Abstract
Isoxazolo[3,4-d] pyridazinones ([3,4-d]s) are selective positive modulators of the metabotropic glutamate receptors (mGluRs) subtypes 2 and 4, with no functional cross reactivity at mGluR(1a), mGLuR(5) or mGluR(8). Modest binding for two of the [3,4-d]s is observed at the allosteric fenobam mGluR(5) site, but not sufficient to translate into a functional effect. The structure activity relationship (SAR) for mGluR(2) and mGluR(4) are distinct: the compounds which select for mGluR(2) all contain fluorine on the N-6 aryl group. Furthermore, the [3,4-d]s in this study showed no significant binding at inhibitory GABA(A,) nor excitatory NMDA receptors, and previously we had disclosed that they lack significant activity at the System Xc-Antiporter. A homology model based on Conn's mGluR(1) crystal structure was examined, and suggested explanations for a preference for allosteric over orthosteric binding, subtype selectivity, and suggested avenues for optimization of efficacy as a reasonable working hypothesis.