The relationship between molecularly imprinted polymer (MIP) morphology and template-rebinding over a series of warfarin-imprinted methacrylic acid co(ethylene dimethacrylate) polymers has been explored. Detailed investigations of the nature of template recognition revealed that an optimal template binding was obtained with polymers possessing a narrow population of pores (~3-4 nm) in the mesopore size range. Importantly, the warfarin-polymer rebinding analyses suggest strategies for regulating ligand binding capacity and specificity through variation of the degree of cross-linking, where polymers prepared with a lower degree of cross-linking afford higher capacity though non-specific in character. In contrast, the co-existence of specific and non-specific binding was found in conjunction with higher degrees of cross-linking and resultant mesoand macropore size distributions. © 2013 by the authors; licensee MDPI, Basel, Switzerland.
CITATION STYLE
Rosengren, A. M., Karlsson, B. C. G., & Nicholls, I. A. (2013). Consequences of morphology on molecularly imprinted polymer-ligand recognition. International Journal of Molecular Sciences, 14(1), 1207–1217. https://doi.org/10.3390/ijms14011207
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