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Stacking and separation of enantiomers by acetonitrile-salt mixtures in micellar electrokinetic chromatography. | LitMetric

Stacking and separation of enantiomers by acetonitrile-salt mixtures in micellar electrokinetic chromatography.

Electrophoresis

Department of Chemistry and The Central Laboratory of the Institute of Molecular Technology for Drug Discovery and Synthesis, Hong Kong Baptist University, Kowloon Tong, Hong Kong, China.

Published: September 2003

AI Article Synopsis

  • The study introduces the "acetonitrile stacking" method as a novel technique for enhancing the preconcentration and separation of enantiomers using micellar electrokinetic chromatography (MEKC).
  • Investigations were conducted on how various experimental variables, particularly the influence of acetonitrile and salt in the sample matrix, affect the stacking and resolution of three pairs of optical isomers.
  • The results reveal that combining off-line salting-out solvent extraction with on-line acetonitrile stacking significantly boosts separation efficiency and peak resolution, especially when dealing with larger injection volumes.

Article Abstract

The feasibility of employing the "acetonitrile stacking" method in micellar electrokinetic chromatography (MEKC) for the on-line preconcentration and separation of enantiomers is demonstrated for the first time. The effects of various experimental parameters on the stacking and separation of three different pairs of optical isomers, i.e., two substituted naphthyl enantiomers and one dansylated-DL-amino acid, were examined. In particular, the effectiveness of the addition of acetonitrile and salt in the sample matrix to induce narrowing of the analyte bands was investigated in the presence of sodium cholate as the chiral surfactant micelle in the separation buffer. For example, it was found that the presence of both acetonitrile and 1% NaCl in the sample matrix (volume ratio = 2:1) led to a significant improvement of the peak height and resolution for the MEKC separation of a pair of R(-)/S(+)-1,1'-binaphthyl diyl hydrogen phosphate enantiomers when the injection sample size was relatively large (e.g., 12% capillary volume). Furthermore, the feasibility of combining salting-out solvent extraction (off-line) and acetonitrile stacking (on-line) as a novel approach for sample preconcentration in capillary electrophoresis was also demonstrated.

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Source
http://dx.doi.org/10.1002/elps.200305549DOI Listing

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