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Investigation of the interaction between S-isoalkyl derivatives of the thiosalicylic acid and human serum albumin.
Vesovic, Marina; Jelic, Ratomir; Nikolic, Milos; Nedeljkovic, Nikola; Zivanovic, Ana; Bukonjic, Andriana; Mrkalic, Emina; Radic, Gordana; Ratkovic, Zoran; Kljun, Jakob; Tomovic, Dusan.
Afiliação
  • Vesovic M; University of Kragujevac, Faculty of Medical Sciences, Department of Pharmacy, Svetozara Markovica 69, Kragujevac, Serbia.
  • Jelic R; University of Kragujevac, Faculty of Medical Sciences, Department of Pharmacy, Svetozara Markovica 69, Kragujevac, Serbia.
  • Nikolic M; University of Kragujevac, Faculty of Medical Sciences, Department of Pharmacy, Svetozara Markovica 69, Kragujevac, Serbia.
  • Nedeljkovic N; University of Kragujevac, Faculty of Medical Sciences, Department of Pharmacy, Svetozara Markovica 69, Kragujevac, Serbia.
  • Zivanovic A; University of Kragujevac, Faculty of Medical Sciences, Department of Pharmacy, Svetozara Markovica 69, Kragujevac, Serbia.
  • Bukonjic A; University of Kragujevac, Faculty of Medical Sciences, Department of Pharmacy, Svetozara Markovica 69, Kragujevac, Serbia.
  • Mrkalic E; University of Kragujevac, Institute for Information Technologies, Department of Science, Jovana Cvijica bb, Kragujevac, Serbia.
  • Radic G; University of Kragujevac, Faculty of Medical Sciences, Department of Pharmacy, Svetozara Markovica 69, Kragujevac, Serbia.
  • Ratkovic Z; University of Kragujevac, Faculty of Science, Department of Chemistry, Radoja Domanovica 12, Kragujevac, Serbia.
  • Kljun J; University of Ljubljana, Faculty of Chemistry and Chemical Technology, Vecna pot 113, Ljubljana, Slovenia.
  • Tomovic D; University of Kragujevac, Faculty of Medical Sciences, Department of Pharmacy, Svetozara Markovica 69, Kragujevac, Serbia.
J Biomol Struct Dyn ; : 1-14, 2024 Jan 08.
Article em En | MEDLINE | ID: mdl-38192057
ABSTRACT
S-isoalkyl derivatives of thiosalicylic acid (isopropyl-(L1), isobutyl-(L2) and isoamyl-(L3)) were selected in order to investigate the binding interaction with the human serum albumin (HSA) using different spectroscopic methods and molecular docking simulation. Association constants and number of binding sites were used to analyze the quenching mechanism. The experimental results showed that the fluorescence quenching of HSA by L1, L2 and L3 occurs because of static quenching and that binding processes were spontaneous, with the leading forces in bonding by hydrogen bonding, hydrophobic interactions, and electrostatic interactions. Fluorescence spectroscopy, UV-Vis spectroscopy and synchronous fluorescence spectroscopy showed that ligands (L1, L2 and L3) can bind to HSA and that the binding of ligands induced some microenvironmental and conformational changes in HSA. The calculated distance between the donor and the acceptor according to fiFörster's theory confirms the energy transfer efficiency between the acceptor and HSA. Results of site marker competitive experiments showed that the tested compounds bind to HSA in domain IIA (Site I). Molecular dynamics and docking calculations demonstrated that L3 binds to the Sudlow site I of HSA with lower values of binding energies compared to L1 and L2, indicating the formation of the most stable ligand-HSA complex. Understanding the binding mechanisms of S-isoalkyl derivatives of the thiosalicylic acid to HSA may provide valuable data for the future studies of their biological activity and application as potential antitumor drugs.Communicated by Ramaswamy H. Sarma.
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Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2024 Tipo de documento: Article

Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2024 Tipo de documento: Article