N-METHYL-D-ASPARTATE RECEPTORS ARE IMPLICATED IN HYPERRESPONSIVENESS FOLLOWING NALOXONE REVERSAL OF ALFENTANIL IN ISOLATED RAT SPINAL-CORD

被引：24

作者：

FENG, JQ ^{[1
]}

KENDIG, JJ ^{[1
]}

机构：

[1] STANFORD UNIV, SCH MED, DEPT ANESTHESIA, STANFORD, CA 94305 USA

来源：

NEUROSCIENCE LETTERS | 1995年 / 189卷 / 02期

关键词：

HYPERALGESIA; SLOW VENTRAL ROOT POTENTIAL; TOLERANCE; WITHDRAWAL; N-METHYL-D-ASPARTATE RECEPTOR; ISOLATED SPINAL CORD;

D O I：

10.1016/0304-3940(95)11465-9

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

In isolated neonatal rat spinal cord, naloxone administered after an opioid increases a nociceptive-related slow ventral root potential (sVRP) to levels above pre-drug controls. We studied the role of N-methyl-D-aspartate (NMDA) receptors in this phenomenon, which may be related to acute tolerance and to hyperalgesia on antagonist-precipitated withdrawal. Naloxone (200 nM) alone produced no significant effect on sVRP area, while naloxone (560 nM) increased area to 121 +/- 17.7% of control (mean +/- SD). Following 200 nM alfentanil, naloxone (200 nM) was associated with a significant rebound in sVRP area to 138 +/- 18.0% of pre-drug control. Hyperresponsiveness developed within 7 min of initial alfentanil exposure. The non-competitive NMDA antagonist MK-801 (20 nM) had no effect on sVRP area when applied alone; higher concentrations produced irreversible depression. MK-801 (20 nM) co-applied with 200 nM alfentanil blocked the rebound increase in sVRP area following naloxone 200 nM and also the increase following naloxone alone (560 nM). The results suggest that alfentanil induces a rapid NMDA receptor-dependent change in spinal cord neuronal excitability.

引用

页码：128 / 130

页数：3

共 15 条

[1] HYPERALGESIA DURING NALOXONE-PRECIPITATED WITHDRAWAL FROM MORPHINE IS ASSOCIATED WITH INCREASED ON-CELL ACTIVITY IN THE ROSTRAL VENTROMEDIAL MEDULLA [J].

BEDERSON, JB ;

FIELDS, HL ;

BARBARO, NM .

SOMATOSENSORY AND MOTOR RESEARCH, 1990, 7 (02) :185-203

[2]

BLASIG J, 1973, PSYCHOPHARMACOLOGIA, V33, P19

[3] OPIOIDS CAN EVOKE DIRECT RECEPTOR-MEDIATED EXCITATORY EFFECTS ON SENSORY NEURONS [J].

CRAIN, SM ;

SHEN, KF .

TRENDS IN PHARMACOLOGICAL SCIENCES, 1990, 11 (02) :77-81

[4]

FENG J, 1995, IN PRESS BR J ANAEST

[5]

FRANCIS DL, 1971, BRIT J PHARMACOL, V41, pP424

[6] MORPHINE ANALGESIA AND ACUTE PHYSICAL-DEPENDENCE - RAPID ONSET OF 2 OPPOSING, DOSE-RELATED PROCESSES [J].

KIM, DH ;

FIELDS, HL ;

BARBARO, NM .

BRAIN RESEARCH, 1990, 516 (01) :37-40

[7] ACUTE TOLERANCE IN MORPHINE ANALGESIA - CONTINUOUS INFUSION AND SINGLE INJECTION IN RATS [J].

KISSIN, I ;

BROWN, PT ;

ROBINSON, CA ;

BRADLEY, EL .

ANESTHESIOLOGY, 1991, 74 (01) :166-171

[8] MAGNITUDE OF ACUTE TOLERANCE TO OPIOIDS IS NOT RELATED TO THEIR POTENCY [J].

KISSIN, I ;

BROWN, PT ;

BRADLEY, EL .

ANESTHESIOLOGY, 1991, 75 (05) :813-816

[9]

LEMMENS HJM, 1994, BRIT J ANAESTH, V72, P83

[10] ENKEPHALIN HYPERPOLARIZES INTERNEURONES IN THE RAT HIPPOCAMPUS [J].

MADISON, DV ;

NICOLL, RA .

JOURNAL OF PHYSIOLOGY-LONDON, 1988, 398 :123-130

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