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首页> 外文期刊>European Journal of Pharmacology: An International Journal >The AMPA receptor/Na(+) channel blocker BIIR 561 CL is protective in a model of global cerebral ischaemia.
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The AMPA receptor/Na(+) channel blocker BIIR 561 CL is protective in a model of global cerebral ischaemia.

机译:AMPA受体/ Na(+)通道阻滞剂BIIR 561 CL在全脑缺血模型中具有保护作用。

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In this study, we investigated whether the novel neuroprotective compound dimethyl-[2-[2-(3-phenyl-[1,2,4]oxadiazol-5-yl)-phenoxy]-ethyl]-amine hydrochloride, BIIR 561 CL, a combined non-competitive antagonist of AMPA receptors and blocker of voltage-gated Na+ channels, is protective in a rat model of severe global ischaemia. BIIR 561 CL administered immediately after 10 min of ischaemia (occlusion of both carotid arteries plus reduction of arterial blood pressure to 38-40 mm Hg) significantly reduced hippocampal damage at 4 x 26.8 mg/kg (subcutaneous injections). The competitive AMPA receptor antagonist 2,3-dihydro-6-nitro-7-sulfamoyl-benz(F)quinoxaline, NBQX, was used as a reference compound and was protective at 3x30 mg/kg (intraperitoneal and/or subcutaneous administration). BIIR 561 CL significantly reduced the ischaemia-induced premature mortality from 33.6% in the controls to 14.3%, whereas NBQX treatment had no statistically significant effect.Thus, BIIR 561 CL could be shown to reduce hippocampal damage and premature mortality in a model of severe global ischaemia. A compound with these properties might be an interesting candidate for the treatment of disorders related to global cerebral ischaemia in man.
机译:在这项研究中,我们调查了新型神经保护化合物二甲基-[2- [2-(3-苯基-[1,2,4]恶二唑-5-基)-苯氧基]-乙基]-胺盐酸盐,BIIR 561 CL ,AMPA受体的非竞争性拮抗剂和电压门控性Na +通道的组合拮抗剂,在严重的全脑缺血大鼠模型中具有保护作用。缺血10分钟后立即给予BIIR 561 CL(两条颈动脉闭塞,动脉血压降至38-40 mm Hg),以4 x 26.8 mg / kg(皮下注射)可显着降低海马损伤。竞争性AMPA受体拮抗剂2,3-二氢-6-硝基-7-氨磺酰基-苯并(F)喹喔啉(NBQX)作为参考化合物,在3x30 mg / kg的剂量下具有保护作用(腹膜内和/或皮下给药)。 BIIR 561 CL可以将缺血引起的过早死亡从对照组的33.6%降低到14.3%,而NBQX治疗没有统计学意义。因此,BIIR 561 CL可以证明在重症模型中可以降低海马损伤和过早死亡全球缺血。具有这些特性的化合物可能是治疗与人类全脑缺血有关的疾病的有趣候选物。

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