Clinical evidence has demonstrated significant hypofunction of GABAergic neurotransmission in patients with schizophrenia, likely contributing to the onset of psychotic symptoms. These symptoms can be alleviated by α1β2γ2GABA-A receptor ligands, which have previously shown antipsychotic activity. Building on this foundation, we synthesized and characterized various derivatives of 2-phenylimidazo[1,2-a]-pyridine containing cyclic amine moieties at the amide backbone to identify potent ligands and expand the chemical space of α1β2γ2GABA-A receptor ligands. The synthesized compounds exhibited K(i) values ranging from 25.0 to 7822.5 nM and positive allosteric properties at α1β2γ2GABA-A receptors. Selected compounds exhibited promising cellular permeability properties, high metabolic stability, and neuroprotective activity. A representative derivative of this series elicited antipsychotic-like properties, reversing amphetamine- and MK-801-induced hyperlocomotion without inducing sedative effects. Our findings indicate that α1β2γ2GABA-A ligands represent a promising strategy for the identification of potential antipsychotic agents with an original mechanism of action.
Targeting GABAergic Hypofunction Associated with Schizophrenia: Identification of α1β2γ2GABA-A Receptor Ligands with Neuroprotective and Antipsychotic Properties.
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作者:Mordyl Barbara, SzafraÅska Katarzyna, Sniecikowska Joanna, Jonczyk Jakub, BieÅko BartÅomiej, Mateos-Jimenez Maria, WojdyÅa Bartosz, GryzÅo Beata, GÅuch-Lutwin Monika, Siwek Agata, Karcz Tadeusz, SÅoczyÅska Karolina, PÄkala Elżbieta, Zakrzewska-Sito Alicja, Mierzejewski Pawel, KoÅaczkowski Marcin, Marcinkowska Monika
| 期刊: | ACS Chemical Neuroscience | 影响因子: | 3.900 |
| 时间: | 2025 | 起止号: | 2025 Jun 18; 16(12):2277-2294 |
| doi: | 10.1021/acschemneuro.5c00098 | ||
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