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氯胺酮用于癫痫持续状态:何时才是现在?

Ketamine in Status Epilepticus: How Soon Is Now?

作者信息

Magro Giuseppe

机构信息

Department of Neurology, Lamezia Terme Hospital, 88046 Catanzaro, Italy.

出版信息

Neurol Int. 2025 May 28;17(6):83. doi: 10.3390/neurolint17060083.

Abstract

Status epilepticus (SE) is a neurological emergency. Current evidence dictates a step-by-step approach with a first line of therapy consisting of benzodiazepines (BDZs). In many situations, the currently approved approach does not terminate a BDZ-resistant SE. This happens in Stage 1 Plus, a framework designed by the author to recognize cases of probable benzodiazepine-resistant status epilepticus even before treatment initiation. These cases include Prolonged SE (SE lasting > 10 min), the absence of prominent motor phenomena, and acute etiology (primary central nervous system etiologies most of all). BDZ-refractory SE cases (Stage 1 Plus) might require a different approach, one targeting the unresponsive GABA signaling state mediated by NMDA/AMPA receptors, such as combined polytherapy with Ketamine from the start. These considerations stem from the receptor trafficking hypotheses: in prolonged seizure activity and primary central nervous system etiologies, GABA receptors get internalized and move away from synapses, and therefore, SE becomes resistant to BDZ. A rational polytherapy that might restore the unresponsiveness to BDZ in SE should include NMDA antagonists, such as Ketamine. Ketamine has proven effective in many experimental models of status epilepticus, and much evidence is gathering supporting its use in humans, especially in refractory and super-refractory SE. We lack studies evaluating combined polytherapy in SE, especially in the early phases. The author suggests here that Ketamine should be used along with first-line BDZ in the early SE stage falling in the category of Stage 1 Plus and as a first-line anesthetic infusion drug in refractory SE, especially in cases progressing from Stage 1 Plus, eventually adding continuous midazolam/propofol infusion in later phases. This systematic review's objective is to summarize the presently available evidence of the early use of combined polytherapy that includes Ketamine, along with the currently available evidence of Ketamine use in early, established, and refractory SE. Nine studies were included. Boluses of Ketamine and Midazolam are effective in pediatric convulsive Stage 1 Plus SE. The results show that earlier Ketamine administration (especially within 12 h of SE onset) was significantly associated with improved seizure control, with a more favorable safety profile than Midazolam in refractory SE. Notably, a dosage of less than 0.9 mg/kg/h proves ineffective in terminating SE. Ketamine has the advantage of preventing intubation, possibly shortening the length of stay in the intensive care unit.

摘要

癫痫持续状态(SE)是一种神经急症。目前的证据表明应采取逐步治疗方法,一线治疗包括使用苯二氮䓬类药物(BDZs)。在许多情况下,目前批准的治疗方法无法终止对BDZ耐药的SE。这种情况发生在1加阶段,这是作者设计的一个框架,用于在治疗开始前识别可能对苯二氮䓬类药物耐药的癫痫持续状态病例。这些病例包括长时间SE(持续时间>10分钟)、无明显运动现象以及急性病因(尤其是原发性中枢神经系统病因)。对BDZ难治的SE病例(1加阶段)可能需要不同的方法,一种针对由NMDA/AMPA受体介导的无反应性GABA信号状态,例如从一开始就联合使用氯胺酮进行多药治疗。这些考虑源于受体转运假说:在长时间癫痫发作活动和原发性中枢神经系统病因中,GABA受体会内化并远离突触,因此,SE对BDZ产生耐药性。一种可能恢复SE对BDZ无反应性的合理多药治疗应包括NMDA拮抗剂,如氯胺酮。氯胺酮在许多癫痫持续状态的实验模型中已被证明有效,并且越来越多的证据支持其在人类中的使用,尤其是在难治性和超难治性SE中。我们缺乏评估SE联合多药治疗的研究,尤其是在早期阶段。作者在此建议,氯胺酮应在属于1加阶段的早期SE阶段与一线BDZ一起使用,并在难治性SE中作为一线麻醉输注药物,尤其是在从1加阶段进展而来的病例中,最终在后期添加持续的咪达唑仑/丙泊酚输注。本系统评价的目的是总结目前关于早期联合使用包括氯胺酮在内的多药治疗的现有证据,以及氯胺酮在早期、已确诊和难治性SE中使用的现有证据。纳入了9项研究。氯胺酮和咪达唑仑推注对小儿惊厥性1加阶段SE有效。结果表明,早期给予氯胺酮(尤其是在SE发作后12小时内)与更好的癫痫控制显著相关,在难治性SE中其安全性比咪达唑仑更有利。值得注意的是,剂量低于0.9mg/kg/h在终止SE方面被证明无效。氯胺酮具有防止插管的优势,可能会缩短在重症监护病房的住院时间。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0602/12195624/308bd25725a0/neurolint-17-00083-g001.jpg

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