chrislaine
Hirst, David J.
Yuan, Fang
Arastu‐Kapur, Shirin
Horn, Martin
Mares, Michael
Bogyo, Matthew
Drag, Marcin
Deu, Edgar
author_sort de Vries, Laura E.
collection PubMed
description Malarial dipeptidyl aminopeptidases (DPAPs) are cysteine proteases important for parasite development thus making them attractive drug targets. In order to develop inhibitors specific to the parasite enzymes, it is necessary to map the determinants of substrate specificity of the parasite enzymes and its mammalian homologue cathepsin C (CatC). Here, we screened peptide‐based libraries of substrates and covalent inhibitors to characterize the differences in specificity between parasite DPAPs and CatC, and used this information to develop highly selective DPAP1 and DPAP3 inhibitors. Interestingly, while the primary amino acid specificity of a protease is often used to develop potent inhibitors, we show that equally potent and highly specific inhibitors can be developed based on the sequences of nonoptimal peptide substrates. Finally, our homology modelling and docking studies provide potential structural explanations of the differences in specificity between DPAP1, DPAP3, and CatC, and between substrates and inhibitors in the case of DPAP3. Overall, this study illustrates that focusing the development of protease inhibitors solely on substrate specificity might overlook important structural features that can be exploited to develop highly potent and selective compounds.
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spelling pubmed-68518532019-11-18 Characterization of P. falciparum dipeptidyl aminopeptidase 3 specificity identifies differences in amino acid preferences between peptide‐based substrates and covalent inhibitors de Vries, Laura E. Sanchez, Mateo I. Groborz, Katarzyna Kuppens, Laurie Poreba, Marcin Lehmann, Christine Nevins, Neysa Withers‐Martinez, Chrislaine Hirst, David J. Yuan, Fang Arastu‐Kapur, Shirin Horn, Martin Mares, Michael Bogyo, Matthew Drag, Marcin Deu, Edgar FEBS J Original Articles Malarial dipeptidyl aminopeptidases (DPAPs) are cysteine proteases important for parasite development thus making them attractive drug targets. In order to develop inhibitors specific to the parasite enzymes, it is necessary to map the determinants of substrate specificity of the parasite enzymes and its mammalian homologue cathepsin C (CatC). Here, we screened peptide‐based libraries of substrates and covalent inhibitors to characterize the differences in specificity between parasite DPAPs and CatC, and used this information to develop highly selective DPAP1 and DPAP3 inhibitors. Interestingly, while the primary amino acid specificity of a protease is often used to develop potent inhibitors, we show that equally potent and highly specific inhibitors can be developed based on the sequences of nonoptimal peptide substrates. Finally, our homology modelling and docking studies provide potential structural explanations of the differences in specificity between DPAP1, DPAP3, and CatC, and between substrates and inhibitors in the case of DPAP3. Overall, this study illustrates that focusing the development of protease inhibitors solely on substrate specificity might overlook important structural features that can be exploited to develop highly potent and selective compounds. John Wiley and Sons Inc. 2019-06-24 2019-10 /pmc/articles/PMC6851853/ /pubmed/31177613 http://dx.doi.org/10.1111/febs.14953 Text en © 2019 The Authors. The FEBS Journal published by John Wiley & Sons Ltd on behalf of Federation of European BiochemicalSocieties. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
de Vries, Laura E.
Sanchez, Mateo I.
Groborz, Katarzyna
Kuppens, Laurie
Poreba, Marcin
Lehmann, Christine
Nevins, Neysa
Withers‐Martinez, Chrislaine
Hirst, David J.
Yuan, Fang
Arastu‐Kapur, Shirin
Horn, Martin
Mares, Michael
Bogyo, Matthew
Drag, Marcin
Deu, Edgar
Characterization of P. falciparum dipeptidyl aminopeptidase 3 specificity identifies differences in amino acid preferences between peptide‐based substrates and covalent inhibitors
title Characterization of P. falciparum dipeptidyl aminopeptidase 3 specificity identifies differences in amino acid preferences between peptide‐based substrates and covalent inhibitors
title_full Characterization of P. falciparum dipeptidyl aminopeptidase 3 specificity identifies differences in amino acid preferences between peptide‐based substrates and covalent inhibitors
title_fullStr Characterization of P. falciparum dipeptidyl aminopeptidase 3 specificity identifies differences in amino acid preferences between peptide‐based substrates and covalent inhibitors
title_full_unstemmed Characterization of P. falciparum dipeptidyl aminopeptidase 3 specificity identifies differences in amino acid preferences between peptide‐based substrates and covalent inhibitors
title_short Characterization of P. falciparum dipeptidyl aminopeptidase 3 specificity identifies differences in amino acid preferences between peptide‐based substrates and covalent inhibitors
title_sort characterization of p. falciparum dipeptidyl aminopeptidase 3 specificity identifies differences in amino acid preferences between peptide‐based substrates and covalent inhibitors
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6851853/
https://www.ncbi.nlm.nih.gov/pubmed/31177613
http://dx.doi.org/10.1111/febs.14953
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