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抗惊厥药乙巴比妥(安替隆,二甲基磷酸甲酯)与苯巴比妥对正常人类志愿者毒性作用的比较。

A comparison of the toxicity effects of the anticonvulsant eterobarb (antilon, DMMP) and phenobarbital in normal human volunteers.

作者信息

Smith D B, Goldstein S G, Roomet A

出版信息

Epilepsia. 1986 Mar-Apr;27(2):149-55. doi: 10.1111/j.1528-1157.1986.tb03518.x.

Abstract

Renewed corporate interest in the anticonvulsant drug eterobarb justified renewed clinical and experimental interest in this drug. The unique and clinically intriguing feature of eterobarb is that while sharing the anticonvulsant properties of other barbiturates, the hypnotic side effects usually associated with barbiturates appear to be absent in animal studies and greatly reduced in clinical trials. This study was designed to compare the hypnotic effects of eterobarb with those of phenobarbital in healthy normal human volunteers using a double-blind, placebo-controlled design. Both clinical and neuropsychological parameters of toxicity were measured, while blood barbiturate levels were monitored to correlate neurobehavioral changes with total barbiturate level. As expected, there is a linear relationship between the degree of toxicity and the barbiturate level, but much higher barbiturate levels were tolerated without toxicity by subjects taking eterobarb. For ethical reasons, subjects were not maintained at high levels of toxicity over the 14-week trial. However, both eterobarb and phenobarbital recipients failed to show significant improved performance on Digits Total, a test of mental flexibility (Digit Symbol Substitution). In addition, phenobarbital recipients showed the only significant decrement of performance on Digits Total, and they failed to improve significantly on Trails-Part A, in which all other groups improved. This study confirms that eterobarb has less hypnotic side effects and less neurotoxicity than does phenobarbital.

摘要

企业对抗惊厥药物乙巴比妥重新产生兴趣,这使得人们对该药物重新展开临床和实验研究。乙巴比妥独特且在临床上引人关注的特点是,虽然它具有其他巴比妥类药物的抗惊厥特性,但在动物研究中,通常与巴比妥类药物相关的催眠副作用似乎并不存在,在临床试验中也大幅减少。本研究旨在采用双盲、安慰剂对照设计,比较乙巴比妥与苯巴比妥对健康正常人类志愿者的催眠效果。同时测量了毒性的临床和神经心理学参数,并监测血中巴比妥酸盐水平,以将神经行为变化与巴比妥酸盐总水平相关联。正如预期的那样,毒性程度与巴比妥酸盐水平之间存在线性关系,但服用乙巴比妥的受试者能耐受高得多的巴比妥酸盐水平而无毒性。出于伦理原因,在为期14周的试验中,未让受试者维持在高毒性水平。然而,服用乙巴比妥和苯巴比妥的受试者在数字总和测试(一项精神灵活性测试,数字符号替换)中均未表现出明显的成绩改善。此外,服用苯巴比妥的受试者在数字总和测试中表现出唯一显著的成绩下降,并且在连线测验A部分中未显著改善,而其他所有组在该部分都有改善。本研究证实,乙巴比妥比苯巴比妥具有更少的催眠副作用和神经毒性。

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