Ketanserin binds to the monoamine transporter of chromaffin granules and of synaptic vesicles

Ketanserin binds to the monoamine transporter of chromaffin granules and of synaptic vesicles

[3H]Ketanserin binding studies were performed on purified chromaffin granule membranes. Binding was found to occur on one class of sites and was temperature dependent. At 30 degrees the equilibrium dissociation constant KD was 45 nM. At 0 degrees, a KD value of 6 nM and a half-life of dissociation o...

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Bibliographic Details
Published in:Molecular pharmacology Vol. 33; no. 6; p. 672
Main Authors: Darchen, F, Scherman, D, Laduron, P M, Henry, J P
Format: Journal Article
Language:English
Published: United States 01-06-1988
Subjects:
Animals
Binding Sites
Biogenic Amines - metabolism
Brain - metabolism
Carrier Proteins - metabolism
Cattle
Chromaffin Granules - metabolism
Chromaffin System - metabolism
In Vitro Techniques
Ketanserin - analogs & derivatives
Ketanserin - metabolism
Ketanserin - pharmacology
Kinetics
Male
Mice
Synaptic Vesicles - metabolism
Tetrabenazine - metabolism
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Summary:[3H]Ketanserin binding studies were performed on purified chromaffin granule membranes. Binding was found to occur on one class of sites and was temperature dependent. At 30 degrees the equilibrium dissociation constant KD was 45 nM. At 0 degrees, a KD value of 6 nM and a half-life of dissociation of 40 sec were measured. Methysergide, an antagonist of 5-hydroxytryptamine2 (5-HT2) receptors structurally unrelated to ketanserin, did not displace ketanserin binding. Tetrabenazine, an inhibitor of the monoamine transporter of chromaffin granules, displaced [3H]ketanserin binding. Conversely, ketanserin inhibited the binding of [3H] dihydrotetrabenazine, a ligand that specifically binds to the monoamine transporter. The inhibition was of the competitive type, indicating that both drugs bind to the same site. Ketanserin binding did not depend upon ATP-induced energization of chromaffin granules. ATP-dependent 5-HT uptake by chromaffin granule ghosts was inhibited by ketanserin with an IC50 value of 70 nM. A series of ketanserin derivatives were tested for their ability to displace [3H]dihydrotetrabenazine; EC50 values differed by more than 2 orders of magnitude and were not correlated to affinities on 5-HT2 receptors. In mouse brain, [3H]ketanserin was found to bind to methysergide-sensitive and to tetrabenazine-sensitive sites. In the striatum, tetrabenazine-sensitive sites represented a larger fraction than the methysergide-sensitive ones, whereas the reverse was true in the frontal cortex. It is concluded that nonspecific displaceable binding sites of [3H]ketanserin previously described in the striatum are tetrabenazine binding sites associated with the synaptic vesicle monoamine transporter.
ISSN:0026-895X