Downstream Allosteric Modulation of NMDA Receptors by 3-Benzazepine Derivatives
Ritter N; Disse P; Aymanns I; Mücher L; Schreiber JA; Brenker C; Strünker T; Schepmann D; Budde T; Strutz-Seebohm N; Ametamey SM; Wünsch B; Seebohm G
Research article (journal) | Peer reviewedAbstract
N-Methyl-D-aspartate receptors (NMDARs) composed of different splice variants display distinct pH sensitivities and are crucial for learning and memory, as well as for inflammatory or injury processes. Dysregulation of the NMDAR has been linked to diseases like Parkinson's, Alzheimer's, schizophrenia, and drug addiction. The development of selective receptor modulators, therefore, constitutes a promising approach for numerous therapeutical applications. Here, we identified (R)-OF-NB1 as a promising splice variant selective NMDAR antagonist. We investigated the interaction of (R)-OF-NB1 and NMDAR from a biochemical, bioinformatical, and electrophysiological perspective to characterize the downstream allosteric modulation of NMDAR by 3-benzazepine derivatives. The allosteric modulatory pathway starts at the ifenprodil binding pocket in the amino terminal domain and immobilizes the connecting α5-helix to the ligand binding domain, resulting in inhibition. In contrast, the exon 5 splice variant GluN1-1b elevates the NMDARs flexibility and promotes the open state of its ligand binding domain.
Details about the publication
Authors from the University of Münster
| Aymanns, Isabel | |
| Brenker, Christoph | |
| Budde, Thomas | |
| Mücher, Lena | |
| Ritter, Nadine | |
| Schepmann, Dirk | |
| Schreiber, Julian Alexander | |
| Seebohm, Guiscard | |
| Strünker, Timo | |
| Strutz-Seebohm, Nathalie | |
| Wünsch, Bernhard |
Projects the publication originates from
RTG 2515: Chemical Biology of Ion Channels (Chembion) Duration: 01/10/2019 - 31/03/2024 | 1st Funding period Funded by: DFG - Research Training Group Type of project: Main DFG-project hosted at University of Münster |