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- A practical approach to simultaneously determine both the concentration and enantiomeric composition of a wide variety of chiral compounds.
- The method employs simple measurements, is fast, uses inexpensive materials, and produces minimal wastage.
- A notable solution for High-throughput screening, specifically in the pharmaceutical domain.
OVERVIEW
Georgetown University researchers have developed an analytical method for the determination of the absolute configuration and/or the concentration/yield and/or the enantiomeric/diastereomeric composition of a chiral analyte in the sample. The method utilizes the formation of a covalent bond between a quinone, (hetero)aryl isocyanate, and/or (hetero)aryl isothiocyanate probe and an analyte in a sample. Chiroptical and/or optical spectroscopic signal techniques are used in the analysis of the probe–analyte derivatives.
BACKGROUND
In recent years, optical methods such as circular dichroism (CD) spectroscopy have become a popular, cost-effective alternative for enantiomeric ratio (er) determination. The simplicity of CD analysis combined with the possibility of fast and parallel data collection at minimal solvent usage can reduce the workload and increase sample throughput. This invention presents an inexpensive, commercially available achiral aryliso(thio)cyanate sensor that smoothly
reacts with amino and alcohol groups under mild conditions toward urea or carbamate products exhibiting characteristic UV and CD signals above 300 nm, which is used for quantitative er and concentration analysis.
Benefit
Market Application
Publications
Rapid organocatalytic chirality analysis of amines, amino acids, alcohols, amino alcohols and diols with achiral iso(thio)cyanate probes.DOI:10.1039/D1SC02061GChem. Sci., 2021,12, 8784-8790
Chiroptical Switching and Quantitative Chirality Sensing with (Pseudo)halogenated Quinones.Angewandte Chemie.Volume60,Issue52. December 20, 2021. Pages27031-27038.https://onlinelibrary.wiley.com/doi/10.1002/anie.202111542
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