A high seizure burden increases brain concentrations of specialized pro-resolving mediators in the Scn1a+/- mouse model of Dravet syndrome

IF 2.5 3区生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY

Prostaglandins & other lipid mediators Pub Date : 2025-01-01 DOI:10.1016/j.prostaglandins.2024.106943

Ka Lai Yip , Cilla Zhou , Lyndsey L. Anderson , Nicole A. Hawkins , Jennifer A. Kearney , Jonathon C. Arnold

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引用次数: 0

Abstract

Objective

Dravet syndrome is a severe, intractable epilepsy in which 80 % of patients have a de novo mutation in the gene SCN1A. We recently reported that a high seizure burden increased hippocampal concentrations of an array of pro-inflammatory prostaglandins in the Scn1a^+/- mouse model of Dravet syndrome. This raised the possibility that a high seizure burden might also trigger the accumulation of specialized pro-resolving mediators that facilitate the resolution of neuroinflammation and brain repair. The present study therefore aimed to examine whether a high seizure burden increased hippocampal concentrations of various specialized pro-resolving mediators in the Scn1a^+/- mouse model of Dravet syndrome.

Methods

Scn1a^+/- mice at postnatal day 21 (P21) were primed with a single hyperthermia-induced seizure event to induce a high seizure burden. On P24 primed Scn1a^+/- mice with a high seizure burden, unprimed naïve Scn1a^+/- mice and wild-type (WT) mice were euthanized and hippocampal tissue was collected for analysis of various specialized pro-resolving mediators using liquid chromatography mass spectrometry.

Results

Scn1a^+/- mice with a high seizure burden showed increased hippocampal concentrations of the pro-inflammatory leukotrienes B4 and E4. Further, a high seizure burden increased hippocampal concentrations of various special pro-resolving mediators, including the maresins (maresin1), D-series resolvins (RVD1 and RVD4), and protectin (PCTR1). To further characterize these changes, we determined the mRNA expression of lipoxygenase genes, as these synthetic enzymes are common across classes of specialized pro-resolving mediators. However, hippocampal expression of Alox5, Alox12 and Alox15 were not influenced by a high seizure burden.

Significance

We report for the first time that a high seizure burden increases the hippocampal concentrations of various specialized pro-resolving mediators in Scn1a^+/- mice. This provides a platform for future studies to examine whether modulation of these mediators might be exploited to reduce seizures and facilitate brain repair in intractable epilepsy syndromes.

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在Dravet综合征的Scn1a+/-小鼠模型中，高癫痫发作负担增加了专门的促溶解介质的脑浓度。

目的：Dravet综合征是一种严重的顽固性癫痫，其中80%的患者有SCN1A基因的新生突变。我们最近报道，在Dravet综合征的Scn1a+/-小鼠模型中，高癫痫发作负担增加了一系列促炎前列腺素的海马浓度。这提出了一种可能性，即高癫痫发作负担也可能触发专门的促溶解介质的积累，促进神经炎症和大脑修复的解决。因此，本研究旨在研究高癫痫发作负担是否会增加Dravet综合征Scn1a+/-小鼠模型中各种特殊促溶解介质的海马浓度。方法：Scn1a+/-小鼠在出生后第21天（P21）用单一的高温诱发癫痫事件启动，以诱导高癫痫发作负担。对P24引物的高癫痫发作负担Scn1a+/-小鼠，对未引物naïve Scn1a+/-小鼠和野生型（WT）小鼠实施安乐死，收集海马组织，使用液相色谱-质谱法分析各种专门的促溶解介质。结果：高癫痫发作负荷的Scn1a+/-小鼠海马中促炎白三烯B4和E4浓度升高。此外，高癫痫负担增加了海马中各种特殊促溶解介质的浓度，包括maaresin （maresin1）、d系列溶解蛋白（RVD1和RVD4）和保护蛋白（PCTR1）。为了进一步表征这些变化，我们测定了脂氧合酶基因的mRNA表达，因为这些合成酶在各种特殊的促溶解介质中都很常见。然而，Alox5、Alox12和Alox15的海马表达不受高癫痫发作负担的影响。意义：我们首次报道了高癫痫发作负担增加了Scn1a+/-小鼠海马中各种特殊促溶解介质的浓度。这为未来的研究提供了一个平台，以检查这些介质的调节是否可能被利用来减少癫痫发作和促进顽固性癫痫综合征的大脑修复。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Prostaglandins & other lipid mediators 生物-生化与分子生物学

CiteScore

5.80

自引率

3.40%

发文量

审稿时长

2 months

期刊介绍： Prostaglandins & Other Lipid Mediators is the original and foremost journal dealing with prostaglandins and related lipid mediator substances. It includes basic and clinical studies related to the pharmacology, physiology, pathology and biochemistry of lipid mediators. Prostaglandins & Other Lipid Mediators invites reports of original research, mini-reviews, reviews, and methods articles in the basic and clinical aspects of all areas of lipid mediator research: cell biology, developmental biology, genetics, molecular biology, chemistry, biochemistry, physiology, pharmacology, endocrinology, biology, the medical sciences, and epidemiology. Prostaglandins & Other Lipid Mediators also accepts proposals for special issue topics. The Editors will make every effort to advise authors of the decision on the submitted manuscript within 3-4 weeks of receipt.