癫痫发作后全面性脑电图抑制持续时间与海马和颞叶皮质 5-羟色胺受体表达的关系
Serotonin receptor expression in hippocampus and temporal cortex of temporal lobe epilepsy patients by postictal generalized electroencephalographic suppression duration.
机构信息
Comprehensive Epilepsy Center, New York University Grossman School of Medicine, New York, New York, USA.
Center for Cognitive Neurology, New York University Grossman School of Medicine, New York, New York, USA.
出版信息
Epilepsia. 2022 Nov;63(11):2925-2936. doi: 10.1111/epi.17400. Epub 2022 Sep 5.
OBJECTIVE
Prolonged postictal generalized electroencephalographic suppression (PGES) is a potential biomarker for sudden unexpected death in epilepsy (SUDEP), which may be associated with dysfunctional autonomic responses and serotonin signaling. To better understand molecular mechanisms, PGES duration was correlated to 5HT1A and 5HT2A receptor protein expression and RNAseq from resected hippocampus and temporal cortex of temporal lobe epilepsy patients with seizures recorded in preoperative evaluation.
METHODS
Analyses included 36 cases (age = 14-64 years, age at epilepsy onset = 0-51 years, epilepsy duration = 2-53 years, PGES duration = 0-93 s), with 13 cases in all hippocampal analyses. 5HT1A and 5HT2A protein was evaluated by Western blot and histologically in hippocampus (n = 16) and temporal cortex (n = 9). We correlated PGES duration to our previous RNAseq dataset for serotonin receptor expression and signaling pathways, as well as weighted gene correlation network analysis (WGCNA) to identify correlated gene clusters.
RESULTS
In hippocampus, 5HT2A protein by Western blot positively correlated with PGES duration (p = .0024, R = .52), but 5HT1A did not (p = .87, R = .0020). In temporal cortex, 5HT1A and 5HT2A had lower expression and did not correlate with PGES duration. Histologically, PGES duration did not correlate with 5HT1A or 5HT2A expression in hippocampal CA4, dentate gyrus, or temporal cortex. RNAseq identified two serotonin receptors with expression that correlated with PGES duration in an exploratory analysis: HTR3B negatively correlated (p = .043, R = .26) and HTR4 positively correlated (p = .049, R = .25). WGCNA identified four modules correlated with PGES duration, including positive correlation with synaptic transcripts (p = .040, Pearson correlation r = .52), particularly potassium channels (KCNA4, KCNC4, KCNH1, KCNIP4, KCNJ3, KCNJ6, KCNK1). No modules were associated with serotonin receptor signaling.
SIGNIFICANCE
Higher hippocampal 5HT2A receptor protein and potassium channel transcripts may reflect underlying mechanisms contributing to or resulting from prolonged PGES. Future studies with larger cohorts should assess functional analyses and additional brain regions to elucidate mechanisms underlying PGES and SUDEP risk.
目的
发作后广泛脑电图抑制时间延长(PGES)是癫痫猝死(SUDEP)的潜在生物标志物,可能与自主神经反应和 5-羟色胺信号功能障碍有关。为了更好地理解分子机制,我们将 PGES 持续时间与术前评估中记录癫痫发作的颞叶癫痫患者切除海马和颞叶中的 5HT1A 和 5HT2A 受体蛋白表达和 RNAseq 进行了相关性分析。
方法
分析包括 36 例病例(年龄 14-64 岁,癫痫发病年龄 0-51 岁,癫痫持续时间 2-53 年,PGES 持续时间 0-93 秒),其中 13 例均进行海马分析。通过 Western blot 和组织学评估海马(n=16)和颞叶皮层(n=9)中的 5HT1A 和 5HT2A 蛋白。我们将 PGES 持续时间与我们之前的 5-羟色胺受体表达和信号通路 RNAseq 数据集进行了相关性分析,以及加权基因相关网络分析(WGCNA)以识别相关基因簇。
结果
在海马中,Western blot 检测到的 5HT2A 蛋白与 PGES 持续时间呈正相关(p=0.0024,R=0.52),但 5HT1A 无相关性(p=0.87,R=0.0020)。在颞叶皮层中,5HT1A 和 5HT2A 的表达水平较低,与 PGES 持续时间无相关性。组织学分析表明,PGES 持续时间与海马 CA4、齿状回和颞叶皮层中 5HT1A 或 5HT2A 的表达均无相关性。RNAseq 鉴定出两种与 PGES 持续时间相关的 5-羟色胺受体:HTR3B 呈负相关(p=0.043,R=0.26),HTR4 呈正相关(p=0.049,R=0.25)。WGCNA 鉴定出四个与 PGES 持续时间相关的模块,包括与突触转录物的正相关(p=0.040,Pearson 相关 r=0.52),特别是钾通道(KCNA4、KCNC4、KCNH1、KCNIP4、KCNJ3、KCNJ6、KCNK1)。没有模块与 5-羟色胺受体信号相关。
意义
海马中较高的 5HT2A 受体蛋白和钾通道转录物可能反映了导致或导致 PGES 时间延长的潜在机制。未来应该对更大的队列进行评估,以评估功能分析和额外的脑区,以阐明 PGES 和 SUDEP 风险的潜在机制。
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