Title : ( Spectroscopic and molecular modeling study on the separate and simultaneous bindings of alprazolam and fluoxetine hydrochloride to human serum albumin (HSA): W ith the aim of the drug interactions probing )
Authors: FAEZE DANKOOB , Mohammad Reza Housaindokht , Ahmad Asoodeh , Omid Rajabi , Zeinab Rouhbakhsh Zaeri , asma verdian ,Access to full-text not allowed by authors
Abstract
The objective of the present research is to study the interaction of separate and simultaneous of alprazolam (ALP) and fluoxetine hydrochloride (FLX) with human serum albumin (HSA) in phosphate buffer (pH 7.4) using different kinds of spectroscopic, cyclic voltammetry and molecular modeling techniques.The absorbance spectra of protein, drugs and protein-drug showed complex formation between the drugs and HSA. Fluorescence analysis demonstrated that ALP and FLX could quench the fluorescence spectrum of HSA and demonstrated the conformational change of HSA in the presence of both drugs. Also, fluorescence quenching mechanism of HSA–drug complexes both separately and simultaneously was suggested as static quenching. The analysis of UV absorption data and the fluorescence quenching of HSA in the binary and ternary systems showed that FLX decreased the binding affinity between ALP and HSA. On the contrary, ALP increased the binding affinity of FLX and HSA. The results of synchronous fluorescence and three-dimensional fluorescence spectra indicated that the binding of drugs to HSA would modify the microenvironment around the Trp and Tyr residues and the conformation of HSA. The distances between Trp residue and the binding sites of the drugs were estimated according to the Förster theory, and it was demonstrated that non-radiative energy transfer from HSA to the drugs occurred with a high probability. Moreover, according to CV measurements, the decrease of peak current in the cyclic voltamogram of the both drugs in the presence of HSA revealed that they interacted with albumin and binding constants were calculated for binary systems which were in agreement with the binding constants obtained from UV absorption and fluorescence spectroscopy. The prediction of the best binding sites of ALP and FLX in binary and ternary systems in molecular modeling approach was done using of Gibbs free energy
Keywords
, Human serum albumin, Alprazolam, Fluoxetine hydrochloride, Spectroscopy , Cyclic voltammetry Molecular docking@article{paperid:1043312,
author = {DANKOOB, FAEZE and Housaindokht, Mohammad Reza and Asoodeh, Ahmad and Omid Rajabi and Rouhbakhsh Zaeri, Zeinab and Verdian, Asma},
title = {Spectroscopic and molecular modeling study on the separate and simultaneous bindings of alprazolam and fluoxetine hydrochloride to human serum albumin (HSA): W ith the aim of the drug interactions probing},
journal = {Spectrochimica Acta Part A: Molecular and Biomolecular Spectroscopy},
year = {2015},
volume = {137},
month = {January},
issn = {1386-1425},
pages = {1106--1119},
numpages = {13},
keywords = {Human serum albumin، Alprazolam،Fluoxetine hydrochloride،Spectroscopy ،Cyclic voltammetry
Molecular docking},
}
%0 Journal Article
%T Spectroscopic and molecular modeling study on the separate and simultaneous bindings of alprazolam and fluoxetine hydrochloride to human serum albumin (HSA): W ith the aim of the drug interactions probing
%A DANKOOB, FAEZE
%A Housaindokht, Mohammad Reza
%A Asoodeh, Ahmad
%A Omid Rajabi
%A Rouhbakhsh Zaeri, Zeinab
%A Verdian, Asma
%J Spectrochimica Acta Part A: Molecular and Biomolecular Spectroscopy
%@ 1386-1425
%D 2015