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The use of FTIR and NMR spectroscopies to study prepolymerisation interactions in nitrogen heterocycles
Authors:Qendresa Osmani  Helen Hughes  Kevin Flavin  Jimmy Hedin-Dahlstrom  Christopher J Allender  June Frisby  Peter McLoughlin
Institution:(1) Department of Chemical and Life Sciences, Waterford Institute of Technology, Cork Road, Waterford, Ireland;(2) School of Biological and Chemical Sciences, Queen Mary, University of London, Mile End Road, London, E1 4NS, UK;(3) Molecular Recognition Research Unit, Welsh School of Pharmacy, Cardiff University, Redwood Building, King Edward VII Avenue, Cardiff, CF10 3XF, UK
Abstract:A detailed investigation into the functional groups responsible for the formation of a noncovalent complex between 2-aminopyridine (template) and methacrylic acid (functional monomer) has been carried out using FTIR spectroscopy and confirmed by 1H NMR spectroscopic data. The approach adopted to confirm the mechanism of interaction was the analysis of the template plus the structurally similar 2-methylaminopyridine and 2-dimethylaminopyridine. A 1:1 stoichiometry of complexation was determined by Job plot analysis following titration, with FTIR results complementing those of the 1H NMR study. The strength of interaction between 2-aminopyridine and the functional monomer measured through band shifts by FTIR spectroscopy was compared with such interactions for the isomers 3- and 4-aminopyridine. This comparison identified a clear correlation between template pK a, degree of interaction and subsequent nonspecific binding in the nonimprinted polymer. Using FTIR spectroscopy it was also possible to observe the effect of temperature on the prepolymerisation solution. IR spectra showed that lower temperatures led to more stabilized interactions of the hydrogen-bonded complex. The potential advantages of FTIR spectroscopy compared with 1H NMR spectroscopy in studying prepolymerisation solutions have been identified.
Keywords:Molecularly imprinted polymers  FTIR spectroscopy  Template–  monomer interaction  Hydrogen bond  Aminopyridine
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