Identification of Tight-Binding Plasmepsin II and Falcipain 2 Inhibitors in Aqueous Extracts of Marine Invertebrates by the Combination of Enzymatic and Interaction-Based Assays

Identification of Tight-Binding Plasmepsin II and Falcipain 2 Inhibitors in Aqueous Extracts of Marine Invertebrates by the Combination of Enzymatic and Interaction-Based Assays

Natural products from marine origin constitute a very promising and underexplored source of interesting compounds for modern biotechnological and pharmaceutical industries. However, their evaluation is quite challenging and requires specifically designed assays to reliably identify the compounds of...

Full description

Bibliographic Details
Main Authors: Emir Salas-Sarduy, Yasel Guerra, Giovanni Covaleda Cortés, Francesc Xavier Avilés, María A. Chávez Planes
Format: Article
Language:English
Published: MDPI AG 2017-04-01
Series:Marine Drugs
Subjects:
tight-binding protease inhibitor
combined screening strategy
Plasmepsin II
Falcipain 2
Plasmodium falciparum
Online Access:http://www.mdpi.com/1660-3397/15/4/123
id doaj-e6c726e7ff6a4b0792db23896f4c61f6
record_format Article
spelling doaj-e6c726e7ff6a4b0792db23896f4c61f62020-11-24T23:04:30ZengMDPI AGMarine Drugs1660-33972017-04-0115412310.3390/md15040123md15040123Identification of Tight-Binding Plasmepsin II and Falcipain 2 Inhibitors in Aqueous Extracts of Marine Invertebrates by the Combination of Enzymatic and Interaction-Based AssaysEmir Salas-Sarduy0Yasel Guerra1Giovanni Covaleda Cortés2Francesc Xavier Avilés3María A. Chávez Planes4Centro de Estudio de Proteínas, 25 # 455 entre J e I. Facultad de Biología, Universidad de la Habana, 10400 La Habana, CubaCentro de Estudio de Proteínas, 25 # 455 entre J e I. Facultad de Biología, Universidad de la Habana, 10400 La Habana, CubaInstitut de Biotecnologia i de Biomedicina and Departament de Bioquímica i de Biologia Molecular, Universitat Autònoma de Barcelona, 08193 Bellaterra (Barcelona), SpainCoordinación Red CYTED-PROMAL (210RT0398), Proteómica y Quimiogenómica de Inhibidores de Proteasas de Origen Natural con Potencial Terapéutico en Malaria, Universidad Nacional de la Plata, 1900 La Plata, ArgentinaCentro de Estudio de Proteínas, 25 # 455 entre J e I. Facultad de Biología, Universidad de la Habana, 10400 La Habana, CubaNatural products from marine origin constitute a very promising and underexplored source of interesting compounds for modern biotechnological and pharmaceutical industries. However, their evaluation is quite challenging and requires specifically designed assays to reliably identify the compounds of interest in a highly heterogeneous and interfering context. In the present study, we describe a general strategy for the confident identification of tight-binding protease inhibitors in the aqueous extracts of 62 Cuban marine invertebrates, using Plasmodium falciparum hemoglobinases Plasmepsin II and Falcipain 2 as model enzymes. To this end, we first developed a screening strategy that combined enzymatic with interaction-based assays and then validated screening conditions using five reference extracts. Interferences were evaluated and minimized. The results from the massive screening of such extracts, the validation of several hits by a variety of interaction-based assays and the purification and functional characterization of PhPI, a multifunctional and reversible tight-binding inhibitor for Plasmepsin II and Falcipain 2 from the gorgonian Plexaura homomalla, are presented.http://www.mdpi.com/1660-3397/15/4/123tight-binding protease inhibitorcombined screening strategyPlasmepsin IIFalcipain 2Plasmodium falciparum
collection DOAJ
language English
format Article
sources DOAJ
author Emir Salas-Sarduy
Yasel Guerra
Giovanni Covaleda Cortés
Francesc Xavier Avilés
María A. Chávez Planes
spellingShingle Emir Salas-Sarduy
Yasel Guerra
Giovanni Covaleda Cortés
Francesc Xavier Avilés
María A. Chávez Planes
