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(±)-CPP与丙戊茶碱联合应用对单关节炎大鼠产生抗伤害感受作用的电生理研究

Electrophysiological Study of the Antinociception Produced by the Coapplication of (±)-CPP and Propentofylline in Monoarthritic Rats.

作者信息

Laurido Claudio, Martínez José L, Morales Francisco

机构信息

Laboratory of Neurobiology, Department of Biology, Faculty of Chemistry and Biology, University of Santiago of Chile, Avenue Libertador B. O'Higgins 3363, Casilla 40, Correo 33, 9170022 Santiago, Chile.

Vice Rectory of Research, Development and Innovation, University of Santiago of Chile, Avenue Libertador B. O'Higgins 3363, Casilla 40, Correo 33, 9170022 Santiago, Chile.

出版信息

ISRN Pain. 2013 Apr 4;2013:315626. doi: 10.1155/2013/315626. eCollection 2013.

Abstract

The NMDA receptor is central in the generation and maintenance of chronic pain. This receptor has several sites of modulation. One is the glutamate recognition site that can be blocked by (±)-3-(2-carboxypiperazin-yl)propyl-1-phosphoric acid or (±)-CPP. We investigated whether the effect of glial inhibition produced by propentophylline (PPF) can be enhanced when combined with (±)-CPP. We used Sprague-Dawley rats with experimental monoarthritis, administering intrathecally the ED30 for both drugs (3.97 μg of (±)-CPP and 1.42 μg of PPF), since this combination produces an antinociceptive supra-additive effect when used in mechanical nociception (Randall-Selitto test). The combination of (±)-PPF and CPP produced an antinociceptive effect which was greater than that each drug alone as tested by both the C reflex and windup. We conclude that the antinociceptive effect of the combination of (±)-PPF and CPP possibly generates a supra additive interaction type in monoarthritic rats.

摘要

N-甲基-D-天冬氨酸(NMDA)受体在慢性疼痛的产生和维持中起核心作用。该受体有多个调节位点。其中一个是谷氨酸识别位点,可被(±)-3-(2-羧基哌嗪基)丙基-1-磷酸或(±)-CPP阻断。我们研究了丙戊茶碱(PPF)产生的胶质细胞抑制作用与(±)-CPP联合使用时是否能增强。我们使用患有实验性单关节炎的Sprague-Dawley大鼠,鞘内注射两种药物的ED30(3.97μg的(±)-CPP和1.42μg的PPF),因为这种组合在用于机械性伤害感受(Randall-Selitto试验)时会产生超相加性抗伤害感受作用。通过C反射和后放电测试,(±)-PPF和CPP的组合产生的抗伤害感受作用大于每种药物单独使用时的作用。我们得出结论,(±)-PPF和CPP组合的抗伤害感受作用可能在单关节炎大鼠中产生超相加性相互作用类型。

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