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[摘要]:The classical benzodiazepines (Bz) constitute a well-known class of therapeutics displaying hypnotic, anxiolytic and anticonvulsant effects acting upon a specific binding site (BzR) belonging to the GABA(A) receptor complex. Their usefulness, however, is limited by a broad range of side effects; consequently the fact that the action of GABA with the receptor complex could be allosterically modulated by a wide variety of chemical entities, made the Bz binding site, from late eighties to nowdays, the target of extensive research programmes directed to the identification of new ligands displaying varying degrees of affinity-and efficacy-selectivity for the different GABA(A)/BzR-subtypes. The principal aim has been to discover ideal sedative-hypnotic agents (selective alpha(1) agonists), anxiolytic agents (selective alpha(2)/alpha(3) agonists), or cognitive enhancers (selective alpha(5) inverse agonists). In this connection, an important contribution in the field of GABA(A)/BzR ligands was made by the research group directed by Professor Antonio Da Settimo at the University of Pisa. The purpose of this review is therefore to describe the studies, performed from early '80s, on the several classes of BzR ligands developed featuring the indol-3-ylglyoxyl scaffold. All the compounds reported have been summarized on the basis of their main chemical structural features, focusing attention on their SARs, which determined the affinity profiles or efficacy-selectivity. Moreover, the biological studies performed within each class of compounds allowed the identification of new derivatives exhibiting an anxiolytic/nonsedative profile, either in vitro (full alpha(2) agonism and alpha(1) partial agonism/antagonism) and in vivo (anxiolytic/nonsedative activity in mice). |
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