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芬太尼对大鼠局部麻醉诱导镇痛的修饰作用。

Modification of local anesthetic-induced antinociception by fentanyl in rats.

机构信息

Department of Biophysics, Faculty of Medicine, Kahramanmaras Sutcu Imam University, 46100 Kahramanmaras, Turkey.

出版信息

Pharmacol Rep. 2011;63(6):1427-34. doi: 10.1016/s1734-1140(11)70706-x.

Abstract

In clinical practice, using the lowest doses of drugs for anesthesia or analgesia is the main goal. Opioid combinations with local anesthetics can be preferable for achieving adequate anesthesia or analgesia. The primary purpose of this study was to examine possible thermal antinociceptive effects of the opioid -fentanyl and the amide local anesthetics levobupivacaine and lidocaine when locally administered alone or in combination. The paw withdrawal latencies to noxious thermal stimuli in rats were measured to assess the antinociceptive actions of drugs after subcutaneous intraplantar injection into the hind paw. All drugs examined in this study produced dose- and time-dependent increases in the paw withdrawal latencies. Fentanyl is approximately 125 and 500 times more potent than levobupivacaine and lidocaine, respectively. At the same dose, the antinociceptive potency of levobupivacaine was 3.6-fold higher than that of lidocaine. Co-injection of the lowest doses of levobupivacaine and lidocaine dramatically increased the paw withdrawal latency. However, in the presence of fentanyl, the effects of levobupivacaine and lidocaine were different. Although co-injection of levobupivacaine with fentanyl both enhanced and prolonged antinociceptive action, the lidocaine-fentanyl combination did not significantly change the paw withdrawal latency. These results suggest that intraplantar co-administration of fentanyl with levobupivacaine, but not lidocaine, may provide more effective antinociception without increasing the dose requirements.

摘要

在临床实践中,使用最低剂量的药物进行麻醉或镇痛是主要目标。阿片类药物与局部麻醉剂的组合可以更好地实现足够的麻醉或镇痛效果。本研究的主要目的是检查单独或组合局部给予阿片类药物 - 芬太尼和酰胺类局部麻醉剂左旋布比卡因和利多卡因时可能产生的热镇痛作用。通过测量对有害热刺激的后爪撤回潜伏期来评估药物的镇痛作用,以评估药物的镇痛作用。在本研究中检查的所有药物都产生了剂量和时间依赖性的后爪撤回潜伏期增加。芬太尼分别比左旋布比卡因和利多卡因分别约强 125 和 500 倍。在相同剂量下,左旋布比卡因的镇痛效力比利多卡因高 3.6 倍。左旋布比卡因和利多卡因的最低剂量共同注射可显著增加后爪撤回潜伏期。然而,在芬太尼存在下,左旋布比卡因和利多卡因的作用不同。尽管与芬太尼共同注射左旋布比卡因增强并延长了镇痛作用,但利多卡因-芬太尼组合并未显著改变后爪撤回潜伏期。这些结果表明,与单独使用芬太尼相比,在足底内共同给予芬太尼与左旋布比卡因而非利多卡因可能会提供更有效的镇痛作用,而不会增加剂量需求。

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