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Micellar electrokinetic chromatography information


Distribution of analytes (A) in micellar electrokinetic chromatography based on their hydrophobicity.

Micellar electrokinetic chromatography (MEKC) is a chromatography technique used in analytical chemistry. It is a modification of capillary electrophoresis (CE), extending its functionality to neutral analytes,[1] where the samples are separated by differential partitioning between micelles (pseudo-stationary phase) and a surrounding aqueous buffer solution (mobile phase).[2]

The basic set-up and detection methods used for MEKC are the same as those used in CE. The difference is that the solution contains a surfactant at a concentration that is greater than the critical micelle concentration (CMC). Above this concentration, surfactant monomers are in equilibrium with micelles.

In most applications, MEKC is performed in open capillaries under alkaline conditions to generate a strong electroosmotic flow. Sodium dodecyl sulfate (SDS) is the most commonly used surfactant in MEKC applications. The anionic character of the sulfate groups of SDS causes the surfactant and micelles to have electrophoretic mobility that is counter to the direction of the strong electroosmotic flow. As a result, the surfactant monomers and micelles migrate quite slowly, though their net movement is still toward the cathode.[3] During a MEKC separation, analytes distribute themselves between the hydrophobic interior of the micelle and hydrophilic buffer solution as shown in figure 1.

Analytes that are insoluble in the interior of micelles should migrate at the electroosmotic flow velocity, , and be detected at the retention time of the buffer, . Analytes that solubilize completely within the micelles (analytes that are highly hydrophobic) should migrate at the micelle velocity, , and elute at the final elution time, .[4]

  1. ^ Hancu, Gabriel; Rusu, Aura; Simon, Brigitta; Mircia, Eleonora; Gyeresi, Arpad (2013). "Principles of Micellar Electrokinetic Capillary Chromatography Applied in Pharmaceutical Analysis". Advanced Pharmaceutical Bulletin. 3 (1): 1–8. doi:10.5681/apb.2013.001. PMC 3846027. PMID 24312804.
  2. ^ Terabe, S.; Otsuka, K.; Ichikawa, K.; Tsuchiya, A.; Ando, T. (1984). "Electrokinetic separations with micellar solutions and open-tubular capillaries". Anal. Chem. 56: 111–113. doi:10.1021/ac00265a031.
  3. ^ Baker, D.R. "Capillary Electrophoresis" John Wiley & Sons, Inc.: New York, 1995.
  4. ^ Terabe, S.; Otsuka, K.; Ichikawa, K.; Tsuchiya, A.; Ando, T. (1984). "Electrokinetic separations with micellar solutions and open-tubular capillaries". Anal. Chem. 56: 113. doi:10.1021/ac00265a031.

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