Abstract
Non-covalent interactions between aromatic molecules (π-π interactions) play a major role in biological molecular recognition. A simple theoretical model which accounts for the geometric properties of π-π interactions is described. The key feature of this model is that it specifically allows for out-of-plane π-electron density in the calculation of electrostatic interactions. Experimental evidence for the validity of the model comes from studies of the geometric distribution of phenylalanine-phenylalanine interactions in protein X-ray crystal structures. The model has also been used to design a synthetic molecular receptor which recognizes
p
-benzoquinone using H-bonds and edge-to-face π-π interactions. Aromatic stacking interactions provide the crucial link between sequence and three-dimensional structure in double-helical DNA. The π-π interaction model has been used to calculate the conformational preferences of all ten DNA base-pair steps and the results provide new insight into the molecular basis of sequence-dependent DNA structure.
Subject
Pharmacology (medical),Complementary and alternative medicine,Pharmaceutical Science
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