BTS 72664——一种新型中枢神经系统药物,具有潜在的抗惊厥、神经保护和抗偏头痛特性。

S. L. Smith, K. Thompson, B. Sargent, D. Heal
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引用次数: 12

摘要

BTS 72664, (R)-7-[1-(4-氯苯氧基)]乙基]-1,2,4-三唑(1,5- α)嘧啶,从一个旨在发现新型、广谱、非镇静的抗惊厥药物的研究项目中被确定为候选药物。BTS 72664可拮抗双库兰(BIC)和最大电休克(MES)引起的惊厥,ED(50)值分别为1.9和47.5 mg/kg。在啮齿类动物中,它具有广泛的活性,可预防微毒素、戊四氮、iv -氨基吡啶或NMDA引起的癫痫发作,并可预防ba -2小鼠和GEPR-9大鼠的听源性癫痫发作。BTS 72664在抗惊厥模型中的ED(50)与旋转棒和倒水平网格实验中运动损伤小鼠的TD(50)之间存在较大的差异,从而预测其缺乏镇静电位。BTS 72664的抗惊厥作用可能是通过增强通过微毒素敏感氯离子通道的氯离子电流,以及对Na(+)和NMDA通道的弱抑制来实现的。然而,它并不作用于苯二氮卓类药物的结合位点。BTS 72664除了治疗癫痫的潜在用途外,还可用于治疗中风。在永久性大脑中动脉(MCA)闭塞后15分钟开始,每隔12小时给予大鼠50 mg/kg p.o. x 4,使脑梗死面积减少31%(在损伤后2天测量),并加速功能行为模型的恢复。BTS 72664可防止大鼠皮质损伤引起的神经元外谷氨酸、甘氨酸和丝氨酸脑水平升高(参见皮质扩散抑制)。因此,它可能也有抗偏头痛的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
BTS 72664-- a novel CNS drug with potential anticonvulsant, neuroprotective, and antimigraine properties.
BTS 72664, (R)-7-[1-(4-chlorophenoxy)]ethyl]-1,2,4-triazolo(1,5-alpha)pyrimidine, was identified as a drug development candidate from a research program designed to discover novel, broad-spectrum, non-sedative anticonvulsant drugs. BTS 72664 antagonized bicuculline (BIC)- and maximal electroshock (MES)-induced convulsions with ED(50) values of 1.9 and 47.5 mg/kg p.o., respectively. In rodents, it has a wide spectrum of activity preventing seizures induced by picrotoxin, pentylenetetrazol, i.c.v. 4-aminopyridine or NMDA, and audiogenic seizures in DBA-2 mice and GEPR-9 rats. BTS 72664 was also effective in preventing convulsions in amygdala-kindled rats The lack of sedative potential was predicted on the basis of wide separation between ED(50) in anticonvulsant models and TD(50) for motor impairment in mice in rotating rod and inverted horizontal grid tests. BTS 72664 is likely to produce its anticonvulsant effect by enhancing chloride currents through picrotoxin-sensitive chloride channels, and by weak inhibition of Na(+) and NMDA channels. It does not act, however, at the benzodiazepine binding site. In addition to its potential use in the treatment of epilepsy BTS 72664 may be useful in the treatment of stroke. At 50 mg/kg p.o. x 4, given to rats at 12 hourly intervals, starting at 15 min after permanent occlusion of middle cerebral artery (MCA), it reduced cerebral infarct size by 31% (measured at 2 days after insult) and accelerated recovery in a functional behavioral model. BTS 72664 prevented increases in extraneuronal concentrations of glutamate, glycine and serine brain levels induced by a cortical insult to rats (cf. cortical spreading depression). It may, therefore, have also antimigraine activity.
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