Abstract
A series of compounds containing privileged scaffolds of the known histamine H(1) receptor antagonists cetirizine, mianserin, ketotifen, loratadine, and bamipine were synthesized for further optimization as ligands for the related biogenic amine binding dopamine D(3) receptor. A pharmacological screening was carried out at dopamine D(2) and D(3) receptors. In the preliminary testing various ligands have shown moderate to high affinities for dopamine D(3)receptors, for example, N-(4-{4-[benzyl(phenyl)amino]piperidin-1-yl}butylnaphthalen-2-carboxamide (19a) (hD(3)K(i)=0.3 nM; hD(2)K(i)=703 nM), leading to a selectivity ratio of 2343.
MeSH terms
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Amines / chemistry
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Animals
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Binding, Competitive
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CHO Cells
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Cell Line
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Cetirizine / chemical synthesis
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Cetirizine / chemistry
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Cetirizine / pharmacology
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Cricetinae
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Cricetulus
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Dopamine D2 Receptor Antagonists
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Drug Design*
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Drug Evaluation, Preclinical
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Histamine H1 Antagonists / chemical synthesis*
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Histamine H1 Antagonists / chemistry
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Histamine H1 Antagonists / pharmacology*
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Humans
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Ketotifen / chemical synthesis
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Ketotifen / chemistry
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Ketotifen / pharmacology
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Ligands
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Loratadine / chemical synthesis
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Loratadine / chemistry
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Loratadine / pharmacology
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Mianserin / chemical synthesis
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Mianserin / chemistry
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Mianserin / pharmacology
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Molecular Structure
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Piperidines / chemical synthesis
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Piperidines / chemistry
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Piperidines / pharmacology
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Receptors, Dopamine D3 / antagonists & inhibitors*
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Stereoisomerism
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Structure-Activity Relationship
Substances
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Amines
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Dopamine D2 Receptor Antagonists
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Histamine H1 Antagonists
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Ligands
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Piperidines
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Receptors, Dopamine D3
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Mianserin
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Loratadine
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Ketotifen
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bamipine
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Cetirizine