Net production of cerebrospinal fluid is decreased by SCH‐23390

Abstract

A high density of binding sites for the ligands ³H‐SCH‐23390 and ³H‐SKF‐83566 has been found in the choroid plexus. Although these sites have similar pharmacology to D₁ dopamine receptors, the high‐affinity component of ³H‐SCH‐23390 binding in the choroid plexus has been identified as the 5‐HT_1c subtype of serotonin receptor. We investigated the possible role of these receptors in modulating the production of cerebrospinal fluid (CSF) in rats. (R) SCH‐23390 produced up to a 50% decrease in net CSF production, compared to saline. This compound is partial agonist at 5‐HT_1c serotonin receptors, and an antagonist at D₁ dopamine receptors. The (S) enantiomer of SCH‐23390 (SCH‐23388) was ineffective. Drugs interacting with receptors for neurotransmitters in the choroid plexus may hold promise for the treatment of patients with increased intracranial pressure, including those with mass lesions, head trauma, acute or chronic hydrocephalus, or pseudotumor cerebri.