Synthesis of a new series of N-hydroxy, N-alkylamides of aminoacids as ligands of NMDA glycine site

Anew series of N-hydroxy, N-alkylamides of aminoacids structurally related to the N-hydroxy-3-amino-2 pyrrolidone [(±)HA-966] was synthesised and evaluated for the ability to displace [ 3H]Glycine, [ 3H]CGS19755, [ 3H]AMPA and [ 3H]Kainate binding sites. The N-heptyl glycinamide 5a was the most pote...

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Published inEuropean journal of medicinal chemistry Vol. 34; no. 9; pp. 711 - 717
Main Authors Ghidini, Eleonora, Delcanale, Maurizio, Servadio, Vittorino, Pietra, Claudio, Bergamaschi, Marco, Villetti, Gino, Redenti, Enrico, Ventura, Paolo, Merlini, Lucio
Format Journal Article
LanguageEnglish
Published PARIS CEDEX 15 Elsevier Masson SAS 01.09.1999
Elsevier
Subjects
aminoacids
Biological and medical sciences
Chemistry, Medicinal
Glutamatergic system (aspartate and other excitatory aminoacids)
glycine antagonists
hydroxamic acids
Life Sciences & Biomedicine
Medical sciences
N-hydroxyamides of aminoacids
Neuropharmacology
Neurotransmitters. Neurotransmission. Receptors
Pharmacology & Pharmacy
Pharmacology. Drug treatments
Science & Technology
N-hydroxyamides of aminoacids
glycine antagonists
hydroxamic acids
aminoacids
GUINEA-PIG ILEUM
D-ASPARTATE RECEPTOR
AGONISTS
ATOMIC PHYSICOCHEMICAL PARAMETERS
AFFINITY
PHARMACOLOGY
RAT-BRAIN
ANTAGONISTS
BINDING
DIRECTED QUANTITATIVE STRUCTURE
Rat
Aliphatic compound
Rodentia
Central nervous system
Hydroxamic acid
Glutamate receptor
In vitro
α-Aminoacid
Vertebrata
Biological fixation
Mammalia
Structure activity relation
Animal
Glycine receptor
Benzenic compound
NMDA receptor
Chemical synthesis
Brain (vertebrata)
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Summary:Anew series of N-hydroxy, N-alkylamides of aminoacids structurally related to the N-hydroxy-3-amino-2 pyrrolidone [(±)HA-966] was synthesised and evaluated for the ability to displace [ 3H]Glycine, [ 3H]CGS19755, [ 3H]AMPA and [ 3H]Kainate binding sites. The N-heptyl glycinamide 5a was the most potent compound (IC 50 = 4.5 μM) in inhibiting [ 3H]Glycine binding. Compounds 5b, 5d, 5m, 5p, 5q and 5r showed an activity similar to (±)HA-966, whereas 5h, 5i, 5n and 5s appeared less active. None of the compounds tested exhibited a significant displacement of [ 3H]AMPA and [ 3H]Kainate binding sites. Compounds active in the [ 3H]Glycine binding inhibited, to a different degree, NMDA induced contractions in guinea-pig LMPP preparation.
ISSN:0223-5234
1768-3254
DOI:10.1016/S0223-5234(99)00222-6