Enantioresolution of certain pharmaceuticals by liquid chromatography

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Enantioresolution of pharmaceuticals and biologically important compounds continues to be important and challenging task in academia and industry. Sensitive, cost-effective and reproducible methods are reported for chiral separation of such compounds, namely (R,S)-mexiletine, (R,S)-baclofen, -blockers (i.e., (R,S)-atenolol, (R,S)-propranolol, (R,S)-bisoprolol, (R,S)-metoprolol and (R,S)-carvedilol), DL-amino acids (both proteinogenic and non-proteinogenic) and certain chiral aldehydes and ketones. Indirect approach of enantioresolution offers several advantages in comparison to direct approach. These include possibility of synthesis of chiral derivatizing reagents (CDRs) that could react easily with the functional group of the analyte, availability of certain CDRs commercially, excellent separation and detection possibilities of the resulting diastereomers, easy optimization of chromatographic conditions, and the prospect of using relatively inexpensive achiral columns. Cyanuric chloride and 1,5-Di uoro-2,4-dinitrobenzene serve as excellent structural platforms to synthesize a wide spectrum of CDRs by using amino acids and their amides as chiral auxiliaries.

Autorentext

Dr. Shuchi Dixit is currently an International Research Professor in the Department of Chemistry/College of Sciences at Yeungnam University, South Korea. She has obtained Ph.D.(Chemistry) and M.Tech. (Advanced Chemical Analysis) degrees from Indian Institute of Technology, Roorkee, India.

Weitere Informationen

  • Allgemeine Informationen
    • GTIN 09783848443741
    • Sprache Englisch
    • Auflage Aufl.
    • Genre Chemie
    • Größe H220mm x B220mm
    • Jahr 2012
    • EAN 9783848443741
    • Format Kartonierter Einband (Kt)
    • ISBN 978-3-8484-4374-1
    • Titel Enantioresolution of certain pharmaceuticals by liquid chromatography
    • Autor Shuchi Dixit
    • Untertitel Chiral separation of certain pharmaceutically and biologically important compounds
    • Herausgeber LAP Lambert Academic Publishing
    • Anzahl Seiten 232

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