A Novel Class of Succinimide-Derived Negative Allosteric Modulators of Metabotropic Glutamate Receptor Subtype 1 Provides Insight into a Disconnect in Activity between the Rat and Human Receptors

Abstract

Recent progress in the discovery of mGlu<sub>1</sub> allosteric modulators has suggested the modulation of mGlu<sub>1</sub> could offer possible treatment for a number of central nervous system disorders; however, the available chemotypes are inadequate to fully investigate the therapeutic potential of mGlu<sub>1</sub> modulation. To address this issue, we used a fluorescence-based high-throughput screening assay to screen an allosteric modulator-biased library of compounds to generate structurally diverse mGlu<sub>1</sub> negative allosteric modulator hits for chemical optimization. Herein, we describe the discovery and characterization of a novel mGlu<sub>1</sub> chemotype. This series of succinimide negative allosteric modulators, exemplified by VU0410425, exhibited potent inhibitory activity at rat mGlu<sub>1</sub> but was, surprisingly, inactive at human mGlu<sub>1</sub>. VU0410425 and a set of chemically diverse mGlu<sub>1</sub> negative allosteric modulators previously reported in the literature were utilized to examine this species disconnect between rat and human mGlu<sub>1</sub> activity. Mutation of the key transmembrane domain residue 757 and functional screening of VU0410425 and the literature compounds suggests that amino acid 757 plays a role in the activity of these compounds, but the contribution of the residue is scaffold specific, ranging from critical to minor. The operational model of allosterism was used to estimate the binding affinities of each compound to compare to functional data. This novel series of mGlu<sub>1</sub> negative allosteric modulators provides valuable insight into the pharmacology underlying the disconnect between rat and human mGlu<sub>1</sub> activity, an issue that must be understood to progress the therapeutic potential of allosteric modulators of mGlu<sub>1</sub>

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