Literature DB >> 3210902

Cicletanine binding to human plasma proteins and erythrocytes, a particular HSA-drug interaction.

R Zini1, D Morin, P Jouenne, J P Tillement.   

Abstract

The binding of cicletanine to human serum, isolated proteins and red blood cells was studied in vitro by equilibrium dialysis. Our results show this drug is highly bound to serum (97.3%) at therapeutic levels. No saturation to the binding sites was seen. Human serum albumin was shown to mainly responsible for this binding (93.5%) with a saturable process characterized by one binding site with a moderate affinity (K = 75800 M-1) and a non saturable process with a low total affinity (nK = 6400 M-1). Like many basic lipophilic drugs, cicletanine showed a saturable binding to alpha-1-acid glycoprotein with one site and a moderate affinity (K = 38,800 M-1). Its binding to lipoproteins and red blood cells was weak and non saturable. Over the range of therapeutic concentrations, the unbound fraction in blood remains constant (3.6%). Moreover, interactions were studied using bilirubin and non esterified fatty acids at pathological concentrations and these endogenous compounds did not alter cicletanine binding human serum or to human serum albumin likewise cicletanine shared the diazepam-site on HSA but no inhibition could take place between cicletanine and the drugs sharing the same binding site in serum at therapeutic levels.

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Year:  1988        PMID: 3210902     DOI: 10.1016/0024-3205(88)90360-8

Source DB:  PubMed          Journal:  Life Sci        ISSN: 0024-3205            Impact factor:   5.037


  2 in total

1.  Nimesulide binding to components within blood.

Authors:  F Bree; P Nguyen; S Urien; E Albengres; A Macciocchi; J P Tillement
Journal:  Drugs       Date:  1993       Impact factor: 9.546

2.  Stability of the Hsp90 inhibitor 17AAG hydroquinone and prevention of metal-catalyzed oxidation.

Authors:  Wenchang Guo; David Siegel; David Ross
Journal:  J Pharm Sci       Date:  2008-12       Impact factor: 3.534

  2 in total

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