Abstract
We sought to characterize the interactions of an endogenous clonidine-displacing substance (CDS) with the specific receptor sites to which clonidine and its analogs bind: (a) the non-adrenergic imidazole binding site, which is present in the ventrolateral medulla (VLM) but not the frontal cortex, (b) high-affinity and (c) low-affinity states of the α 2-adrenergic receptor, and (d) the α 1-adrenergic receptor. CDS, like clonidine, potently and completely inhibited specific p-[ 3 H] aminoclonidine binding to membranes from the VLM or from the frontal cortex. Both CDS and clonidine bound with highest affinity to imidazole binding sites in the VLM, both were 3-fold selective for high-affinity over low-affinity α 2-adrenergic receptors, and both exhibited lowest affinity for α 1-adrenergic receptors. Unlike clonidine, CDS exhibited 30-fold selectivity for imidazole over α 2-adrenergic receptors but showed only a weak preference for α 2- over α 1-adrenergic receptors, indicating that CDS and clonidine are not identical. We conclude that CDS is an endogenous clonidine-like substance which may be the natural ligand for imidazole binding sites in the VLM. The receptor-binding properties of CDS are consistent with the view that it is a unique and as yet unrecognized compound.
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