Institute of Drug Research, School of Pharmacy, Faculty of Medicine, The Hebrew University of Jerusalem, Jerusalem, Israel.
Istituto di Ricerche Farmacologiche Mario Negri IRCCS, Milano, Italy.
Pharmacol Ther. 2021 Oct;226:107866. doi: 10.1016/j.pharmthera.2021.107866. Epub 2021 Apr 22.
In 2020, racemic-fenfluramine was approved in the U.S. and Europe for the treatment of seizures associated with Dravet syndrome, through a restricted/controlled access program aimed at minimizing safety risks. Fenfluramine had been used extensively in the past as an appetite suppressant, but it was withdrawn from the market in 1997 when it was found to cause cardiac valvulopathy. Available evidence indicates that appetite suppression and cardiac valvulopathy are mediated by different serotonergic mechanisms. In particular, appetite suppression can be ascribed mainly to the enantiomers d-fenfluramine and d-norfenfluramine, the primary metabolite of d-fenfluramine, whereas cardiac valvulopathy can be ascribed mainly to d-norfenfluramine. Because of early observations of markedly improved seizure control in some forms of epilepsy, fenfluramine remained available in Belgium through a Royal Decree after 1997 for use in a clinical trial in patients with Dravet syndrome at average dosages lower than those generally prescribed for appetite suppression. More recently, double-blind placebo-controlled trials established its efficacy in the treatment of convulsive seizures associated with Dravet syndrome and of drop seizures associated with Lennox-Gastaut syndrome, at doses up to 0.7 mg/kg/day (maximum 26 mg/day). Although no cardiovascular toxicity has been associated with the use of fenfluramine in epilepsy, the number of patients exposed to date has been limited and only few patients had duration of exposure longer than 3 years. This article analyzes available evidence on the mechanisms involved in fenfluramine-induced appetite suppression, antiseizure effects and cardiovascular toxicity. Despite evidence that stimulation of 5-HT receptors (the main mechanism leading to cardiac valvulopathy) is not required for antiseizure activity, there are many critical gaps in understanding fenfluramine's properties which are relevant to its use in epilepsy. Particular emphasis is placed on the remarkable lack of publicly accessible information about the comparative activity of the individual enantiomers of fenfluramine and norfenfluramine in experimental models of seizures and epilepsy, and on receptors systems considered to be involved in antiseizure effects. Preliminary data suggest that l-fenfluramine retains prominent antiseizure effects in a genetic zebrafish model of Dravet syndrome. If these findings are confirmed and extended to other seizure/epilepsy models, there would be an incentive for a chiral switch from racemic-fenfluramine to l-fenfluramine, which could minimize the risk of cardiovascular toxicity and reduce the incidence of adverse effects such as loss of appetite and weight loss.
2020 年,在美国和欧洲,通过限制/控制准入方案,批准使用外消旋芬氟拉明治疗 Dravet 综合征相关癫痫发作,该方案旨在尽量降低安全风险。芬氟拉明过去曾广泛用作食欲抑制剂,但 1997 年因发现会导致心脏瓣膜病而被撤出市场。现有证据表明,食欲抑制和心脏瓣膜病是由不同的 5-羟色胺能机制介导的。特别是,食欲抑制主要归因于外消旋芬氟拉明的对映异构体 d-芬氟拉明和 d-去甲芬氟拉明,以及 d-芬氟拉明的主要代谢物,而心脏瓣膜病主要归因于 d-去甲芬氟拉明。由于早期观察到一些形式的癫痫发作控制明显改善,比利时通过皇家法令,在 1997 年后继续提供芬氟拉明,用于 Dravet 综合征患者的临床试验,剂量低于一般用于抑制食欲的剂量。最近,双盲安慰剂对照试验证实了其在治疗 Dravet 综合征相关惊厥性癫痫发作和 Lennox-Gastaut 综合征相关跌倒性癫痫发作的疗效,剂量高达 0.7mg/kg/天(最大 26mg/天)。虽然目前尚未发现芬氟拉明在癫痫中的使用与心血管毒性有关,但暴露于该药物的患者人数有限,只有少数患者的暴露时间超过 3 年。本文分析了与芬氟拉明诱导的食欲抑制、抗癫痫作用和心血管毒性相关的现有证据。尽管有证据表明,5-羟色胺受体的刺激(导致心脏瓣膜病的主要机制)不是抗癫痫活性所必需的,但对于芬氟拉明在癫痫中的作用,仍有许多关键问题尚不清楚。特别强调的是,在癫痫发作和癫痫的实验模型中,芬氟拉明和去甲芬氟拉明的单个对映异构体的比较活性以及被认为与抗癫痫作用相关的受体系统方面,存在显著缺乏公开获取的信息。初步数据表明,l-芬氟拉明在 Dravet 综合征的遗传斑马鱼模型中保留了显著的抗癫痫作用。如果这些发现得到证实并扩展到其他癫痫/癫痫发作模型,将促使从外消旋芬氟拉明向 l-芬氟拉明进行手性转换,从而最大限度地降低心血管毒性风险,并减少食欲减退和体重减轻等不良反应的发生率。
