KMID : 0043320120350040671
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Archives of Pharmacal Research 2012 Volume.35 No. 4 p.671 ~ p.681
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Chiral discrimination of sibutramine enantiomers by capillary electrophoresis and proton nuclear magnetic resonance spectroscopy
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Lee Yong-Jae
Choi Seung-Ho Lee Jin-Hoo Nguyen NgocVan Thi Lee Kyung-Ran Kang Jong-Seong Mar Woong-Chon Kim Kyeong-Ho
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Abstract
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Capillary electrophoresis (CE) and proton nuclear magnetic resonance spectroscopy (1H-NMR) have been used to discriminate the enantiomers of sibutramine using cyclodextrin derivatives. Possible correlation between CE and 1H-NMR was examined. Good correlation between the 1H-NMR shift non-equivalence data for sibutramine and the degree of enantioseparation in CE was observed. In CE study, a method of enantiomeric separation and quantitation of sibutramine was developed using enantiomeric standards. The method was based on the use of 50 mM of phosphate buffer of pH 3.0 with 10 mM of methyl-beta-cyclodextrin (M-¥â-CD). 0.05% of LOD, 0.2% of LOQ for S-sibutramine enantiomer was achieved, and the method was validated and applied to the quantitative determination of sibutramine enantiomers in commercial drugs. On a 600 MHz 1H-NMR analysis, enantiomer signal separation of sibutramine was obtained by fast diastereomeric interaction with a chiral selector M-¥â-CD. For chiral separation and quantification, N-methyl proton peaks (at 2.18 ppm) were selected because of its being singlet and simple for understanding of diastereomeric interaction. Effects of temperature and concentration of chiral selector on enantiomer signal separation were investigated. The optimum condition was 0.5 mg/mL of sibutramine and 10 mg/mL of M-¥â-CD at 10¡ÆC. Distinguishment of 0.5% of S-sibutramine in R-sibutramine was found to be possible by 1H-NMR with M-¥â-CD as chiral selector. Host-guest interaction between sibutramine and M-¥â-CD was confirmed by 1H-NMR studies and CE studies. A Structure of the inclusion complex was proposed considering 1H-NMR and 2D ROESY studies.
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KEYWORD
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Sibutramine, Enantiomer, Chiral discrimination, Methyl-¥â-cyclodextrin, 1HNMR, Capillary electrophoresis
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