EFFECTS OF 5,7DICHLOROKYNURENIC ACID ON CONFLICT, SOCIAL-INTERACTION AND PLUS-MAZE BEHAVIORS

被引：62

作者：

CORBETT, R ^{[1
]}

DUNN, RW ^{[1
]}

机构：

[1] ANAQUEST INC,CENT NERVOUS SYST RES,MURRAY HILL,NJ 07974

来源：

NEUROPHARMACOLOGY | 1993年 / 32卷 / 05期

关键词：

ANXIOLYTIC; CONFLICT BEHAVIOR; STRYCHNINE-INSENSITIVE GLYCINE ANTAGONISTS;

D O I：

10.1016/0028-3908(93)90170-8

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

Antagonists at the N-methyl-D-aspartate (NMDA) receptor site share a number of properties including anticonvulsant and anxiolytic-like behaviors. In the social interaction and elevated plus maze assay, two non-conditioned paradigms predictive of anxiolytic activity, the NMDA antagonists 5,7 DCKA, CPP and MK-801, as well as diazepam, all significantly increased both social interaction time and open arm exploration time, respectively. Likewise, in the Cook and Davidson conditioned conflict paradigm, the NMDA antagonists 5,7 dichlorokynurenic acid (DCKA; 100 and 173 mg/kg), ( +/- )-3-2-carboxypiperazin-4-yl)-propyl-l-phosphonic acid (CPP; 10 mg/kg), dizolcipine (MK-801; 0.03 mg/kg) and the benzodiazepine, diazepam (3-30 mg/kg) significantly disinhibited conflict responding. In addition, administration of 5,7 DCKA did not result in a generalization to a MK-801 discriminative cue in a drug discrimination paradigm. In general, antagonism at the NMDA receptor complex results in anxiolytic-like behavior in rodents. In particular, selective antagonism at the strychnine-insensitive glycine modulatory site (5,7 DCKA) may represent a new and novel class of compounds with potential therapeutic efficacy in anxiety without some of the side effects associated with other NMDA antagonists.

引用

页码：461 / 466

页数：6

共 50 条

[31] The nitric oxide synthesis inhibitor L-NAME produces anxiogenic-like effects in the rat elevated plus-maze test, but not in the social interaction test
Vale, AL
Green, S
Montgomery, AMJ
Shafi, S
JOURNAL OF PSYCHOPHARMACOLOGY, 1998, 12 (03) : 268 - 272
[32] Anxiogenic effects in the rat elevated plus-maze of 5-HT2C agonists into ventral but not dorsal hippocampus
Alves, SH
Pinheiro, G
Motta, V
Landeira-Fernandez, J
Cruz, APM
BEHAVIOURAL PHARMACOLOGY, 2004, 15 (01): : 37 - 43
[33] Pharmacological evaluation of the anxiolytic-like effects of EMD 386088, a partial 5-HT6 receptor agonist, in the rat elevated plus-maze and Vogel conflict tests
Jastrzebska-Wiesek, Magdalena
Siwek, Agata
Partyka, Anna
Kubacka, Monika
Mogilski, Szczepan
Wasik, Anna
Kolaczkowski, Marcin
Wesolowska, Anna
NEUROPHARMACOLOGY, 2014, 85 : 253 - 262
[34] ROLE OF RESOCIALIZATION AND OF 5-HT1A RECEPTOR ACTIVATION ON THE ANXIOGENIC EFFECTS INDUCED BY ISOLATION IN THE ELEVATED PLUS-MAZE TEST
MAISONNETTE, S
MORATO, S
BRANDAO, ML
PHYSIOLOGY & BEHAVIOR, 1993, 54 (04) : 753 - 758
[35] Social isolation stress enhances the effect of 5-HT1A agonist 8-OH-DPAT on the rat elevated plus-maze
Noppamars Wongwitdecha
Nattaporn Yoopan
Annals of General Psychiatry, 7 (Suppl 1)
[36] EFFECTS OF BLOCKADE OF 5-HT2 RECEPTORS AND ACTIVATION OF 5-HT1A RECEPTORS ON THE EXPLORATORY ACTIVITY OF RATS IN THE ELEVATED PLUS-MAZE
MOTTA, V
MAISONNETTE, S
MORATO, S
CASTRECHINI, P
BRANDAO, ML
PSYCHOPHARMACOLOGY, 1992, 107 (01) : 135 - 139
[37] EVIDENCE THAT MCPP-INDUCED ANXIETY IN THE PLUS-MAZE IS MEDIATED BY POSTSYNAPTIC 5-HT2C RECEPTORS BUT NOT BY SYMPATHOMIMETIC EFFECTS
GIBSON, EL
BARNFIELD, AMC
CURZON, G
NEUROPHARMACOLOGY, 1994, 33 (3-4) : 457 - 465
[38] BEHAVIORAL-EFFECTS OF 5-HT RECEPTOR LIGANDS IN THE AVERSIVE BRAIN-STIMULATION, ELEVATED PLUS-MAZE AND LEARNED HELPLESSNESS TESTS
GRAEFF, FG
AUDI, EA
ALMEIDA, SS
GRAEFF, EO
HUNZIKER, MHL
NEUROSCIENCE AND BIOBEHAVIORAL REVIEWS, 1990, 14 (04): : 501 - 506
[39] MIANSERIN-INDUCED 5-HT(2) RECEPTOR DOWN-REGULATION RESULTS IN ANXIOLYTIC EFFECTS IN THE ELEVATED PLUS-MAZE TEST
BENJAMIN, D
SAIFF, EI
NEVINS, T
LAL, H
DRUG DEVELOPMENT RESEARCH, 1992, 26 (03) : 287 - 297
[40] CHRONIC MIANSERIN OR ELTOPRAZINE TREATMENT IN RATS - EFFECTS ON THE ELEVATED PLUS-MAZE TEST AND ON LIMBIC 5-HT2C RECEPTOR LEVELS
ROCHA, B
RIGO, M
DISCALA, G
SANDNER, G
HOYER, D
EUROPEAN JOURNAL OF PHARMACOLOGY, 1994, 262 (1-2) : 125 - 131

← 1 2 3 4 5 →