Sequential design of experiments approach for the multiproduct analysis of cholesterol‐lowering drugs by ultra‐high‐performance supercritical fluid chromatography

Sequential design of experiments approach for the multiproduct analysis of cholesterol‐lowering drugs by ultra‐high‐performance supercritical fluid chromatography

A multiproduct approach toward method development is presented for a fast and reliable analysis of the eight most important cholesterol‐lowering drugs via ultra‐high‐performance supercritical fluid chromatography. A two‐step approach based on design of experiments was applied: (1) selection of the s...

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Veröffentlicht in:Journal of separation science 2020-11, Vol.43 (22), p.4234-4242
Hauptverfasser: Santana, Igor Miranda, Jardim, Isabel Cristina Sales Fontes, Breitkreitz, Márcia Cristina
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Sprache:eng
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Acetonitrile
Cholesterol
Chromatography
Design of experiments
Design optimization
Drugs
Economic conditions
Elution
Ethanol
Flow velocity
Ions
pharmaceutical analysis
statins
Supercritical fluids
Toruses
ultra‐high performance supercritical fluid chromatography
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container_end_page 4242
container_issue 22
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container_title Journal of separation science
container_volume 43
creator Santana, Igor Miranda
Jardim, Isabel Cristina Sales Fontes
Breitkreitz, Márcia Cristina
description A multiproduct approach toward method development is presented for a fast and reliable analysis of the eight most important cholesterol‐lowering drugs via ultra‐high‐performance supercritical fluid chromatography. A two‐step approach based on design of experiments was applied: (1) selection of the stationary phase, organic modifier, and diluent in the mobile phase through a multilevel categorical design and (2) optimization of the elution strength by varying the pressure, temperature, and gradient using a central composite design. Finally, the flow rate was adjusted. The first design selected UPC2 Torus 1‐AA as the column, ethanol:water as the organic modifier, and acetonitrile:ethanol 3:2 v/v as the diluent. The results led to a pressure, column temperature, and gradient elution of 14.83 MPa, 42°C, and 5–15.5% of ethanol:water in CO2, respectively. The flow rate was set at 1.8 mL/min, providing a total analysis time of 4 min. This multiproduct method was validated and applied to 11 different commercial products available in the Brazilian market, and it was found to be accurate, with r > 0.990, recoveries between 95 and 105%, and precision not higher than 5.4%. Therefore, this method was shown to be a greener alternative for the analysis of these pharmaceuticals.
doi_str_mv 10.1002/jssc.202000702
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subjects Acetonitrile
Cholesterol
Chromatography
Design of experiments
Design optimization
Drugs
Economic conditions
Elution
Ethanol
Flow velocity
Ions
pharmaceutical analysis
statins
Supercritical fluids
Toruses
ultra‐high performance supercritical fluid chromatography
title Sequential design of experiments approach for the multiproduct analysis of cholesterol‐lowering drugs by ultra‐high‐performance supercritical fluid chromatography
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