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High-Throughput LC–MS/MS Proteomic Analysis of a Mouse Model of Mesiotemporal Lobe Epilepsy Predicts Microglial Activation Underlying Disease Development

癫痫发生 癫痫持续状态 神经退行性变 红藻氨酸 星形胶质细胞 癫痫 串联质谱法 神经科学 蛋白质组学 化学 生物 病理 医学 疾病 中枢神经系统 生物化学 质谱法 谷氨酸受体 受体 色谱法 基因
作者
Vasiliki Bitsika,Venceslas Duveau,Julia Simon‐Areces,William Mullen,Corinne Roucard,Manousos Makridakis,George Mermelekas,Pantelis Savvopoulos,Antoine Depaulis,Antonia Vlahou
出处
期刊:Journal of Proteome Research [American Chemical Society]
卷期号:15 (5): 1546-1562 被引量:39
标识
DOI:10.1021/acs.jproteome.6b00003
摘要

Uncovering the molecular mechanisms of mesiotemporal lobe epilepsy (MTLE) is critical to identify therapeutic targets. In this study, we performed global protein expression analysis of a kainic acid (KA) MTLE mouse model at various time-points (1, 3, and 30 days post-KA injection -dpi), representing specific stages of the syndrome. High-resolution liquid chromatography coupled to tandem mass spectrometry (LC-MS/MS), in combination with label-free protein quantification using three processing approaches for quantification, was applied. Following comparison of KA versus NaCl-injected mice, 22, 53, and 175 proteins were differentially (statistically significant) expressed at 1, 3 and 30dpi, respectively, according to all three quantification approaches. Selected findings were confirmed by multiple reaction monitoring LC-MS/MS. As a positive control, the astrocyte marker GFAP was found to be upregulated (3dpi: 1.9 fold; 30dpi: 12.5 fold), also verified by IHC. The results collectively suggest that impairment in synaptic transmission occurs even right after initial status epilepticus (1dpi), with neurodegeneration becoming more extensive during epileptogenesis (3dpi) and sustained at the chronic phase (30dpi), where also extensive glial- and astrocyte-mediated inflammation is evident. This molecular profile is in line with observed phenotypic changes in human MTLE, providing the basis for future studies on new molecular targets for the disease.
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