Dataciencia

Colección SciELO Chile

Design and synthesis of chromone-based monoamine oxidase B inhibitors with improved drug-like properties

Indexado

WoS	WOS:000833530700006
Scopus	SCOPUS_ID:85132934729

DOI

10.1016/J.EJMECH.2022.114507

Año

2022

Tipo

artículo de investigación

Citas Totales

Autores Afiliación Chile

Instituciones Chile

% Participación
Internacional

Autores
Afiliación Extranjera

Instituciones
Extranjeras

Abstract

The absence of disease modifying drugs in Parkinson's disease therapy urges for new chemical entities acting on relevant PD-associated biological targets. As a result, developing selective and reversible inhibitors targeting MAO-B is still a desirable line of therapeutic research. Within this framework, a small library of chromone derivatives was synthesized and screened towards human monoamine oxidases. Structural modifications on the chromone 3-phenylcarboxamide resulted in potent MAO-B inhibitors with an improved drug-like profile, and for the first time we obtained potent and selective chromone 2-phenylcarboxamides acting in the low nanomolar range. Compounds 5-hydroxy-4-oxo-N-phenyl-4H-chromene-3-carboxamide (38) (IC50 = 13.0 nM) and N-(4-chlorophenyl)-5-hydroxy-4-oxo-4H-chromene-3-carboxamide (41) (IC50 = 8.3 nM) stood out as reversible, potent, selective and non-cytotoxic MAO-B inhibitors bearing a favourable drug-like profile. Both compounds displayed cytoprotective effects towards iron(III) oxidative stressor.

Revista

Revista	ISSN
European Journal Of Medicinal Chemistry	0223-5234

Métricas Externas

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Disciplinas de Investigación

WOS
Chemistry, Medicinal

Scopus
Pharmacology
Drug Discovery
Organic Chemistry

SciELO
Sin Disciplinas

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Publicaciones WoS (Ediciones: ISSHP, ISTP, AHCI, SSCI, SCI), Scopus, SciELO Chile.

Colaboración Institucional

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Autores - Afiliación

Ord.	Autor	Género	Institución - País
1	Reis, Joana	Mujer	Universidade do Porto - Portugal Univ Porto - Portugal
2	Fernandes, Carlos	Hombre	Universidade do Porto - Portugal Univ Porto - Portugal
3	Salem, Hoda	Mujer	Universidade do Porto - Portugal Univ Porto - Portugal
4	Maia, Marta	Mujer	Universidade do Porto - Portugal Univ Porto - Portugal
5	Tomé, Cláudia	Mujer	Universidade do Porto - Portugal Univ Porto - Portugal
6	Benfeito, Sofia	Mujer	Universidade do Porto - Portugal Univ Porto - Portugal
7	Teixeira, Jose	Hombre	Universidade do Porto - Portugal University of Coimbra, Center for Neuroscience and Cell Biology - Portugal Univ Coimbra - Portugal Univ Porto - Portugal
8	Oliveira, Paulo J.	Hombre	University of Coimbra, Center for Neuroscience and Cell Biology - Portugal Univ Coimbra - Portugal
9	Uriarte, Eugenio	Hombre	Universidad de Santiago de Compostela - España Universidad Autónoma de Chile - Chile Univ Santiago de Compostela - España
10	Ortuso, Francesco	Hombre	Università degli studi Magna Graecia di Catanzaro - Italia Univ Magna Grcecia Catanzaro - Italia
11	Alcaro, Stefano	Hombre	Università degli studi Magna Graecia di Catanzaro - Italia Univ Magna Grcecia Catanzaro - Italia
12	Bagetta, Donatella	Mujer	Università degli studi Magna Graecia di Catanzaro - Italia Univ Magna Grcecia Catanzaro - Italia
13	Cagide, F.	Hombre	Universidade do Porto - Portugal Univ Porto - Portugal
14	Borges, Fernanda	Mujer	Universidade do Porto - Portugal Univ Porto - Portugal

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Financiamiento

Fuente
Fundação para a Ciência e a Tecnologia
COST Action
Foundation for Science and Technology (FCT)
FEDER/COMPETE
POPH
European Cooperation in Science and Technology
Programa Operacional Temático Factores de Competitividade

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Agradecimientos

Agradecimiento
This project is supported by Foundation for Science and Technology (FCT) and FEDER/COMPETE (Grants UID/QUI/00081/2020 and PTDC/MED-QUI/29164/2017, PT-OPENSCREEN-NORTE-01-0145-FEDER-085468). Thanks are due to FCT, POPH and FEDER/COMPETE for J Reis and F. Cagide grants. The authors also thank the COST action CA15135 (Multi-Target Paradigm for Innovative Ligand Identification in the Drug Discovery Process, MuTaLig) for support.
This project is supported by Foundation for Science and Technology (FCT) and FEDER/COMPETE (Grants UID/QUI/00081/2020 and PTDC/MED-QUI/29164/2017, PT-OPENSCREEN-NORTE-01-0145-FEDER-085468). Thanks are due to FCT, POPH and FEDER/COMPETE for J Reis and F. Cagide grants. The authors also thank the COST action CA15135 (Multi-Target Paradigm for Innovative Ligand Identification in the Drug Discovery Process, MuTaLig) for support.
This project is supported by Foundation for Science and Technology (FCT) and FEDER/COMPETE (Grants UID/QUI/00081/2020 and PTDC/MED-QUI/29164/2017, PT-OPENSCREEN-NORTE-01-0145-FEDER-085468) . Thanks are due to FCT, POPH and FEDER/COMPETE for J Reis and F. Cagide grants. The authors also thank the COST action CA15135 (Multi-Target Paradigm for Innovative Ligand Identification in the Drug Discovery Process, MuTaLig) for support.