Quantitative parameters of complexes of tris(1-alkylindol-3-yl)methylium salts with serum albumin: Relevance for the design of drug candidates

Quantitative parameters of complexes of tris(1-alkylindol-3-yl)methylium salts with serum albumin: Relevance for the design of drug candidates

Triarylmethane derivatives are extensively investigated as antitumor and antibacterial drug candidates alone and as photoactivatable compounds. In the series of tris(1-alkylindol-3-yl)methylium salts (TIMs) these two activities differed depending on the length of N-alkyl chain, with C4–5 derivatives...

Ausführliche Beschreibung

Gespeichert in:
Bibliographische Detailangaben
Veröffentlicht in:Journal of photochemistry and photobiology. B, Biology Biology, 2016-09, Vol.162, p.570-576
Hauptverfasser: Durandin, Nikita A., Tsvetkov, Vladimir B., Bykov, Evgeny E., Kaluzhny, Dmitry N., Lavrenov, Sergey N., Tevyashova, Anna N., Preobrazhenskaya, Maria N.
Format: Artikel
Sprache:eng
Schlagworte:
Binding Sites
Circular Dichroism
Human serum albumin
Humans
Ibuprofen - chemistry
Ibuprofen - metabolism
Indoles - chemistry
Indoles - metabolism
Molecular docking
Molecular Docking Simulation
Protein Binding
Protein Structure, Tertiary
Salts - chemistry
Serum Albumin - chemistry
Serum Albumin - metabolism
Spectrometry, Fluorescence
Spectroscopy
Thermodynamics
Triarylmethane dyes
Triindolylmethane derivatives
Warfarin - chemistry
Warfarin - metabolism
Online-Zugang:Volltext
Tags: Tag hinzufügen
Keine Tags, Fügen Sie den ersten Tag hinzu!
Beschreibung
Zusammenfassung:Triarylmethane derivatives are extensively investigated as antitumor and antibacterial drug candidates alone and as photoactivatable compounds. In the series of tris(1-alkylindol-3-yl)methylium salts (TIMs) these two activities differed depending on the length of N-alkyl chain, with C4–5 derivatives being the most potent compared to the shorter or longer chain analogs and to the natural compound turbomycin A (no N-substituent). Given that the human serum albumin (HSA) is a major transporter protein with which TIMs can form stable complexes, and that the formation of these complexes might be advantageous for phototoxicity of TIMs we determined the quantitative parameters of TIMs-HSA binding using spectroscopic methods and molecular docking. TIMs bound to HSA (1:1 stoichiometry) altered the protein's secondary structure by changing the α-helix/β-turn ratio. The IIa subdomain (Sudlow site I) is the preferred TIM binding site in HSA as determined in competition experiments with reference drugs ibuprofen and warfarin. The values of binding constants increased with the number of CH2 groups from 0 to 6 and then dropped down for C10 compound, a dependence similar to the one observed for cytocidal potency of TIMs. We tend to attribute this non-linear dependence to an interplay between hydrophobicity and steric hindrance, the two key characteristics of TIMs-HSA complexes calculated in the molecular docking procedure. These structure-activity relationships provide evidence for rational design of TIMs-based antitumor and antimicrobial drugs. [Display omitted] •Triindolylmethylium salts (TIMs) are selective HSA subdomain IIa ligands.•A 1:1 host-guest model of complex formation is confirmed.•TIMs alter HSA conformation by decreasing the α-helix content.•Hydrophobic interactions largely contribute to the TIMs-HSA complex formation.•N-residue number ideal for both binding and cytotoxicity is similar but not identical.
ISSN:1011-1344
1873-2682
DOI:10.1016/j.jphotobiol.2016.07.017