Ligand and structure-based discovery of phosphorus-containing compounds as potential metalloproteinase inhibitors.

Cañizares-Carmenate, Y; Perera-Sardiña, Y; Marrero-Ponce, Y; Díaz-Amador, R; Torrens, F; Castillo-Garit, J A

Cañizares-Carmenate, Y; Perera-Sardiña, Y; Marrero-Ponce, Y; Díaz-Amador, R; Torrens, F; Castillo-Garit, J A.

Afiliación

Cañizares-Carmenate Y; Unit of Computer-Aided Molecular ''Biosilico" Discovery and Bioinformatic Research (CAMD-BIR Unit), Departamento de Farmacia, Facultad de Química-Farmacia, Universidad Central ''Marta Abreu" de Las Villas, Santa Clara, Cuba.
Perera-Sardiña Y; Departamento de Ciencias Básicas Biomédicas, Facultad de Ciencias de la Salud, Universidad de Talca, Talca, Chile.
Marrero-Ponce Y; Grupo de Medicina Molecular Y Traslacional (MeM & T), Escuela de Medicina, Universidad San Francisco de Quito, Edificio de Especialidades Médicas, Quito, Ecuador.
Díaz-Amador R; Laboratorio de Bioinformática y Química Computacional, Escuela de Química y Farmacia, Facultad de Medicina, Universidad Católica de Maule, Maule, Chile.
Torrens F; Institut Universitari de Ciència Molecular, Universitat de València, Edifici d'Instituts de Paterna, València, Spain.
Castillo-Garit JA; Instituto Universitario de Investigación y Desarrollo Tecnológico (IDT), Universidad Tecnológica Metropolitana, Santiago, Chile.

SAR QSAR Environ Res ; 35(3): 219-240, 2024 Mar.

Article en En | MEDLINE | ID: mdl-38380444

ABSTRACT

ABSTRACT

In this study, a methodology is proposed, combining ligand- and structure-based virtual screening tools, for the identification of phosphorus-containing compounds as inhibitors of zinc metalloproteases. First, we use Dragon molecular descriptors to develop a Linear Discriminant Analysis classification model, which is widely validated according to the OECD principles. This model is simple, robust, stable and has good discriminating power. Furthermore, it has a defined applicability domain and it is used for virtual screening of the DrugBank database. Second, docking experiments are carried out on the identified compounds that showed good binding energies to the enzyme thermolysin. Considering the potential toxicity of phosphorus-containing compounds, their toxicological profile is evaluated according to Protox II. Of the five molecules evaluated, two show carcinogenic and mutagenic potential at small LD50, not recommended as drugs, while three of them are classified as non-toxic, and could constitute a starting point for the development of new vasoactive metalloprotease inhibitor drugs. According to molecular dynamics simulation, two of them show stable interactions with the active site maintaining coordination with the metal. A high agreement is evident between QSAR, docking and molecular dynamics results, demonstrating the potentialities of the combination of these tools.

Asunto(s)

Simulación de Dinámica Molecular; Relación Estructura-Actividad Cuantitativa; Simulación del Acoplamiento Molecular; Ligandos; Metaloproteasas; Fósforo

Palabras clave

Docking; linear discriminant analysis; molecular dynamics; thermolysin inhibitor; virtual screening; zinc metalloproteinase

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Texto completo: 1 Bases de datos: MEDLINE Asunto principal: Relación Estructura-Actividad Cuantitativa / Simulación de Dinámica Molecular Idioma: En Revista: SAR QSAR Environ Res Año: 2024 Tipo del documento: Article País de afiliación: Cuba

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