Investigation of deep eutectic solvents as additives to β‐CD for enantiomeric separations of Zopiclone, Salbutamol, and Amlodipine by CE

The enantioseparation of chiral drugs via CE was first investigated using β‐CD as chiral additive and deep eutectic solvents (DESs) as auxiliary additive. The results showed that improved separation of tested chiral drugs was obtained in the presence of DESs and β‐CD compared to the single β‐CD sepa...

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Published inElectrophoresis Vol. 40; no. 15; pp. 1992 - 1995
Main Authors Mu, Yi, Wu, Xi, Huang, Yan‐Ping, Liu, Zhao‐Sheng
Format Journal Article
LanguageEnglish
Published Germany Wiley Subscription Services, Inc 01.08.2019
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ISSN0173-0835
1522-2683
1522-2683
DOI10.1002/elps.201900067

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Abstract The enantioseparation of chiral drugs via CE was first investigated using β‐CD as chiral additive and deep eutectic solvents (DESs) as auxiliary additive. The results showed that improved separation of tested chiral drugs was obtained in the presence of DESs and β‐CD compared to the single β‐CD separation system. With the optimized condition, resolutions of DESs applied β‐CD separation system for rac‐Zopiclone, rac‐Salbutamol, and rac‐Amlodipine increased 3–4.2 times as single β‐CD separation system. The resolutions reached 4.74, 6.37, and 9.67, respectively. The results demonstrate that DESs are viable additives to CD system in CE for the separation of the chiral drugs.
AbstractList The enantioseparation of chiral drugs via CE was first investigated using β‐CD as chiral additive and deep eutectic solvents (DESs) as auxiliary additive. The results showed that improved separation of tested chiral drugs was obtained in the presence of DESs and β‐CD compared to the single β‐CD separation system. With the optimized condition, resolutions of DESs applied β‐CD separation system for rac‐Zopiclone, rac‐Salbutamol, and rac‐Amlodipine increased 3–4.2 times as single β‐CD separation system. The resolutions reached 4.74, 6.37, and 9.67, respectively. The results demonstrate that DESs are viable additives to CD system in CE for the separation of the chiral drugs.
The enantioseparation of chiral drugs via CE was first investigated using β ‐CD as chiral additive and deep eutectic solvents (DESs) as auxiliary additive. The results showed that improved separation of tested chiral drugs was obtained in the presence of DESs and β ‐CD compared to the single β ‐CD separation system. With the optimized condition, resolutions of DESs applied β ‐CD separation system for rac ‐Zopiclone, rac ‐Salbutamol, and rac ‐Amlodipine increased 3–4.2 times as single β ‐CD separation system. The resolutions reached 4.74, 6.37, and 9.67, respectively. The results demonstrate that DESs are viable additives to CD system in CE for the separation of the chiral drugs.
The enantioseparation of chiral drugs via CE was first investigated using β-CD as chiral additive and deep eutectic solvents (DESs) as auxiliary additive. The results showed that improved separation of tested chiral drugs was obtained in the presence of DESs and β-CD compared to the single β-CD separation system. With the optimized condition, resolutions of DESs applied β-CD separation system for rac-Zopiclone, rac-Salbutamol, and rac-Amlodipine increased 3-4.2 times as single β-CD separation system. The resolutions reached 4.74, 6.37, and 9.67, respectively. The results demonstrate that DESs are viable additives to CD system in CE for the separation of the chiral drugs.The enantioseparation of chiral drugs via CE was first investigated using β-CD as chiral additive and deep eutectic solvents (DESs) as auxiliary additive. The results showed that improved separation of tested chiral drugs was obtained in the presence of DESs and β-CD compared to the single β-CD separation system. With the optimized condition, resolutions of DESs applied β-CD separation system for rac-Zopiclone, rac-Salbutamol, and rac-Amlodipine increased 3-4.2 times as single β-CD separation system. The resolutions reached 4.74, 6.37, and 9.67, respectively. The results demonstrate that DESs are viable additives to CD system in CE for the separation of the chiral drugs.
Author Wu, Xi
Liu, Zhao‐Sheng
Huang, Yan‐Ping
Mu, Yi
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Keywords β-CD
Capillary electrophoresis
Deep eutectic solvents
Chiral separation
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Snippet The enantioseparation of chiral drugs via CE was first investigated using β‐CD as chiral additive and deep eutectic solvents (DESs) as auxiliary additive. The...
The enantioseparation of chiral drugs via CE was first investigated using β ‐CD as chiral additive and deep eutectic solvents (DESs) as auxiliary additive. The...
The enantioseparation of chiral drugs via CE was first investigated using β-CD as chiral additive and deep eutectic solvents (DESs) as auxiliary additive. The...
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StartPage 1992
SubjectTerms Additives
Albuterol - analysis
Albuterol - chemistry
Albuterol - isolation & purification
Amlodipine - analysis
Amlodipine - chemistry
Amlodipine - isolation & purification
Azabicyclo Compounds - analysis
Azabicyclo Compounds - chemistry
Azabicyclo Compounds - isolation & purification
beta-Cyclodextrins - chemistry
Capillary electrophoresis
Ceramics industry
Chiral separation
Deep eutectic solvents
Drugs
electrophoresis
Electrophoresis, Capillary - methods
Piperazines - analysis
Piperazines - chemistry
Piperazines - isolation & purification
Separation
Solvents
Solvents - chemistry
Stereoisomerism
β‐CD
Title Investigation of deep eutectic solvents as additives to β‐CD for enantiomeric separations of Zopiclone, Salbutamol, and Amlodipine by CE
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