Evaluating the Capacity of Human Serum Albumin to Reduce Non-Specific Binding of Meloxicam in the Ultrafiltration Process

IMRE, SILVIA

doi:10.31925/farmacia.2021.6.7

Cited by 3 publications

(3 citation statements)

References 35 publications

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“…Regarding the main known disadvantage of the method represented by the nonspecific binding (NSB) of drugs to parts of the UF device, we considered it to be negligible in our study, taking into consideration the literature reports made by Wang and Williams, who have shown that even in the case of highly lipophilic compounds, NSB is not a limitation when drugs are incubated with the UF device in protein matrices because of their ability to block the NSB sites 37 . This theory was also tested and proven in our previous experience 38 …”

Section: Resultsmentioning

confidence: 96%

“…37 This theory was also tested and proven in our previous experience. 38 The concentrations of carvedilol for the binding assays ranges were chosen taking into account the maximum plasma concentrations detected in patients reported in previous studies. Depending on the dose regimen and type of pharmaceutical formulation administered (immediate release, controlled release), a great variability regarding the maximum plasma concentration was often observed with ranges that could go from a value below 7 ng/mL to a value over 350 ng/mL.…”

Section: Determination Of the Degree Of Binding Of Cvd And Its Enanti...mentioning

confidence: 99%

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Enantioselective binding of carvedilol to human serum albumin and alpha‐1‐acid glycoprotein

et al. 2023

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Carvedilol, a highly protein‐bound beta‐blocker, is used in therapy as a racemic mixture of its two enantiomers that exhibit different pharmacological activity. The aim of this study was to evaluate the stereoselective nature of its binding to the two major plasma proteins: albumin and alpha‐1‐acid glycoprotein. The determination of the plasma protein‐binding degree for carvedilol and its enantiomers was achieved using ultrafiltration for the separation of the free fraction, followed by LC‐MS/MS quantification, using two different developed and validated methods in terms of stationary phase: achiral C18 type and chiral ovomucoid type. Furthermore, molecular docking methods were applied in order to investigate and to better understand the mechanism of protein‐binding for S‐(−)‐ and R‐(+)‐carvedilol. A difference in the binding behavior of the two enantiomers to the plasma proteins was observed when taken individually, with R‐(+)‐carvedilol having a higher affinity for albumin and S‐(−)‐carvedilol for alpha‐1‐acid glycoprotein. However, in the case of the racemic mixture, the binding of the S enantiomer to alpha‐1‐acid glycoprotein seemed to be influenced by the presence of its antipode, although no such influence was observed in the case of albumin. The results raise the question of a binding competition between the two enantiomers for alpha‐1‐acid glycoprotein.

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Section: Resultsmentioning

confidence: 96%

Section: Determination Of the Degree Of Binding Of Cvd And Its Enanti...mentioning

confidence: 99%

Enantioselective binding of carvedilol to human serum albumin and alpha‐1‐acid glycoprotein

et al. 2023

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“…According to the data sheet of the product, only the Centrifree devices were specifically designed for separating free from bound microsolutes in biological samples, but other PPB studies report good results also obtained using the Amicon Ultra devices, initially designed for concentration of different components of biological samples (antigens, antibodies, enzymes, nucleic acids, microorganisms), protein extraction and purification (Du et al, 2014;Imre et al, 2021).…”

Section: Classical Ultrafiltration Methodsmentioning

confidence: 99%

Comparison of Different Ultrafiltration Devices for the Study of Plasma Protein Binding of Carvedilol

Toma,

Farczádi,

Ion

et al. 2023

Acta Biologica Marisiensis

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The aim of the present study was to assess the suitability of different Amicon Ultra and Centrifree ultrafiltration devices for the study of the plasma protein binding process in the case of carvedilol, a highly protein-bound and lipophilic beta-blocking agent. Samples at different levels of concentration were prepared in both proteic and non-proteic matrices (human plasma, 5% human serum albumin solution and saline solution) and subjected to the classical ultrafiltration method using the different devices considered. Furthermore, an attempt to apply a previously described modified ultrafiltration method was also made. The analysis and quantification was achieved using a validated LC-MS/MS method. For the Centrifree devices, the determined unbound fractions of carvedilol and the corresponding binding degree were in accordance to literature data, while for the Amicon Ultra devices a great degree of carvedilol adsorbtion to the sample reservoir was observed, the analyte not being detected in the ultrafiltrate samples. Thus, it was further demonstrated that the type of ultrafiltration device used has a significant influence on the outcome of a plasma protein binding study. In the case of carvedilol, the evaluation of the protein binding interaction could be achieved using the Centrifree ultrafiltration devices, but not the Amicon Ultra devices.

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Hollow Fiber-in-Syringe Equilibrium Sampling Through Supported-Liquid Membrane for Evaluation of Drug-Plasma Binding

Barri,

Ramzi,

Idkaidek

et al. 2024

Bioanalysis

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Evaluating the Capacity of Human Serum Albumin to Reduce Non-Specific Binding of Meloxicam in the Ultrafiltration Process

Cited by 3 publications

References 35 publications

Enantioselective binding of carvedilol to human serum albumin and alpha‐1‐acid glycoprotein

Enantioselective binding of carvedilol to human serum albumin and alpha‐1‐acid glycoprotein

Comparison of Different Ultrafiltration Devices for the Study of Plasma Protein Binding of Carvedilol

Hollow Fiber-in-Syringe Equilibrium Sampling Through Supported-Liquid Membrane for Evaluation of Drug-Plasma Binding

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