AI Article Synopsis

  • The study examined how the drug 3H-spiperone labels serotonin-S2 receptors in rat frontal cortex tissue and measured the dissociation times of various serotonin antagonists from these receptors.
  • Dissociation half-times ranged from 4.8 minutes for pipamperone to 160 minutes for ritanserin, showing no clear correlation with chemical structure or drug properties.
  • The research highlights the importance of determining drug-receptor dissociation times for understanding drug interactions and their implications in pharmacology and drug design, with patterns of inhibition classified based on dissociation rates.

Article Abstract

The labelling by 3H-spiperone of serotonin-S2 receptors in rat frontal cortex tissue adsorbed to glass fibre filters was investigated. For 12 unlabelled serotonin antagonists the dissociation time from serotonin-S2 receptors was measured using rat frontal cortex tissue preparations adsorbed to glass fibre filters. The dissociation half-time varied from 4.8 min for pipamperone to 160 min for ritanserin. The drug-receptor dissociation time was not related to a particular class of chemical structure, or to the lipophilicity or the acid dissociation constant of the drugs. The essential requirement of experimental determination of the drug-receptor dissociation time for each drug individually is illustrated. The possible applications of the knowledge of the drug-receptor dissociation time in in vitro and in vivo receptor studies, in pharmacological and pharmacokinetic studies and in drug design and receptor modelling is discussed. For various serotonin-S2 antagonists, the type of inhibition produced by the drug on 3H-ketanserin binding to serotonin-S2 receptors was determined using suspensions of rat frontal cortical tissue. The observed patterns of inhibition were clearly related to the drug-receptor dissociation times: rapidly dissociating drugs produced competitive inhibition, drugs with dissociation half-times between 15-30 min produced mixed type inhibition, and the very slowly dissociating ritanserin produced non-competitive inhibition.

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Source
http://dx.doi.org/10.3109/10799898809049011DOI Listing

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