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采用串联质量标签对复发性癫痫发作犬的脑脊液进行定量蛋白质组学研究。

Quantitative proteomics of cerebrospinal fluid using tandem mass tags in dogs with recurrent epileptic seizures.

机构信息

Diagnostic Laboratory, Faculty of Veterinary Medicine, School of Health Sciences, Aristotle University of Thessaloniki, Thessaloniki, Greece.

Institute of Biodiversity, Animal Health & Comparative Medicine and School of Veterinary Medicine, College of Medicine, Veterinary Medicine and Life Sciences, University of Glasgow, Glasgow G61 1QH, UK.

出版信息

J Proteomics. 2021 Jan 16;231:103997. doi: 10.1016/j.jprot.2020.103997. Epub 2020 Oct 2.

Abstract

This prospective study included four dog groups (group A: healthy dogs, groups B: dogs with idiopathic epilepsy under antiepileptic medication (AEM), C: idiopathic epilepsy dogs without AEM administration, D: dogs with structural epilepsy). The purpose of the study was to compare the proteomic profile among the four groups. Samples were analyzed by a quantitative Tandem Mass Tags approach using a Q-Exactive-Plus mass-spectrometer. Identification and relative quantification were performed using Proteome Discoverer, and data were analyzed using R. Gene ontology terms were analyzed based on Canis lupus familiaris database. Data are available via ProteomeXchange with identifier PXD018893. Eighteen proteins were statistically significant among the four groups (P < 0.05). MMP2 and EFEMP2 appeared down-regulated whereas HP and APO-A1 were up-regulated (groups B, D). CLEC3B and PEBP4 were up-regulated whereas APO-A1 was down-regulated (group C). IGLL1 was down-regulated (groups B, C) and up-regulated (group D). EFEMP2 was the only protein detected among the four groups and PEBP4 was significantly different among the epileptic dogs. Western blot and SPARCL immunoassay were used to quantify HP abundance change, validating proteomic analysis. Both, showed good correlation with HP levels identified through proteomic analysis (r = 0.712 and r = 0.703, respectively). SIGNIFICANCE: The proteomic analysis from CSF of dogs with epileptic seizures could reflect that MMP2, HP and APO-A1 may contribute to a blood-brain barrier disruption through the seizure-induced inflammatory process in the brain. MMP2 change may indicate the activation of protective mechanisms within the brain tissue. Antiepileptic medication could influence several cellular responses and alter the CSF proteome composition.

摘要

本前瞻性研究纳入了四个犬类组别(A 组:健康犬;B 组:接受抗癫痫药物(AEM)治疗的特发性癫痫犬;C 组:未接受 AEM 治疗的特发性癫痫犬;D 组:结构性癫痫犬)。研究目的是比较这四组的蛋白质组图谱。使用 Q-Exactive-Plus 质谱仪通过定量串联质量标签方法分析样本。使用 Proteome Discoverer 进行鉴定和相对定量,使用 R 进行数据分析。基于犬数据库分析基因本体术语。数据可通过 ProteomeXchange 以标识符 PXD018893 获取。四个组之间有 18 种蛋白质具有统计学意义(P < 0.05)。MMP2 和 EFEMP2 下调,而 HP 和 APO-A1 上调(B、D 组)。CLEC3B 和 PEBP4 上调,而 APO-A1 下调(C 组)。IGLL1 下调(B、C 组)和上调(D 组)。EFEMP2 是四个组中唯一检测到的蛋白质,PEBP4 在癫痫犬中差异显著。Western blot 和 SPARCL 免疫测定用于定量 HP 丰度变化,验证蛋白质组分析。Western blot 和 SPARCL 免疫测定均与通过蛋白质组分析鉴定的 HP 水平具有良好相关性(r = 0.712 和 r = 0.703)。意义:癫痫发作犬脑脊液的蛋白质组分析可能反映 MMP2、HP 和 APO-A1 可能通过大脑中癫痫诱导的炎症过程导致血脑屏障破坏。MMP2 变化可能表明脑组织内的保护机制被激活。抗癫痫药物可能影响多种细胞反应并改变 CSF 蛋白质组组成。

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