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KRM-II-81抑制了一名药物难治性癫痫患者皮质组织神经网络中的癫痫样活动。

KRM-II-81 suppresses epileptifom activity across the neural network of cortical tissue from a patient with pharmacoresistant epilepsy.

作者信息

Smith Jodi L, Wertz Jeremy, Lippa Arnold, Ping Xingjie, Jin Xiaoming, Cook James M, Witkin Jeffrey M, Cerne Rok

机构信息

Laboratory of Antiepileptic Drug Discovery, Ascension St. Vincent, Indianapolis, IN, USA.

Specialty Care, Indianapolis, IN, USA.

出版信息

Heliyon. 2023 Dec 16;10(1):e23752. doi: 10.1016/j.heliyon.2023.e23752. eCollection 2024 Jan 15.

Abstract

A clinical case of a 19-year-old male patient with pharmacoresistant seizures occurring following parieto-occipital tumor-resection at age 6 is described. Seizure surgery work-up included prolonged video EEG monitoring and head CT without contrast. Seizure focus was localized to the left temporal lobe, and we felt that the patient was an excellent candidate for seizure surgery. The patient underwent a left frontotemporal craniotomy for removal of the seizure focus with intraoperative electrocorticography (ECoG) conducted pre and post resection. ECoG recordings pre- and post-resection confirmed resolution of seizure generation. Imaging obtained immediately postoperatively showed complete resection of the residual tumor with no evidence of recurrence in follow-ups. A year after the surgery the patient is seizure-free but remains on seizure medication. With the patient's consent the excised epileptogenic tissue was used for research studies. The microelectrode recordings confirmed epileptiform activity in the excised tissue incubated in excitatory artificial cerebrospinal fluid. The epileptiform activity in the epileptogenic tissue was suppressed by addition of KRM-II-81, a novel α2/3 subtype preferring GABA receptor (GABAAR) potentiator with previously demonstrated antiepileptic efficacy in multiple animal models of epilepsy and with reduced potential for CNS side-effects compared to classical benzodiazepine GABAAR potentiators. These findings support the proposition that KRM-II-81 might reduce seizure burden in pharmacoresistant patients.

摘要

本文描述了一例临床病例,患者为19岁男性,6岁时因顶枕部肿瘤切除术后出现药物难治性癫痫。癫痫手术评估包括长时间视频脑电图监测和头颅平扫CT。癫痫病灶定位于左侧颞叶,我们认为该患者是癫痫手术的理想候选者。患者接受了左额颞开颅手术,以切除癫痫病灶,并在切除前后进行术中皮质脑电图(ECoG)监测。切除前后的ECoG记录证实癫痫发作源已消除。术后立即进行的影像学检查显示残留肿瘤已完全切除,随访中无复发迹象。术后一年,患者无癫痫发作,但仍在服用抗癫痫药物。在患者同意下,切除的致痫组织被用于研究。微电极记录证实,在兴奋性人工脑脊液中孵育的切除组织中存在癫痫样活动。通过添加KRM-II-81可抑制致痫组织中的癫痫样活动,KRM-II-81是一种新型的α2/3亚型选择性GABA受体(GABAAR)增强剂,在多种癫痫动物模型中已证明具有抗癫痫疗效,与经典苯二氮䓬类GABAAR增强剂相比,其产生中枢神经系统副作用的可能性降低。这些发现支持了KRM-II-81可能减轻药物难治性患者癫痫负担的观点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4dd0/10784158/14873231cd73/gr1.jpg

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