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产前接触抗癫痫药物后的出生缺陷。

Birth defects after prenatal exposure to antiepileptic drugs.

作者信息

Perucca Emilio

机构信息

Clinical Pharmacology Unit, Department of Internal Medicine and Therapeutics, University of Pavia, and Laboratories for Diagnostics and Applied Biological Research, Institute of Neurology, IRCCS C Mondino Foundation, Pavia, Italy.

出版信息

Lancet Neurol. 2005 Nov;4(11):781-6. doi: 10.1016/S1474-4422(05)70224-6.

Abstract

BACKGROUND

Exposure to antiepileptic drugs (AEDs) in the first trimester of pregnancy has been associated with an increased risk of major congenital anomalies (MCAs) in offspring. Most of the studies, however, have been fraught with methodological shortcomings, and differences in ascertainment methods and classifications prevent meaningful data pooling. Individual studies lacked the statistical power to assess comparative risks associated with specific AEDs.

RECENT DEVELOPMENTS

Several larger-scale studies, including collaborative multinational registries, have been set up to compare MCA risks associated with different treatments, including newer generation AEDs. Results have largely been consistent with the notion that monotherapy with the most commonly used AEDs is associated with an increase in risk of MCAs by two to three times, and that the magnitude of risk increases in offspring exposed to polytherapy. Available evidence does not suggest that epilepsy per se is associated with a major increase in the risk of MCAs. Almost all studies have suggested that exposure to valproic acid is associated with a greater incidence of MCAs than other AEDs. Valproic acid is also the only AED for which a dose-dependency has been confirmed in several studies: the increase in risk of MCAs, compared with other AEDs, is especially evident at doses above 800-1000 mg/day. Data from the North American registry have suggested that phenobarbital may also have a higher teratogenic risk compared with AEDs other than valproic acid, but evidence remains inconclusive. Information about effects on fetuses of newer generation AEDs other than lamotrigine and oxcarbazepine is scant. Although teratogenic effects of lamotrigine and oxcarbazepine have not been established with certainty, none of the investigations to date identified any statistically significant difference in rates of MCAs between infants exposed to lamotrigine or oxcarbazepine and infants exposed to carbamazepine. In the case of lamotrigine, moreover, a positive correlation between maternal dose and rates of MCAs has been identified. WHERE NEXT?: Collaborative pregnancy registries worldwide are at work to fill remaining gaps in knowledge. Issues to be addressed include the comparative risks associated with phenobarbital, with low-dose valproic acid, with newer generation AEDs, and with specific AED combinations; the influence of potential confounders; and the interaction of AED-associated risks with other risk factors, such as genetic profiles. Large scale studies may also clarify whether individual AEDs differ in their ability to cause specific anomalies. Finally, studies are urgently needed to investigate other potential adverse effects of AED exposure, with special reference to effects on postnatal intellectual development.

摘要

背景

孕期头三个月接触抗癫痫药物(AEDs)与后代发生重大先天性畸形(MCAs)的风险增加有关。然而,大多数研究存在方法学上的缺陷,且确定方法和分类的差异阻碍了有意义的数据汇总。个别研究缺乏评估与特定AEDs相关的比较风险的统计能力。

最新进展

已经开展了几项大规模研究,包括跨国合作登记处,以比较与不同治疗方法相关的MCA风险,包括新一代AEDs。结果在很大程度上与以下观点一致:使用最常用的AEDs进行单药治疗会使MCA风险增加两到三倍,并且接受联合治疗的后代的风险程度会增加。现有证据并不表明癫痫本身会使MCA风险大幅增加。几乎所有研究都表明,接触丙戊酸比接触其他AEDs导致MCA的发生率更高。丙戊酸也是唯一在多项研究中已证实存在剂量依赖性的AED:与其他AEDs相比,MCA风险增加在每日剂量高于800 - 1000毫克时尤为明显。北美登记处的数据表明,与除丙戊酸之外的AEDs相比,苯巴比妥可能也具有更高的致畸风险,但证据仍不确凿。关于除拉莫三嗪和奥卡西平之外的新一代AEDs对胎儿影响的信息很少。虽然拉莫三嗪和奥卡西平的致畸作用尚未确定,但迄今为止的所有调查均未发现接触拉莫三嗪或奥卡西平的婴儿与接触卡马西平的婴儿之间的MCA发生率存在任何统计学上的显著差异。此外,就拉莫三嗪而言,已确定母体剂量与MCA发生率之间存在正相关。

下一步方向

全球范围内的合作妊娠登记处正在努力填补知识空白。需要解决的问题包括与苯巴比妥、低剂量丙戊酸、新一代AEDs以及特定AED组合相关的比较风险;潜在混杂因素的影响;以及AED相关风险与其他风险因素(如基因图谱)的相互作用。大规模研究还可能阐明个别AEDs在导致特定异常方面的能力是否存在差异。最后,迫切需要开展研究以调查AED暴露的其他潜在不良影响,特别是对出生后智力发育的影响。

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