Bimodal modulation by nicotine of anxiety in the social interaction test: Role of the dorsal hippocampus
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File, SE
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Kings Coll London, GKT Sch Biomed Sci, Ctr Res Neurosci, Psychopharmacol Res Unit, London WC2R 2LS, EnglandKings Coll London, GKT Sch Biomed Sci, Ctr Res Neurosci, Psychopharmacol Res Unit, London WC2R 2LS, England
File, SE
[1
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Kenny, PJ
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Kings Coll London, GKT Sch Biomed Sci, Ctr Res Neurosci, Psychopharmacol Res Unit, London WC2R 2LS, EnglandKings Coll London, GKT Sch Biomed Sci, Ctr Res Neurosci, Psychopharmacol Res Unit, London WC2R 2LS, England
Kenny, PJ
[1
]
Ouagazzal, AM
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Kings Coll London, GKT Sch Biomed Sci, Ctr Res Neurosci, Psychopharmacol Res Unit, London WC2R 2LS, EnglandKings Coll London, GKT Sch Biomed Sci, Ctr Res Neurosci, Psychopharmacol Res Unit, London WC2R 2LS, England
Ouagazzal, AM
[1
]
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[1] Kings Coll London, GKT Sch Biomed Sci, Ctr Res Neurosci, Psychopharmacol Res Unit, London WC2R 2LS, England
In conditions generating moderate levels of anxiety in the social interaction test (low Light, unfamiliar arena or high light, familiar arena), parenteral administration of nicotine had bimodal actions, low doses (0.01 and 0.1 mg/kg ip) had anxiolytic effects and high doses (0.5 and 1.0 mg/kg ip) had anxiogenic effects. In test conditions where anxiety was lowest (low light, familiar arena) and highest (high light, unfamiliar arena), nicotine was without effect after intraperitoneal or hippocampal administration. Thus, nicotine plays a modulatory role in which the activity of other neurotransmitters is crucial to its expression. After bilateral administration to the dorsal hippocampus, nicotine (0.1-8.0 mu g) had anxiogenic effects in conditions of moderate anxiety; mecamylamine (30 ng) was silent in these conditions, indicating no intrinsic tone. Our results show that the dorsal hippocampus is one area that can mediate anxiogenic effects in the social interaction test, but the brain region mediating anxiolytic effects remains to be identified.
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INST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLANDINST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLAND
BRAZELL, MP
MITCHELL, SN
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INST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLANDINST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLAND
MITCHELL, SN
GRAY, JA
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INST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLANDINST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLAND
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INST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLANDINST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLAND
BRAZELL, MP
MITCHELL, SN
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INST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLANDINST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLAND
MITCHELL, SN
GRAY, JA
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INST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLANDINST PSYCHIAT, DEPT PSYCHOL,MRC,BRAIN BEHAV & PSYCHIAT RES GRP, DE CRESPIGNY PK,DENMARK HILL, LONDON SE5 8AF, ENGLAND