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find Author "廖卫平" 5 results
  • 癫痫性脑病相关基因的致病潜力评估

    Release date:2018-07-18 02:17 Export PDF Favorites Scan
  • Molecular characteristics of SCN1A mutation causing partial epilepsy with febrile seizures plus

    ObjectiveTo explore the molecular characteristics of partial epilepsy with febrile seizures plus(PEFS+). MethodsWe systematically reviewed all SCN1A mutation-related publications that published between Jan.2000 and Dec.2014 on Pubmed and established a database of SCN1A mutations (http://www.gzneurosci.com/SCN1Adatabase/). The characteristics of mutations that cause PEFS+ were analyzed and compared with that of severe myoclonic epilepsy in infancy (SMEI). ResultsThe database included 1, 257 SCN1A mutations, which identified from 1, 727 unrelated cases. In which there were 30 mutations, from 32 unrelated cases, were associated with PEFS+. 76.7% (23/30) mutations were missense, of which 47.8% (11/23) were located on pore region. Significant difference in the percentage of truncation mutation was observed between PEFS+ and SMEI (P < 0.05). There was no significant difference in the percentage of missense mutation that located on the pore region between PEFS+ and SMEI; but the differ significantly in D-value of the missense mutations, which quantified the alteration of amino acid(P=0.042, rank sum test). ConclusionsPEFS+, which distinguishes from GEFS+ and SMEI in clinical and molecular characteristics, is a special phenotype of epilepsy that is associated with SCN1A mutations.

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  • GABRB3突变引发GABAA受体突触聚集差异化导致轻重不一的癫痫综合征

    Release date:2020-01-09 08:49 Export PDF Favorites Scan
  • Adjunctive lacosamide for partial-onset seizures: efficacy and safety results from a randomized placebo-controlled trial

    ObjectivesTo evaluate the efficacy and safety of lacosamide (200mg/d and 400mg/d)when added to 1 to 3 antiepileptic drugs (AEDs) in adults with uncontrolled partial-onset seizures. MethodsDuring this multicenter, double-blind, placebo-controlled trial, patients were randomized to placebo or lacosamide 200 or 400mg/day after an 8-week baseline period. Lacosamide was titrated in weekly increments to target dose over 4 weeks and maintained for 12 weeks followed by 12 weeks for withdrawal. The reductions of seizure frequence during maintain period and proportion of ≥50% reduction of seizures frequence were analysed. Besides,adverse effects were also recorded. ResultsFive hundred fourty patients were randomized, 515 patients completed the trial (Full analysis set, FAS), including 394 were per-protocol set (PPS). The reduction of seizure frequence during maintain period every 4 weeks among 200mg/d,400mg/d group and placebo group were 26.35%,40.12%,21.69%(P=0.000 5) and 25.61%,46.86%,23.06%(P<0.000 1), respectively in FAS and PPS. The proportion of ≥50% reduction of seizures frequence among three groups were 29.82%,38.15%,22.49%(P=0.006 8) and 27.94%,42.37%,22.86%(P=0.002 3), respectively in FAS and PPS. The incidences of adverse events were 5.84%, 36.11%, 19.55% among three groups. Compared with each other, there was statistic significance between 400mg/d and placebo groups. ConclusionIn this trial, adjunctive lacosamide significantly reduced seizure frequency in patients with uncontrolled partial-onset seizures. Along with favorable pharmacokinetic and tolerability profiles, these results support further development of lacosamide as an AED.

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  • 《癫痫发作分类标准更新:国际抗癫痫联盟立场声明》中国专家解读

    基于2017版癫痫发作分类框架,国际抗癫痫联盟(International League Against Epilepsy,ILAE)完成了癫痫发作操作性分类标准的更新。本次修订由ILAE执行委员会任命的37人工作组共同完成:通过改良Delphi法(共识阈值设定为超过三分之二的多数)公开征求意见后形成修订方案。该修订方案在ILAE 官网公示征求意见后,执委会任命7名专家组成修订小组对反馈意见进行整合,最终更新的分类标准于2025年4月在Epilepsia上发表。更新后的分类标准延续四大主要发作类别:局灶性、全面性、未知是否为局灶性或全面性和无法分类的发作,共包含4个主要类别和21种具体发作类型,并特别注重非英语语种的术语可译性,旨在为从资源有限地区到高级专科癫痫中心的所有癫痫从业人员建立统一术语体系,并为患者及照护者提供通俗易懂的表述。鉴于癫痫发作分类在癫痫诊断和治疗中的重要作用,本文融合中国癫痫领域专家解读《癫痫发作分类标准更新:国际抗癫痫联盟立场声明》并形成共识,旨在推进该分类标准在我国癫痫领域临床和科研中的应用。

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