DIFFERENTIAL-EFFECTS OF SELECTIVE OPIOID PEPTIDE ANTAGONISTS ON THE ACQUISITION OF PAVLOVIAN FEAR CONDITIONING

被引：46

作者：

FANSELOW, MS ^{[1
]}

KIM, JJ ^{[1
]}

YOUNG, SL ^{[1
]}

CALCAGNETTI, DJ ^{[1
]}

DECOLA, JP ^{[1
]}

HELMSTETTER, FJ ^{[1
]}

LANDEIRAFERNANDEZ, J ^{[1
]}

机构：

[1] DARTMOUTH COLL, DEPT PSYCHOL, HANOVER, NH 03755 USA

来源：

PEPTIDES | 1991年 / 12卷 / 05期

基金：

美国国家科学基金会;

关键词：

OPIOID ANTAGONIST; PAVLOVIAN CONDITIONING; FEAR; FREEZING; MU OPIOID RECEPTOR; DELTA OPIOID RECEPTOR; KAPPA OPIOID RECEPTOR; NOR-BINALTORPHIMINE; 16-METHYL CYPRENORPHINE; NALTRINDOLE; NALOXONAZINE; STRESS-INDUCED ANALGESIA; CYS2TYR3ORN5PEN7-AMIDE;

D O I：

10.1016/0196-9781(91)90056-U

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Pretreatment with opioid antagonists enhances acquisition of Pavlovian fear conditioning. The present experiments attempted to characterize the type of opioid receptor responsible for this effect using a procedure that assessed the fear of rats to a chamber previously associated with electric shock (1 mA, 0.75 s). Freezing, a species-typical immobility, was employed as an index of fear. Two mu-opioid antagonists, CTOP (40 ng) and naloxonazine (10-mu-g), enhanced conditioning. On the other hand, the kappa-antagonist nor-binaltorphimine reduced conditioning. Two delta-antagonist treatments (16-methyl cyprenorphine and naltrindole) had no reliable effect on acquisition. Thus the enhancement of conditioning appears to be mediated by mu-receptors. Previous research has shown that the conditional fear produced by these procedures caused an analgesia that is also mediated by mu-receptors. It is argued that the enhancement effect occurs because of an antagonism of this analgesia and that the analgesia normally acts to regulate the level of fear conditioning.

引用

页码：1033 / 1037

页数：5

共 33 条

[1] ENDOGENOUS PAIN CONTROL-SYSTEMS - BRAIN-STEM SPINAL PATHWAYS AND ENDORPHIN CIRCUITRY [J].

BASBAUM, AI ;

FIELDS, HL .

ANNUAL REVIEW OF NEUROSCIENCE, 1984, 7 :309-338

[2] DELTA-OPIOID ANTAGONIST, NALTRINDOLE, SELECTIVELY BLOCKS ANALGESIA INDUCED BY DPDPE BUT NOT DAGO OR MORPHINE [J].

CALCAGNETTI, DJ ;

HOLTZMAN, SG .

PHARMACOLOGY BIOCHEMISTRY AND BEHAVIOR, 1991, 38 (01) :185-190

[3] QUATERNARY NALTREXONE REVEALS THE CENTRAL MEDIATION OF CONDITIONAL OPIOID ANALGESIA [J].

CALCAGNETTI, DJ ;

HELMSTETTER, FJ ;

FANSELOW, MS .

PHARMACOLOGY BIOCHEMISTRY AND BEHAVIOR, 1987, 27 (03) :529-531

[4] [D-ALA2,LEU5,CYS6]ENKEPHALIN - SHORT-TERM AGONIST EFFECTS AND LONG-TERM ANTAGONISM AT DELTA OPIOID RECEPTORS [J].

CALCAGNETTI, DJ ;

FANSELOW, MS ;

HELMSTETTER, FJ ;

BOWEN, WD .

PEPTIDES, 1989, 10 (02) :319-326

[5] PAIN MODULATION BY 5-HYDROXYTRYPTAMINERGIC AGENTS AND MORPHINE AS MEASURED BY 3 PAIN TESTS [J].

DENNIS, SG ;

MELZACK, R .

EXPERIMENTAL NEUROLOGY, 1980, 69 (02) :260-270

[6] EVIDENCE THAT NALOXONAZINE PRODUCES PROLONGED ANTAGONISM OF CENTRAL DELTA-OPIOID RECEPTOR ACTIVITY INVIVO [J].

DRAY, A ;

NUNAN, L .

BRAIN RESEARCH, 1984, 323 (01) :123-127

[7] MODULATION OF APPETITIVELY AND AVERSIVELY MOTIVATED BEHAVIOR BY THE KAPPA-OPIOID ANTAGONIST MR2266 [J].

FANSELOW, MS ;

CALCAGNETTI, DJ ;

HELMSTETTER, FJ .

BEHAVIORAL NEUROSCIENCE, 1989, 103 (03) :663-672

[8] SHOCK-INDUCED ANALGESIA ON THE FORMALIN TEST - EFFECTS OF SHOCK SEVERITY, NALOXONE, HYPOPHYSECTOMY, AND ASSOCIATIVE VARIABLES [J].

FANSELOW, MS .

BEHAVIORAL NEUROSCIENCE, 1984, 98 (01) :79-95

[9]

FANSELOW MS, 1980, PAVLOVIAN J BIOL SCI, V15, P177

[10] CONDITIONED FEAR-INDUCED OPIATE ANALGESIA - A COMPETING MOTIVATIONAL STATE THEORY OF STRESS ANALGESIA [J].

FANSELOW, MS .

ANNALS OF THE NEW YORK ACADEMY OF SCIENCES, 1986, 467 :40-54

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