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Dibenzodiazepinone-type muscarinic receptor antagonists conjugated to basic peptides: Impact of the linker moiety and unnatural amino acids on M2R selectivity

Weinhart, Corinna. G. ; Wifling, David ; Schmidt, Maximilian. F. ; Neu, Eduard ; Höring, Carina ; Clark, Timothy ; Gmeiner, Peter ; Keller, Max



Abstract

The family of human muscarinic acetylcholine receptors (MRs) is characterized by a high sequence homology among the five subtypes (M1R-M5R), being the reason for a lack of subtype selective MR ligands. In continuation of our work on dualsteric dibenzodiazepinone-type M2R antagonists, a series of M2R ligands containing a dibenzodiazepinone pharmacophore linked to small basic peptides was ...

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