(S)-(-)-2-(-Hydroxyethyl)benzimidazole (1)-derived diastereomeric monoaza-[18]crown-6 compounds 5 and 6 were synthesised with an additional chiral centre bearing a phenyl ring. The aim was to achieve enhanced enantioselective discrimination, compared with monoaza-[15]crown-5 (7). Surprisingly, reversal of enantioselective binding for chiral guest enantiomers between the two differently sized [15]crown-5 and [18]crown-6 azacrowns were discovered; all three were prepared from the same parent compound, 1. To complete the observations, another [18]crown-6-sized azacrown (10) without an additional chiral centre was synthesised from 1 and screened for its enantioselective binding abilities towards the chiral guest enantiomers investigated; these results corroborated the observations. Single-crystal XRD analysis and molecular docking studies revealed that changes to the conformational aspects of [18]crown-6 and [15]crown-5 azacrowns were the major contributing factors to this peculiar behaviour.

• 出版日期2015-3