Abstract
An overview of molecular modelling approaches, related to chiral separations on polysaccharide-based and macrocyclic antibiotic chiral selectors, is presented. Both atomistic calculations and empirical fitting procedures are discussed. Atomistic calculations, such as docking and molecular dynamics can be used to model the interactions between enantiomers and the chiral stationary phase. This may help obtaining information about the chiral recognition mechanism. Conversely, in empirical fitting procedures, mathematical models for relevant separation parameters are fitted to experimental observations. The latter use theoretical molecular descriptors, calculated from the molecular structure, which are combined into a model to predict a given response, for example, retention. Such relationships, when used in chiral separations, are often called quantitative structure enantioselective retention relationships (QSERR) and an increased interest in them can be observed in the literature. Different regression models are discussed, such as multiple linear regression and partial least squares.
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