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急性偏头痛治疗:新型药物

Acute migraine therapy: the newer drugs.

作者信息

Schoenen J

机构信息

Department of Neurology CHR Citadelle, University of Liège, Belgium.

出版信息

Curr Opin Neurol. 1997 Jun;10(3):237-43. doi: 10.1097/00019052-199706000-00012.

Abstract

In 1996, our knowledge of acute antimigraine therapy expanded in three major areas. First, large surveys have confirmed the remarkable efficacy profile of sumatriptan in clinical practice. No satisfying clinical, pharmacokinetic or genetic explanations were found for its major shortcomings: nonresponders, headache recurrence and noncardiac chest symptoms. Second, the novel 5-HT1B/D agonists zolmitriptan (311C90), rizatriptan (MK-462), eletriptan (UK-116,044), avitriptan (BMS-180048) and alniditan (R091274) were all proved superior to placebo for attack treatment, but their advantages over sumatriptan are yet to be analysed in more detail. A higher lipophilicity explains (except for alniditan) their greater oral bioavailability and better central nervous system penetration. A central action now proved experimentally in animals and in humans for 5-HT1B/D agonists such as zolmitriptan may be advantageous for the antimigraine efficacy, but it could also increase sedation. Third, an endothelin (Ro470203, bosentan) and a neurokinin 1 (RPR100893) receptor antagonist were found to be ineffective in migraine. Both compounds are potent inhibitors of neurogenic plasma extravasation in rat dura mater, which might suggest that this pharmacological property does not necessarily predict efficacy in aborting migraine attacks.

摘要

1996年,我们在急性偏头痛治疗方面的知识在三个主要领域得到了扩展。首先,大规模调查证实了舒马曲坦在临床实践中的显著疗效。对于其主要缺点,即无反应者、头痛复发和非心脏性胸部症状,未找到令人满意的临床、药代动力学或遗传学解释。其次,新型5-HT1B/D激动剂佐米曲坦(311C90)、利扎曲坦(MK-462)、依立曲坦(UK-116,044)、阿维曲坦(BMS-180048)和阿尼地坦(R091274)在发作治疗中均被证明优于安慰剂,但其相对于舒马曲坦的优势尚待更详细地分析。较高的亲脂性(阿尼地坦除外)解释了它们更高的口服生物利用度和更好的中枢神经系统渗透性。现已在动物和人类实验中证明,佐米曲坦等5-HT1B/D激动剂的中枢作用可能有利于抗偏头痛疗效,但也可能增加镇静作用。第三,发现一种内皮素(Ro470203,波生坦)和一种神经激肽1(RPR100893)受体拮抗剂对偏头痛无效。这两种化合物都是大鼠硬脑膜中神经源性血浆外渗的有效抑制剂,这可能表明这种药理特性不一定能预测中止偏头痛发作的疗效。

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