Patil Abhijit Anil, Vinayan K P, Roy Arun Grace
Department of Neurology, Division of Paediatric Neurology, Amrita Institute of Medical Sciences, Kochi, Kerala, India.
Ann Indian Acad Neurol. 2019 Jul-Sep;22(3):311-315. doi: 10.4103/aian.AIAN_229_18.
gene encodes a sodium-gated potassium channel subunit that plays an important role in regulating excitability in neurons. Quinidine is a partial antagonist of this channel. We report the clinical characteristics of two south Indian children with -related epileptic encephalopathy. Both of them had very high seizure burden which were resistant to antiepileptic and dietary therapy. Pharmacological response to quinidine in these children is described. Case 1 had 30% reduction in seizure burden at 20 mg/kg/day and 80% reduction at 36 mg/kg/day; case 2 had 30% reduction at 20 mg/kg/day. Serial electrocardiography was used to monitor the cardiotoxicity. Serum quinidine levels were not measured due to nonavailability. A critical review on the current status of targeted treatment of -related epileptic encephalopathies with quinidine is attempted.
基因编码一种钠门控钾通道亚基,该亚基在调节神经元兴奋性方面发挥重要作用。奎尼丁是该通道的部分拮抗剂。我们报告了两名患有与[相关基因缺失]相关癫痫性脑病的南印度儿童的临床特征。他们两人的癫痫发作负担都非常高,对抗癫痫药物和饮食疗法均耐药。描述了这些儿童对奎尼丁的药理反应。病例1在每日20mg/kg剂量时癫痫发作负担降低30%,在36mg/kg/日时降低80%;病例2在20mg/kg/日时降低30%。采用连续心电图监测心脏毒性。由于无法获取,未测量血清奎尼丁水平。本文尝试对目前使用奎尼丁靶向治疗与[相关基因缺失]相关癫痫性脑病的现状进行批判性综述。 (注:原文中“-related”处似乎有信息缺失,翻译时按“[相关基因缺失]”暂代以便语句通顺,你可根据实际情况修改。)
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