首页> 外文期刊>Pain. >Chronic treatment with systemic morphine induced tolerance to the systemic and peripheral antinociceptive effects of morphine on both carrageenin induced mechanical hyperalgesia and spinal c-Fos expression in awake rats.
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Chronic treatment with systemic morphine induced tolerance to the systemic and peripheral antinociceptive effects of morphine on both carrageenin induced mechanical hyperalgesia and spinal c-Fos expression in awake rats.

机译:全身性吗啡的慢性治疗诱导了对吗啡对角叉菜胶诱导的机械痛觉过敏和清醒大鼠脊髓c-Fos表达的全身和外周镇痛作用的耐受。

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The effects of intravenous (3 mg/kg i.v.) and intraplantar (50 micrograms/50 microliters i.pl.) morphine were investigated on spinal c-Fos expression induced 2 h after intraplantar carrageenin (6 mg/150 microliters of saline) and on carrageenin (2 mg/150 microliters of saline) induced mechanical hyperalgesia, at day 4, in both naive and chronic morphine treated (80 mg/kg/day s.c. on days 1, 2 and 3) rats. In naive rats, i.v. and i.pl. morphine significantly decreased spinal c-Fos expression (64 +/- 4% and 44 +/- 4% reduction of control carrageenin c-Fos expression, P < 0.0001 for both, respectively) and mechanical hyperalgesia (maximal increase: 326 +/- 29%, P < 0.0001 and 87 +/- 5%, P < 0.005 of control carrageenin paw pressure vocalisation threshold (VTPP), respectively), which only developed in the carrageenin injected paw. Both treatments were ineffective in chronic morphine treated rats (92 +/- 9% and 106 +/- 6% of control carrageenin c-Fos expression; 33 +/- 17% and 30 +/- 15% increase of controlcarrageenin VTPP, respectively). Furthermore, only i.v. morphine increased the VTPP in the contralateral paw, in naive rats (maximal increase: 90 +/- 8%, P < 0.0001 of control carrageenin VTPP), its effects being significantly less pronounced than for the inflamed paw (P < 0.0001). These studies based on spinal c-Fos expression as an indirect marker of spinal nociceptive processes and on behavioural experiments clearly revealed that chronic treatment with systemic morphine induced tolerance to both its systemic and peripheral effects.
机译:研究了静脉内(3 mg / kg iv)和足底内(50微克/ 50微升i.pl.)吗啡对plant骨角叉菜胶(6 mg / 150微升盐水)2 h后诱导的脊髓c-Fos表达的影响以及对于第4天,角叉菜胶(2 mg / 150微升盐水)在幼稚和慢性吗啡治疗(第1、2和3天的皮下剂量为80 mg / kg /天,皮下注射)诱导的机械性痛觉过敏。在幼稚大鼠中,静脉注射和i.pl。吗啡显着降低脊髓c-Fos表达(对照角叉菜胶c-Fos表达降低64 +/- 4%和44 +/- 4%,分别为P <0.0001)和机械性痛觉过敏(最大增加:326 +/-分别为角叉菜胶注射爪的29%(P <0.0001和87 +/- 5%,P <0.005),分别为对照组角叉菜胶爪发声阈值(VTPP)。两种治疗方法在慢性吗啡治疗的大鼠中均无效(对照角叉菜胶c-Fos表达的92 +/- 9%和106 +/- 6%;对照角叉菜胶VTPP分别增加33 +/- 17%和30 +/- 15% )。此外,只有i.v.吗啡在幼稚大鼠的对侧爪中增加了VTPP(最大增加:90 +/- 8%,对照角叉菜胶VTPP的P <0.0001),其作用远不如发炎的爪明显(P <0.0001)。这些基于脊髓c-Fos表达作为脊髓伤害过程间接指标的研究和行为实验清楚地表明,全身性吗啡的慢性治疗可诱导其对全身和外周作用的耐受性。

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