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Imaging mass spectrometry of frontal white matter lipid changes in human alcoholics

机译:人酗酒中额外白质脂质变化的成像质谱

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BackgroundChronic alcohol use disorders (AUD) are associated with white matter (WM) degeneration with altered myelin integrity. Matrix assisted laser desorption ionization-imaging mass spectrometry (MALDI-IMS) enables high throughput analysis of myelin lipid biochemical histopathology to help characterize disease mechanisms. PurposeThis study utilized MALDI-IMS to investigate?frontal lobe WM myelin lipid abnormalities in AUD. MethodsStandardized cores of formalin-fixed WM from Brodmann Area 4 (BA4) and BA8/9 of 20 postmortem AUD and 19 control adult human brains were embedded in carboxymethyl-cellulose, cryo-sectioned (8?μm), thaw-mounted onto indium tin oxide (ITO) -coated glass slides, and sublimed with 2,5-dihydroxybenzxoic acid (DHB) matrix. Lipids were imaged by MALDI-time of flight in the negative ionization mode. Data were visualized with FlexImaging software v4.0 and analyzed with ClinProTools v3.0. ResultsPrincipal component analysis (PCA) and data bar plots of MALDI-IMS data differentiated AUD from control WM. The dominant effect of AUD was to broadly reduce expression of sphingolipids (sulfatides and ceramides) and phospholipids. Data bar plots demonstrated overall similar responses to AUD in BA4 and BA8/9. However, differential regional effects of AUD on WM lipid profiles were manifested by non-overlapping expression or discordant responses to AUD for a subset of lipid ions. ConclusionsHuman AUD is associated with substantial inhibition of frontal lobe WM lipid expression with regional variability in these effects. MALDI-IMS can be used to characterize the nature of AUD-associated lipid biochemical abnormalities for correlation with lifetime exposures and WM degeneration, altered gene expression, and responses to abstinence or treatment.
机译:BackgroundChronic酒精使用障碍(AUD)与白质(WM)变性相关,具有改变的髓鞘完整性。基质辅助激光解吸电离成像质谱(MALDI-IMS)能够实现髓鞘脂质生化组织病理学的高通量分析,以帮助表征疾病机制。目的研究利用MALDI-IM进行探讨?甲型中的前叶WM骨髓脂质异常。 Metable50甲醛4(BA4)和Ba8 / 9的福尔马林固定WM的标准化核心嵌入了羧甲基 - 纤维素,冷冻切片(8Ωμm),解冻到铟锡上氧化物(ITO) - 涂层玻璃载玻片,并用2,5-二羟基苯并酸(DHB)基质升华。通过在负电离模式中的飞行飞行时间进行脂质。使用Fleximaging Software V4.0可视化数据,并使用ClinProtools V3.0进行分析。 MARDI-IMS数据分化来自控制WM的结果丙烯分量分析(PCA)和数据条图。 AUD的显着效果是大致减少鞘脂(硫酸酯和神经酰胺)和磷脂的表达。数据条图显示了对BA4和BA8 / 9中的AUD的总体相似的响应。然而,通过非重叠表达或对脂质离子的副本的非重叠表达或不和谐的反应表现出对WM脂质曲线的差异区域效应。结论Human AUD与额叶WM脂质表达的大量抑制相关,具有这些效果的区域变异性。 Maldi-IMS可用于表征患有患病性脂质化学异常的性质与寿命暴露和WM变性,改变的基因表达,以及对禁欲或治疗的反应的相关性。

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