Identification of Tight-Binding Plasmepsin II and Falcipain 2 Inhibitors in Aqueous Extracts of Marine Invertebrates by the Combination of Enzymatic and Interaction-Based Assays
Marine Drugs
tight-binding protease inhibitor
combined screening strategy
Plasmepsin II
Falcipain 2
Plasmodium falciparum
author_facet Emir Salas-Sarduy
Yasel Guerra
Giovanni Covaleda Cortés
Francesc Xavier Avilés
María A. Chávez Planes
author_sort Emir Salas-Sarduy
title Identification of Tight-Binding Plasmepsin II and Falcipain 2 Inhibitors in Aqueous Extracts of Marine Invertebrates by the Combination of Enzymatic and Interaction-Based Assays
title_short Identification of Tight-Binding Plasmepsin II and Falcipain 2 Inhibitors in Aqueous Extracts of Marine Invertebrates by the Combination of Enzymatic and Interaction-Based Assays
title_full Identification of Tight-Binding Plasmepsin II and Falcipain 2 Inhibitors in Aqueous Extracts of Marine Invertebrates by the Combination of Enzymatic and Interaction-Based Assays
title_fullStr Identification of Tight-Binding Plasmepsin II and Falcipain 2 Inhibitors in Aqueous Extracts of Marine Invertebrates by the Combination of Enzymatic and Interaction-Based Assays
title_full_unstemmed Identification of Tight-Binding Plasmepsin II and Falcipain 2 Inhibitors in Aqueous Extracts of Marine Invertebrates by the Combination of Enzymatic and Interaction-Based Assays
title_sort identification of tight-binding plasmepsin ii and falcipain 2 inhibitors in aqueous extracts of marine invertebrates by the combination of enzymatic and interaction-based assays
publisher MDPI AG
series Marine Drugs
issn 1660-3397
publishDate 2017-04-01
description Natural products from marine origin constitute a very promising and underexplored source of interesting compounds for modern biotechnological and pharmaceutical industries. However, their evaluation is quite challenging and requires specifically designed assays to reliably identify the compounds of interest in a highly heterogeneous and interfering context. In the present study, we describe a general strategy for the confident identification of tight-binding protease inhibitors in the aqueous extracts of 62 Cuban marine invertebrates, using Plasmodium falciparum hemoglobinases Plasmepsin II and Falcipain 2 as model enzymes. To this end, we first developed a screening strategy that combined enzymatic with interaction-based assays and then validated screening conditions using five reference extracts. Interferences were evaluated and minimized. The results from the massive screening of such extracts, the validation of several hits by a variety of interaction-based assays and the purification and functional characterization of PhPI, a multifunctional and reversible tight-binding inhibitor for Plasmepsin II and Falcipain 2 from the gorgonian Plexaura homomalla, are presented.
topic tight-binding protease inhibitor
combined screening strategy
Plasmepsin II
Falcipain 2
Plasmodium falciparum
url http://www.mdpi.com/1660-3397/15/4/123
work_keys_str_mv AT emirsalassarduy identificationoftightbindingplasmepsiniiandfalcipain2inhibitorsinaqueousextractsofmarineinvertebratesbythecombinationofenzymaticandinteractionbasedassays
AT yaselguerra identificationoftightbindingplasmepsiniiandfalcipain2inhibitorsinaqueousextractsofmarineinvertebratesbythecombinationofenzymaticandinteractionbasedassays
AT giovannicovaledacortes identificationoftightbindingplasmepsiniiandfalcipain2inhibitorsinaqueousextractsofmarineinvertebratesbythecombinationofenzymaticandinteractionbasedassays
AT francescxavieraviles identificationoftightbindingplasmepsiniiandfalcipain2inhibitorsinaqueousextractsofmarineinvertebratesbythecombinationofenzymaticandinteractionbasedassays
AT mariaachavezplanes identificationoftightbindingplasmepsiniiandfalcipain2inhibitorsinaqueousextractsofmarineinvertebratesbythecombinationofenzymaticandinteractionbasedassays
_version_ 1725629975616290816

Similar Items