首页> 外文期刊>Japanese Journal of Pharmacology >THE ANTICONVULSANT ACTIVITY OF ETHYL α-PHENYLBUTYROYL ALLOPHANATE (P-5257)
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THE ANTICONVULSANT ACTIVITY OF ETHYL α-PHENYLBUTYROYL ALLOPHANATE (P-5257)

机译:α-苯甲酸丁二醇酯(P-5257)的抗惊厥活性

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References(26) Cited-By(1) Cyclic derivatives of barbiturates (1, 2), hydantoins (3, 4), oxazolidines (5, 6), succinimides (7) and straight-chain derivatives of phenylacetylurea (8-10) have widely been used as the therapeutic antiepileptics. Phenylacetylurea (phenurone) was introduced by opening the hydantoin ring. The compound has been shown being a unique anticonvulsant for the treatment of the psychomotor epilepsy which had been relatively refractory to the other antiepileptics (11, 12). However, a number of side effects such as gastrointestinal disturbance, hepatotoxicity and personality disturbance, all inherent to the compound have limited the clinical use (11, 13). Further studies for the elimination of the side effects of the phenurone have introduced pheneturide (9) and N-acetyl pheneturide (crampol) (10) which still showed some similar side effects. Looking for less toxic and more effective anticonvulsant extensive studies of a series of allophanate compounds have chemically and pharmacologically been in succession in this laboratory. Among the derivatives studied, ethyl α-phenylbutyroyl allophanate (P-5257) has proved considerably unique in the anticonvulsant activity being highly potent, longer-durating and less toxic. The pharmacological effects of the compound compared with those of the derivatives of phenurone are described in the present report.
机译:参考文献(26)被引用的By(1)巴比妥酸盐(1、2),乙内酰脲(3、4),恶唑烷(5、6),琥珀酰亚胺(7)和苯乙酰脲(8-10)的直链衍生物的环状衍生物已广泛用作治疗性抗癫痫药。通过打开乙内酰脲环引入苯乙酰脲(苯乙酮)。该化合物已显示是治疗精神运动性癫痫的独特抗惊厥药,对其他抗癫痫药相对较难治疗(11、12)。然而,该化合物固有的许多副作用,如胃肠道疾病,肝毒性和人格障碍,限制了其临床应用(11、13)。为消除菲咯酮的副作用而进行的进一步研究已经引入了苯乙硫脲(9)和N-乙酰基苯乙脲(crampol)(10),它们仍显示出一些相似的副作用。为了寻找毒性更小,更有效的抗惊厥药,该实验室已对一系列脲基甲酸酯化合物进行了广泛的化学和药理研究。在研究的衍生物中,已证明α-苯基丁酰脲基甲酸酯乙酯(P-5257)的独特之处在于其抗惊厥活性强,持续时间长且毒性小。在本报告中描述了该化合物与菲咯酮衍生物相比的药理作用。

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