Multipoint recognition of catecholamines by hydrindacene-based receptors accompanied by the complexation-induced conformational switching

摘要

The molecular recognition of catecholamines by hydrindacene-based receptors 1 and 2, as well as the durene-based receptor 3, and the guest-induced conformational changes are reported. These receptors selectively bind adrenaline and dopamine salts through the guests' ammonium group and 3-hydroxyl group on the aromatic ring. In the case of adrenaline, an additional hydrogen bond with a benzylic hydroxyl group is formed. In 2% CD3CN/CDCl3, the association constants are of the order of 10(4)m(-1), which is much larger than with guests without the 3-hydroxyl groups (10(3)m(-1)). The two amide groups of receptor 1 can rotate freely around the C-aromatic-C-amide bond, whereas the tert-amide in 2 changes between two stable conformations at a slow enough rate to allow detection by H-1 NMR spectroscopy. In the absence of a guest molecule, the syn-conformer is less stable than the anti-conformer. On complex formation with adrenaline, the syn-conformer becomes dominant due to an intramolecular dipole-reversal effect in addition to multipoint hydrogen bonding.