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二氮嗪、克罗卡林和平尼地尔对大鼠脑皮质切片中肾上腺素能神经传递及⁸⁶Rb⁺外流的不同作用。

Differential effects of diazoxide, cromakalim and pinacidil on adrenergic neurotransmission and 86Rb+ efflux in rat brain cortical slices.

作者信息

Takata Y, Shimada F, Kato H

机构信息

Department of Pharmacology, Faculty of Pharmaceutical Sciences, Teikyo University, Kanagawa, Japan.

出版信息

J Pharmacol Exp Ther. 1992 Dec;263(3):1293-301.

PMID:1469635
Abstract

The effects of diazoxide, cromakalim and pinacidil on depolarization-evoked tritium overflow from the rat brain cortical slices preloaded with [3H]noradrenaline were studied. Diazoxide inhibited both transmural nerve stimulation (TNS)- and 25 mM K(+)-evoked tritium overflows more potently than cromakalim. Diazoxide effects were only partially antagonized and cromakalim ones were totally reversed by 1 microM glibenclamide. Diazoxide, but not cromakalim, reduced the 45 mM K(+)-evoked tritium overflow, which was not antagonized by glibenclamide. Both diazoxide and cromakalim stimulated 86Rb+ efflux to a similar extent, the effects being completely abolished by glibenclamide. Glibenclamide (> or = 3 microM) by itself enhanced the TNS-evoked tritium overflow. Pinacidil increased both TNS- and K+ (25 and 45 mM)-evoked tritium overflows with little effect on 86Rb+ efflux. Pinacidil-induced increase in the TNS-evoked tritium overflow was still observed in the presence of cocaine or hydrocortisone. Pinacidil failed to affect the inhibitory action of xylazine on the TNS-evoked tritium overflow, whereas phentolamine attenuated it. These results indicate that ATP-sensitive K+ channels are present in the adrenergic nerve endings of rat brain. These channels seem to be pharmacologically different from those reported for vascular smooth muscles and pancreatic beta-cells.

摘要

研究了二氮嗪、克罗卡林和吡那地尔对预先加载[3H]去甲肾上腺素的大鼠脑皮质切片去极化诱发的氚溢出的影响。二氮嗪比克罗卡林更有效地抑制跨壁神经刺激(TNS)和25 mM K(+)诱发的氚溢出。1 microM格列本脲仅部分拮抗二氮嗪的作用,而完全逆转克罗卡林的作用。二氮嗪可降低45 mM K(+)诱发的氚溢出,但克罗卡林无此作用,且格列本脲不能拮抗二氮嗪的这一作用。二氮嗪和克罗卡林刺激86Rb+外流的程度相似,格列本脲可完全消除其作用。格列本脲(≥3 microM)本身可增强TNS诱发的氚溢出。吡那地尔增加TNS和K+(25和45 mM)诱发的氚溢出,对86Rb+外流影响很小。在存在可卡因或氢化可的松的情况下,仍可观察到吡那地尔诱导的TNS诱发的氚溢出增加。吡那地尔不影响赛拉嗪对TNS诱发的氚溢出的抑制作用,而酚妥拉明可减弱该作用。这些结果表明,大鼠脑肾上腺素能神经末梢存在ATP敏感性钾通道。这些通道在药理学上似乎与报道的血管平滑肌和胰腺β细胞的通道不同。

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