Evaluation of enantioselective binding of fluoxetine to human serum albumin by ultrafiltration and CE – Experimental design and quality considerations

Escuder-Gilabert

et al. 2013

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The estimation of apparent binding constants and limit mobilities of the complexes of the enantiomers that characterize the interaction of enantiomers with chiral selectors, in this case highly sulfated β-cyclodextrin, was approached using a simple and economic electrophoretic modality, the complete filling technique (CFT) in counter-current mode. The enantiomers of eight psychoactive drugs, four antihistamines (dimethindene, promethazine, orphenadrine and terfenadine) and four antidepressants (bupropion, fluoxetine, nomifensine and viloxazine) were separated for the first time for this cyclodextrin (CD). Estimations of thermodynamic and electrophoretic enantioselectivies were also performed. Results indicate that, in general, thermodynamic enantioselectivity is the main component explaining the high resolution found, but also one case suggests that electrophoretic enantioselectivity itself is enough to obtain a satisfactory resolution. CFT results advantageous compared with conventional capillary electrophoresis (CE) and partial filling technique (PFT) for the study of the interaction between drugs and chiral selectors. It combines the use of a simple fitting model (as in CE), when the enantiomers do not exit the chiral selector plug during the separation (i.e. mobility of electroosmotic flow larger than mobility of CD), and drastic reduction of the consumption (and cost; ~99.7%) of the CD reagent (as in PFT) compared with the conventional CE.

Section: Resultsmentioning

confidence: 97%

“…In order to estimate K ′ and

μ_{i}^{CD}

Section: Resultsmentioning

confidence: 97%

Characterizing the interaction between enantiomers of eight psychoactive drugs and highly sulfated‐β‐cyclodextrin by counter‐current capillary electrophoresis

Escuder-Gilabert

et al. 2013

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“…For the NMF–HSA binding study, routines made/adapted in MATLAB® 4.2 were used for calculations, and the results generated were verified using EXCEL® and STATGRAPHICS®. The mathematical aspects were previously described in detail (Asensi‐Bernardi et al , , and references therein) and they are briefly described here. An accepted mathematical model describing the ligand–HSA interaction, applicable for each enantiomer in the case of a chiral molecule, considering m classes of independent active sites on HSA, each with n i binding sites, is:

r = \frac{b}{P} = \frac{D - d}{P} = \sum_{i = 1}^{m} n_{i} \frac{K_{i} d}{1 + K_{i} d}

…”

Section: Methodsmentioning

confidence: 99%

“…Most of the pharmacokinetic and pharmacological processes exhibit a high degree of enantioselectivity, owing to the characteristic chirality of biomolecules, and this results in differences between the pharmacological activities of drug enantiomers. In fact, very often one of them is most active while the other may produce side‐effects and even toxicity in some cases (Asensi‐Bernardi et al , ). Therefore, investigation of the enantioselectivity of drugs in their pharmacokinetic and pharmacological properties represents a great challenge for clinical pharmacology (Escuder Gilabert et al , ).…”

Section: Introductionmentioning

confidence: 99%

“…This methodology includes the incubation of drug–protein mixtures at the microliter level, their ultrafiltration through cellulose filters and the chiral analysis of the unbound fraction by EKC‐partial filling technique using heptakis‐2,3,6‐tri‐ O ‐methyl‐ β ‐cyclodextrin (TM‐ β ‐CD) as chiral selector. A recent mathematical approach of our group (Asensi‐Bernardi et al , ) was used to estimate affinity constants ( K 1 ) and verify the stoichiometry ( n 1 ), for both enantiomers of nomifensine, as well as to estimate their enantioselectivity ( ES ). Protein binding in percentage ( PB ) to HSA at physiological concentration levels and total plasma proteins were also estimated and compared with in vivo literature data.…”

Section: Introductionmentioning

confidence: 99%

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Electrokinetic chromatographic estimation of the enantioselective binding of nomifensine to human serum albumin and total plasma proteins

Sagrado

et al. 2012

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This report is the first evidence of enantioselective binding of nomifensine to human serum albumin (HSA) and plasma proteins. The overall process with HSA included: (i) consistent experimental design along two independent sessions; (ii) incubation of nomifensine-HSA designed mixtures; (iii) ultrafiltration for separating the unbound enantiomers fraction; (iv) electrokinetic chromatography (EKC) using heptakis-2,3,6-tri-O-methyl-β-cyclodextrin as chiral selector to provide experimental data for enantiomers (first, E1, and second, E2, eluted ones); and (v) a recent direct equation allowing univariate tests and robust statistics to provide consistent parameters and uncertainty. A significant enantioselectivity to HSA (2.7 ± 0.1) was encountered, related to a 1:1 stoichiometry and log affinity constants of 3.24 ± 0.10 and 3.67 ± 0.08 for E1 and E2, respectively. The protein binding (PB) estimated at physiological concentration levels was 40 ± 5 and 63 ± 4% for E1 and E2, respectively. The use of synthetic human sera allowed in vitro estimation of the total plasma PB for the racemate (61 ± 5%; coincident with in vivo values), and its enantiomers (58 ± 7 and 64 ± 4% for E1 and E2, respectively). Comparison allowed the relative importance of HSA respect to other plasma proteins for binding nomifensine to be established.

Determination of fluoxetine enantiomers in pharmaceutical formulations by electrokinetic chromatography–counter current technique

Fornet-Herrero

et al. 2012

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In this work, an electrokinetic chromatography-counter current procedure for the separation of fluoxetine enantiomers using highly sulfated β-cyclodextrin was optimized and applied to the determination of the enantiomers in three pharmaceutical formulations according to the matrix features. Quality criteria were applied to facilitate its transferability to testing laboratories. Fluoxetine was used therapeutically as the racemate, although a stereospecificity associated with its interactions with the neuronal serotonin-uptake carrier was demonstrated. In this context, the development of enantioselective methods for the chiral analysis of pharmaceuticals allowing stereoisomer ratio estimations has increasing interest in pharmaceutical industry. The proposed method allows the quantification of both enantiomers in less than 2 min with high resolution (R(s) = 2.4).