Pharmacological and Physicochemical Properties of Pre‐Versus Postsynaptic 5‐Hydroxytryptamine1A Receptor Binding Sites in the Rat Brain: A Quantitative Autoradiographic Study
- 1 April 1992
- journal article
- research article
- Published by Wiley in Journal of Neurochemistry
- Vol. 58 (4) , 1338-1346
- https://doi.org/10.1111/j.1471-4159.1992.tb11347.x
Abstract
Numerous data suggested that the pharmacological and biochemical properties of 5‐hydroxytryptaminelA (5‐HTIA) receptors exhibit some regional differences in the CNS, notably within the raphe nuclei compared with various fore‐brain areas (such as the hippocampus). This possibility has been further investigated in the dorsal raphe nucleus and two areas within the hippocampus, the dentate gyrus and the CA1 area, using the quantitative autoradiographic technique. The potencies of 5′‐guanylylimidodiphosphate to inhibit the specific binding of 125I‐Bolton‐Hunter‐8‐methoxy‐2‐(N‐propyl‐N‐propylamino)tetralin (125I‐BH‐8‐MeO‐N‐PAT) to 5‐HT1A sites and of N‐ethylmaleimide to block these sites irreversibly were identical in the dorsal raphe nucleus and the hippocampal areas in rat brain sections. In contrast, slight but significant differences were noted in the pH dependence and pharmacological properties of 5‐HT1A sites labeled by 125I‐BH‐8‐MeO‐N‐PAT in these three regions. Similarly, heat denaturation experiments and tissue exposure to either phospholipase A2 or the alkylating agent 8‐methoxy‐2‐(N‐2′‐chloropropyl,N‐propyl)aminotetraline revealed regional differences in the properties of 5‐HT1A sites. However, in most cases, the observed variations were of greater amplitude between the CA1 area and the dentate gyrus, where 5‐HT1A sites are located postsynaptically, than between any one of these areas and the dorsal raphe nucleus where they act as (presynaptic) so‐matodendritic autoreceptors. These data further support that subtypes of 5‐HT1A receptors probably exist in the rat brain, but this heterogeneity seems unrelated to the pre‐ or postsynaptic location of these receptors.Keywords
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