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结节性硬化症的致痫性:一项立体脑电图研究。

Epileptogenicity in tuberous sclerosis complex: A stereoelectroencephalographic study.

机构信息

National Institute of Health and Medical Research U1028/National Center for Scientific Research, Mixed Unit of Research 5292, Lyon Neuroscience Research Center, Lyon, France.

Department of Functional Neurology and Epileptology, Member of the ERN EpiCARE Lyon University Hospital and Lyon 1 University, Lyon, France.

出版信息

Epilepsia. 2020 Jan;61(1):81-95. doi: 10.1111/epi.16410. Epub 2019 Dec 20.

Abstract

OBJECTIVE

In tuberous sclerosis complex (TSC)-associated drug-resistant epilepsy, the optimal invasive electroencephalographic (EEG) and operative approach remains unclear. We examined the role of stereo-EEG in TSC and used stereo-EEG data to investigate tuber and surrounding cortex epileptogenicity.

METHODS

We analyzed 18 patients with TSC who underwent stereo-EEG (seven adults). One hundred ten seizures were analyzed with the epileptogenicity index (EI). In 13 patients with adequate tuber sampling, five anatomical regions of interest (ROIs) were defined: dominant tuber (tuber with highest median EI), perituber cortex, secondary tuber (tuber with second highest median EI), nearby cortex (normal-appearing cortex in the same lobe as dominant tuber), and distant cortex (in other lobes). At the seizure level, epileptogenicity of ROIs was examined by comparing the highest EI recorded within each anatomical region. At the patient level, epileptogenic zone (EZ) organization was separated into focal tuber (EZ confined to dominant tuber) and complex (all other patterns).

RESULTS

The most epileptogenic ROI was the dominant tuber, with higher EI than perituber cortex, secondary tuber, nearby cortex, and distant cortex (P < .001). A focal tuber EZ organization was identified in seven patients. This group had 80% Engel IA postsurgical outcome and distinct dominant tuber characteristics: continuous interictal discharges (IEDs; 100%), fluid-attenuated inversion recovery (FLAIR) hypointense center (86%), center-to-rim EI gradient, and stimulation-induced seizures (71%). In contrast, six patients had a complex EZ organization, characterized by nearby cortex as the most epileptogenic region and 40% Engel IA outcome. At the intratuber level, the combination of FLAIR hypointense center, continuous IEDs, and stimulation-induced seizures offered 98% specificity for a focal tuber EZ organization.

SIGNIFICANCE

Tubers with focal EZ organization have a striking similarity to type II focal cortical dysplasia. The presence of distinct EZ organizations has significant implications for EZ hypothesis generation, invasive EEG approach, and resection strategy.

摘要

目的

在结节性硬化症(TSC)相关药物难治性癫痫中,最佳的侵入性脑电图(EEG)和手术方法仍不清楚。我们研究了立体 EEG 在 TSC 中的作用,并使用立体 EEG 数据来研究结节及其周围皮层的致痫性。

方法

我们分析了 18 例接受立体 EEG 检查的 TSC 患者(7 例成人)。用致痫性指数(EI)分析了 110 次发作。在 13 例有足够结节样本的患者中,定义了五个感兴趣的解剖区域(ROI):优势结节(EI 中位数最高的结节)、结节周围皮质、次要结节(EI 中位数第二高的结节)、附近皮质(优势结节同侧同叶的正常外观皮质)和远隔皮质(其他叶的皮质)。在发作水平上,通过比较每个解剖区域内记录的最高 EI 来检查 ROI 的致痫性。在患者水平上,将致痫区(EZ)组织分为局限性结节(EZ 局限于优势结节)和复杂性(所有其他类型)。

结果

最具致痫性的 ROI 是优势结节,其 EI 高于结节周围皮质、次要结节、附近皮质和远隔皮质(P<0.001)。7 例患者存在局限性结节 EZ 组织,术后 80%的患者达到 Engel ⅠA级,且具有明显的优势结节特征:连续的发作间期放电(IED;100%)、液体衰减反转恢复(FLAIR)低信号中心(86%)、中心到边缘 EI 梯度和刺激诱导的发作(71%)。相比之下,6 例患者存在复杂性 EZ 组织,其特征为附近皮质为最具致痫性的区域,且术后 40%的患者达到 Engel ⅠA级。在结节内水平,FLAIR 低信号中心、连续 IED 和刺激诱导发作的组合对局限性结节 EZ 组织具有 98%的特异性。

意义

具有局限性 EZ 组织的结节与 II 型局灶性皮质发育不良具有惊人的相似性。明确的 EZ 组织具有重要的意义,可以为 EZ 假说的产生、侵入性 EEG 方法和切除术策略提供依据。

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