THE SEVERITY OF NALOXONE-PRECIPITATED OPIATE WITHDRAWAL IS ATTENUATED BY FELBAMATE, A POSSIBLE GLYCINE ANTAGONIST

被引：21

作者：

KOSTEN, TA ^{[1
]}

DECAPRIO, JL ^{[1
]}

ROSEN, MI ^{[1
]}

机构：

[1] YALE UNIV,SCH MED,DEPT PSYCHIAT,DIV SUBST ABUSE,NEW HAVEN,CT

来源：

NEUROPSYCHOPHARMACOLOGY | 1995年 / 13卷 / 04期

关键词：

HA-966; D-CYCLOSERINE; MORPHINE; N-METHYL-D-ASPARTATE; GLUTAMATE; CHRONIC DRUG EFFECTS; GLYCINE PARTIAL AGONISTS;

D O I：

10.1038/sj.npp.1380291

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

Recent studies indicate that an N-methyl-D-aspartate (NMDA) receptor system in the rostral medulla is involved in opiate withdrawal. Although NMDA antagonists attenuate naloxone-precipitated opiate withdrawal, they can cause phencyclidine (PCP)like effects that contraindicate clinical use. Because NMDA channels contain sites for the glutamate coagonist, glycine, we assessed the effects of glycinergic agents on naloxone-precipitated opiate withdrawal in rats. The putative antagonist, felbamate (100, 300 mg/kg), attenuated overall withdrawal severity in a dose-related manner and reduced occurrences of chews, teeth chatters, and penile grooming. The partial agonist, D-cycloserine (3, 10 mg/kg), attenuated withdrawal severity, but not in a dose-related manner. Conversely, the low dose of the partial agonist, (+/-)-HA-966 (3, 10 mg/kg), heightened the occurrences of some withdrawal signs. These results support a role for glycine in opiate withdrawal and suggest that these agents, which do not cause PCPlike effects, may be potential treatment for agents for opiate detoxification.

引用

页码：323 / 333

页数：11

共 53 条

[1] TOLERANCE OF LOCUS COERULEUS NEURONS TO MORPHINE AND SUPPRESSION OF WITHDRAWAL RESPONSE BY CLONIDINE [J].

AGHAJANIAN, GK .

NATURE, 1978, 276 (5684) :186-188

[2] OPIATE WITHDRAWAL INCREASES GLUTAMATE AND ASPARTATE EFFLUX IN THE LOCUS-COERULEUS - AN IN-VIVO MICRODIALYSIS STUDY [J].

AGHAJANIAN, GK ;

KOGAN, JH ;

MOGHADDAM, B .

BRAIN RESEARCH, 1994, 636 (01) :126-130

[3]

AKAOKA H, 1991, J NEUROSCI, V11, P3830

[4]

BLASIG J, 1973, PSYCHOPHARMACOLOGIA, V33, P19

[5] PHENCYCLIDINE INHIBITION OF THE RATE OF DEVELOPMENT OF AMYGDALOID KINDLED SEIZURES [J].

BOWYER, JF .

EXPERIMENTAL NEUROLOGY, 1982, 75 (01) :173-183

[6] NEUROPROTECTIVE EFFECT OF FELBAMATE AFTER KAINIC ACID-INDUCED STATUS EPILEPTICUS [J].

CHRONOPOULOS, A ;

STAFSTROM, C ;

THURBER, S ;

HYDE, P ;

MIKATI, M ;

HOLMES, GL .

EPILEPSIA, 1993, 34 (02) :359-366

[7]

Collingridge GL, 1983, J PHYSIOL-LONDON, V334, P34

[8] BLOOD-BRAIN-BARRIER PENETRATION OF FELBAMATE [J].

CORNFORD, EM ;

YOUNG, D ;

PAXTON, JW ;

SOFIA, RD .

EPILEPSIA, 1992, 33 (05) :944-954

[9]

DANYSZ W, 1993, PHARM BIOCH BEHAV, V48, P111

[10] ACTIONS OF D-CYCLOSERINE AT THE N-METHYL-D-ASPARTATE-ASSOCIATED GLYCINE RECEPTOR-SITE INVIVO [J].

EMMETT, MR ;

MICK, SJ ;

CLER, JA ;

RAO, TS ;

IYENGAR, S ;

WOOD, PL .

NEUROPHARMACOLOGY, 1991, 30 (11) :1167-1171

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