Direct Oral FXa Inhibitors Binding to Human Serum Albumin: Spectroscopic, Calorimetric, and Computational Studies.

Mariño-Ocampo, Nory; Rodríguez, Diego F; Guerra Díaz, Daniel; Zúñiga-Núñez, Daniel; Duarte, Yorley; Fuentealba, Denis; Zacconi, Flavia C

Mariño-Ocampo, Nory; Rodríguez, Diego F; Guerra Díaz, Daniel; Zúñiga-Núñez, Daniel; Duarte, Yorley; Fuentealba, Denis; Zacconi, Flavia C.

Afiliação

Mariño-Ocampo N; Escuela de Química, Facultad de Química y de Farmacia, Pontificia Universidad Católica de Chile, Santiago 7820436, Chile.
Rodríguez DF; Escuela de Química, Facultad de Química y de Farmacia, Pontificia Universidad Católica de Chile, Santiago 7820436, Chile.
Guerra Díaz D; Escuela de Química, Facultad de Química y de Farmacia, Pontificia Universidad Católica de Chile, Santiago 7820436, Chile.
Zúñiga-Núñez D; Escuela de Química, Facultad de Química y de Farmacia, Pontificia Universidad Católica de Chile, Santiago 7820436, Chile.
Duarte Y; Center for Bioinformatics and Integrative Biology, Facultad de Ciencias de la Vida, Universidad Andrés Bello, Santiago 8370035, Chile.
Fuentealba D; Escuela de Química, Facultad de Química y de Farmacia, Pontificia Universidad Católica de Chile, Santiago 7820436, Chile.
Zacconi FC; Escuela de Química, Facultad de Química y de Farmacia, Pontificia Universidad Católica de Chile, Santiago 7820436, Chile.

Int J Mol Sci ; 24(5)2023 Mar 03.

Article em En | MEDLINE | ID: mdl-36902328

RESUMO

Direct FXa inhibitors are an important class of bioactive molecules (rivaroxaban, apixaban, edoxaban, and betrixaban) applied for thromboprophylaxis in diverse cardiovascular pathologies. The interaction of active compounds with human serum albumin (HSA), the most abundant protein in blood plasma, is a key research area and provides crucial information about drugs' pharmacokinetics and pharmacodynamic properties. This research focuses on the study of the interactions between HSA and four commercially available direct oral FXa inhibitors, applying methodologies including steady-state and time-resolved fluorescence, isothermal titration calorimetry (ITC), and molecular dynamics. The HSA complexation of FXa inhibitors was found to occur via static quenching, and the complex formation in the ground states affects the fluorescence of HSA, with a moderate binding constant of 104 M-1. However, the ITC studies reported significantly different binding constants (103 M-1) compared with the results obtained through spectrophotometric methods. The suspected binding mode is supported by molecular dynamics simulations, where the predominant interactions were hydrogen bonds and hydrophobic interactions (mainly π-π stacking interactions between the phenyl ring of FXa inhibitors and the indole moiety of Trp214). Finally, the possible implications of the obtained results regarding pathologies such as hypoalbuminemia are briefly discussed.

Assuntos

Fator X; Albumina Sérica Humana; Tromboembolia Venosa; Humanos; Anticoagulantes; Sítios de Ligação; Calorimetria/métodos; Simulação de Acoplamento Molecular; Ligação Proteica; Albumina Sérica Humana/química; Espectrometria de Fluorescência; Termodinâmica; Fator X/antagonistas & inibidores

Palavras-chave

FXa inhibitors; apixaban; betrixaban; commercially available FXa inhibitors; direct oral FXa inhibitors; edoxaban; fluorescence; human serum albumin; isothermal titration calorimetry; molecular modeling; rivaroxaban

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Fator X / Tromboembolia Venosa / Albumina Sérica Humana Idioma: En Ano de publicação: 2023 Tipo de documento: Article

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