Human platelet 5-HT2 receptor binding sites re-evaluated: A criticism of recurrent techniques

Abstract

The human platelet 5-HT₂ receptor may resemble a peripheral model of central 5-HT₂ binding sites and has been linked to changes in 5-HT₂ receptor function in depression. Therefore, evaluation of the human platelet 5-HT₂ binding characteristics is important. Comparing [³H]ketanserin and [³H]LSD as ligands clearly indicated [³H]LSD as ligand of choice for binding studies dealing with the human platelet 5-HT₂ receptor. [³H]LSD binding was specific, saturable, and depended upon incubation time, protein concentration and previous handling of tissue, i.e., use of fresh or frozen tissue. In contrast, studies with [³H]ketanserin were unsatisfactory. Although mean receptor densities and affinities have been relatively constant between individuals and over time in healthy subjects with [³H]LSD, examination of the individual data showed considerable variations within single subjects. Thus, K_D ranged between 0.50 and 0.68 nM, and B_max was in the range of 64.9 to 97.1 fmol/mg protein in healthy individual subjects. Therefore, we recommend [³H]LSD as ligand of choice to study platelet 5-HT₂ receptor binding in humans. Furthermore, repeated measurement of individual data over time should be interpreted cautiously, especially when data from depressed patients are under examination.