Guedes R C, de Azeredo F A, Hicks T P, Clarke R J, Tashiro T
Departamento de Nutriçao, Universidade Federal de Pernambuco, Recife,Brazil.
Exp Brain Res. 1987;69(1):113-8. doi: 10.1007/BF00247034.
The slow potential change (spc) accompanying spreading depression (SD) was studied in rats and in a seizure-sensitive strain of Mongolian gerbil under three different experimental paradigms, each involving the use of naloxone. Gerbils undergoing electroconvulsive shock treatment displayed SD during the post-ictal phase, which was blocked by the intraperitoneal (i.p.) administration of naloxone (20-50 mg kg-1). Topical application of naloxone to the exposed cortex of the anaesthetized gerbil and rat blocked the spc of SD evoked by KCl. Microiontophoretic ejection of naloxone during extracellular recordings reversed cell refractoriness following the spc, demonstrated by the observation of a maintained sensitivity to iontophoretic pulses of glutamate. The results suggest a possible involvement of naloxone-sensitive processes in the mechanism responsible for cortical SD.
在三种不同的实验范式下,对大鼠和癫痫敏感型蒙古沙鼠的伴随扩散性抑制(SD)的慢电位变化(spc)进行了研究,每种范式均涉及使用纳洛酮。接受电惊厥休克治疗的沙鼠在发作后期出现SD,腹腔注射(i.p.)纳洛酮(20 - 50 mg kg-1)可阻断该现象。向麻醉的沙鼠和大鼠暴露的皮层局部应用纳洛酮可阻断由氯化钾诱发的SD的spc。在细胞外记录期间通过微量离子电泳注入纳洛酮,可逆转spc后的细胞不应期,这可通过观察对谷氨酸离子电泳脉冲保持敏感性得以证明。结果表明,对纳洛酮敏感的过程可能参与了皮层SD的发生机制。