卡马西平对佐剂诱导的慢性炎症大鼠模型脊髓水平热敏感痛的镇痛作用。

Antinociceptive action of carbamazepine on thermal hypersensitive pain at spinal level in a rat model of adjuvant-induced chronic inflammation.

机构信息

Department of Anesthesiology, Kinki University Faculty of Medicine, 377-2 Ohno-higashi, Osaka-sayama, Osaka 589-8511, Japan.

出版信息

J Anesth. 2011 Feb;25(1):78-86. doi: 10.1007/s00540-010-1046-7. Epub 2010 Nov 27.

DOI:10.1007/s00540-010-1046-7

PMID:21113631

Abstract

PURPOSE

Systemic carbamazepine, a voltage-gated sodium channel blocker, has been reported to dose-dependently reduce inflammatory hyperalgesia. However, the antinociceptive effects of carbamazepine on the spinal cord in inflammatory conditions are unclear. The aim of the present study was to evaluate the antinociceptive effects of carbamazepine on the spinal cord in a chronic inflammatory condition.

METHODS

In Sprague-Dawley rats, a chronic inflammatory condition was induced by complete Freund's adjuvant (CFA) inoculation into the tail. Tail flick (TF) latencies were measured following intraperitoneal carbamazepine, or intrathecal carbamazepine or tetrodotoxin injection in intact rats and in the chronic inflammatory rats. From the values of TF latency at 60 min after drug injection, the effective dose required to produce 50% response (ED(50)) of each drug was derived.

RESULTS

Carbamazepine attenuated thermal responses with both systemic and intrathecal administration. The effect was more evident in rats with chronic inflammation than in intact rats; the ED(50s) of intraperitoneal carbamazepine in intact and inflamed rats were 12.39 and 1.54 mg/kg, and those of intrathecal carbamazepine were 0.311 and 0.048 nmol, respectively. Intrathecal tetrodotoxin also clearly inhibited the response, with ED(50s) of 1.006 pmol in intact rats and 0.310 pmol in inflamed rats. The relative potencies of intrathecal carbamazepine versus tetrodotoxin for inhibition were approximately 1:150-1:300 in intact and inflamed rats.

CONCLUSION

These results indicate that the inhibition of voltage-gated sodium channels, at least tetrodotoxin-sensitive channels, may contribute to the antinociceptive effect of carbamazepine on CFA-induced inflammatory pain, since lower doses of intrathecal carbamazepine and tetrodotoxin attenuated thermal responses to a greater extent in inflamed rats than in intact rats.

摘要

目的

全身性卡马西平是一种电压门控钠离子通道阻滞剂，据报道其可剂量依赖性地减轻炎症性痛觉过敏。然而，卡马西平在炎症状态下对脊髓的镇痛作用尚不清楚。本研究旨在评估卡马西平在慢性炎症状态下对脊髓的镇痛作用。

方法

在 Sprague-Dawley 大鼠中，通过将完全弗氏佐剂（CFA）接种到尾巴中来诱导慢性炎症状态。在完整大鼠和慢性炎症大鼠中，通过腹腔内给予卡马西平或鞘内给予卡马西平或河豚毒素注射后测量尾部拍打（TF）潜伏期。从药物注射后 60 分钟的 TF 潜伏期值中，得出每种药物产生 50%反应所需的有效剂量（ED（50））。

结果

卡马西平通过全身和鞘内给药均减弱了热反应。在慢性炎症大鼠中，这种作用比在完整大鼠中更为明显；完整和炎症大鼠中腹腔内给予卡马西平的 ED（50）分别为 12.39 和 1.54mg/kg，鞘内给予卡马西平的 ED（50）分别为 0.311 和 0.048nmol。鞘内河豚毒素也明显抑制了反应，在完整大鼠中的 ED（50）为 1.006pmol，在炎症大鼠中的 ED（50）为 0.310pmol。鞘内卡马西平与河豚毒素抑制的相对效力在完整和炎症大鼠中分别约为 1:150-1:300。

结论

这些结果表明，抑制电压门控钠离子通道，至少是河豚毒素敏感通道，可能有助于卡马西平对 CFA 诱导的炎症性疼痛的镇痛作用，因为鞘内给予较低剂量的卡马西平和河豚毒素在炎症大鼠中比在完整大鼠中更能减轻热反应。

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卡马西平对佐剂诱导的慢性炎症大鼠模型脊髓水平热敏感痛的镇痛作用。

Antinociceptive action of carbamazepine on thermal hypersensitive pain at spinal level in a rat model of adjuvant-induced chronic inflammation.

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