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Efficacy and tolerability of the new antiepileptic drugs: comparison of two recent guidelines

机译:新型抗癫痫药的功效和耐受性:两项最新指南的比较

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Until the early 1990s six major compounds (carbamazepine, ethosuximide, phenobarbital, phenytoin. primidone, and valproic acid) were available for the treatment of epilepsy. However, these drugs have pharmacokinetic limitations, teratogenic potential, and a negative effect on cognitive functions that impairs the quality of patients' lives and limits the use of these drugs in some patients. In addition, 20-30% of patients are refractory to these drugs. The development of ten new antiepileptic drugs (vigabatrin, felbamate. gabapentin, lamotrigine. topiramate, tiagabine, oxcarbazepine, levetiracetam, zonisamide, and pregabalin) has expanded treatment options. The newer drugs may be better tolerated, have fewer drug interactions, and seem to affect cognitive functions to a lesser extent than old drugs. Guidelines on the use of new antiepileptic drugs have been developed in the USA and in the UK. Both guidelines offer a clear picture of the efficacy, safety, and tolerability of the new antiepileptic drugs and agree on their use as add-on treatment in patients who do not respond to conventional drugs. The guidelines differ in the type and strength of recommendations. Whereas the US guidelines recommend treatment in newly diagnosed epilepsy with a standard drug or a new drug depending on the individual patient's characteristics, the UK guidelines recommend that a new antiepileptic drug should be considered only if there is no benefit from an old antiepileptic drug, an old drug is contraindicated, there is a previous negative experience with the same drug, or the patient is a woman of childbearing potential. The limited amount of information on the new antiepileptic drugs may explain the discrepancies among the two guidelines and between these and other recommendations. Comparative, pragmatic, long-term and open trials should be done to show long-term efficacy and comparative features of the new antiepileptic drugs, and to better assess the effect on quality-of-life, cost-effectiveness, tolerability, and teratogenic potential. In addition, the conflicts should be resolved between the needs of the regulatory bodies and those of the treating physicians. Finally, there is a need for trial designs to be standardised.
机译:直到1990年代初,已有六种主要化合物(卡马西平,乙妥西米特,苯巴比妥,苯妥英钠,普利米酮和丙戊酸)可用于治疗癫痫。但是,这些药物具有药代动力学的局限性,致畸性,并且对认知功能有负面影响,这损害了患者的生活质量并限制了某些患者使用这些药物。此外,有20-30%的患者对这些药物无效。十种新的抗癫痫药的开发(维格巴林,非拜贝特,加巴喷丁,拉莫三嗪,托吡酯,替加滨,奥卡西平,左乙拉西坦,唑尼沙胺和普瑞巴林)扩大了治疗选择。与旧药物相比,较新的药物可能具有更好的耐受性,较少的药物相互作用并且似乎对认知功能的影响程度较小。在美国和英国已经制定了使用新的抗癫痫药的指南。两项指南均清楚地显示了新抗癫痫药的功效,安全性和耐受性,并同意将其用作对常规药物无反应的患者的附加治疗。指南的建议类型和强度不同。美国指南建议根据个体患者的特征,使用标准药物或新药治疗新近诊断的癫痫病,英国指南建议仅在旧抗癫痫药无益处的情况下才应考虑使用新抗癫痫药。禁忌使用旧药物,以前曾使用过相同的药物,或者患者是有生育能力的女性。有关新抗癫痫药的信息量有限,可能解释了这两个指南之间以及这些建议与其他建议之间的差异。应该进行比较,实用,长期和开放性试验,以显示新抗癫痫药物的长期疗效和比较特征,并更好地评估其对生活质量,成本效益,耐受性和致畸性的影响。此外,应解决监管机构和主治医师之间的矛盾。最后,需要使试验设计标准化。

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