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2,3-丁二酮一肟通过促进γ-氨基丁酸(GABA)激活电流,保护小鼠免受印防己毒素的惊厥作用。

2,3-Butanedione monoxime protects mice against the convulsant effect of picrotoxin by facilitating GABA-activated currents.

作者信息

Brightman T, Ye J H, Ortiz-Jimenez E, Flynn E J, Wu W H, McArdle J J

机构信息

Department of Pharmacology and Toxicology, New Jersey Medical School (UMDNJ), Newark 07103-2714, USA.

出版信息

Brain Res. 1995 Apr 24;678(1-2):110-6. doi: 10.1016/0006-8993(95)00175-p.

Abstract

While adult mice receiving picrotoxin (PTX) alone responded with clonic and tonic-clonic seizures, this response was greatly suppressed for mice simultaneously injected with 2,3-butanedione monoxime (BDM). For example, 60% and 10% of the mice convulsed when injected (i.p.) with 3.0 mg/kg PTX alone or PTX plus 205 mg/kg of BDM, respectively. In contrast, a non-oxime analogue of BDM, 2,3-butanedione (BTD), did not have this anticonvulsant effect. In order to explore the basis for the anticonvulsant effect of BDM, we recorded GABA-activated currents (IGABA) of frontal cortical as well as ventromedial hypothalamic neurons before, during and after exposure to this oxime. BDM had a biphasic effect on IGABA. That is, high concentrations (100 microM-40 mM) decreased and lower concentrations (0.01 microM-0.001 microM) potentiated IGABA; these effects of BDM reversed upon washout of the oxime. In contrast, BTD had no effect on IGABA. Finally, when 0.001 microM BDM, 10-30 microM PTX and GABA were co-applied the inhibitory effect of the toxin on IGABA was markedly suppressed. These data suggest that the anticonvulsant effect of oximes involves facilitation of the inhibitory action of GABA.

摘要

单独接受印防己毒素(PTX)的成年小鼠会出现阵挛性和强直 - 阵挛性癫痫发作,但同时注射2,3 - 丁二酮单肟(BDM)的小鼠这种反应会受到极大抑制。例如,腹腔注射3.0 mg/kg PTX单独或PTX加205 mg/kg BDM时,分别有60%和10%的小鼠惊厥。相比之下,BDM的非肟类似物2,3 - 丁二酮(BTD)没有这种抗惊厥作用。为了探究BDM抗惊厥作用的基础,我们记录了额叶皮质以及下丘脑腹内侧神经元在接触这种肟之前、期间和之后的GABA激活电流(IGABA)。BDM对IGABA有双相作用。也就是说,高浓度(100 microM - 40 mM)会降低IGABA,而低浓度(0.01 microM - 0.001 microM)会增强IGABA;冲洗掉肟后,BDM的这些作用会逆转。相比之下,BTD对IGABA没有影响。最后,当共同应用0.001 microM BDM、10 - 30 microM PTX和GABA时,毒素对IGABA的抑制作用明显受到抑制。这些数据表明肟的抗惊厥作用涉及促进GABA的抑制作用。

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