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亨廷顿病患者侧脑室下区脂质组学结构缺失。

Subventricular zone lipidomic architecture loss in Huntington's disease.

机构信息

Department of Pharmacology and Clinical Pharmacology, University of Auckland, Auckland, New Zealand.

Centre for Brain Research, University of Auckland, Auckland, New Zealand.

出版信息

J Neurochem. 2018 Sep;146(5):613-630. doi: 10.1111/jnc.14468. Epub 2018 Aug 8.

DOI:10.1111/jnc.14468
PMID:29804301
Abstract

The human subventricular zone (SVZ) has a defined cytological and neurochemical architecture, with four constituent laminae that act in concert to support its neurogenic activity. Lipidomic specialisation has previously been demonstrated in the neurologically normal human SVZ, with enrichment of functionally important lipid classes in each lamina. The SVZ is also responsive to neurodegenerative disorders, where thickening of the niche and enhanced proliferation of resident cells were observed in Huntington's disease (HD) brains. In this study, we hypothesised lipidomic changes in the HD SVZ. Using matrix-assisted laser desorption/ionisation (MALDI) imaging mass spectrometry, this analysis shows differences in the lipidomic architecture in the post-mortem Vonsattel grade III cases. Relative to matched, neurologically normal specimens (N = 4), the lipidomic signature of the HD SVZ (N = 4) was characterized by loss of sulfatides and triglycerides in the myelin layer, with an ectopic and focal accumulation of sphingomyelins and ceramide-1-phosphate observed in this lamina. A striking loss of lipidomic patterning was also observed in the ependymal layer, where the local abundance of phosphatidylinositols was significantly reduced in HD. This comprehensive spatially resolved lipidomic analysis of the human HD SVZ identifies alterations in lipid architecture that may shed light on the mechanisms of SVZ responses to neurodegeneration in HD. Open Science: This manuscript was awarded with the Open Materials Badge. For more information see: https://cos.io/our-services/open-science-badges/.

摘要

人类侧脑室下区 (SVZ) 具有明确的细胞学和神经化学结构,由四个组成层协同作用,支持其神经发生活性。此前已在神经正常的人类 SVZ 中证明了脂质组学的特化,每个层中都富含功能重要的脂质类。SVZ 还对神经退行性疾病有反应,在亨廷顿病 (HD) 大脑中观察到龛位增厚和常驻细胞增殖增强。在这项研究中,我们假设 HD SVZ 的脂质组学发生了变化。使用基质辅助激光解吸/电离 (MALDI) 成像质谱法,该分析显示了 Vonsattel 分级 III 例死后 SVZ 的脂质组学结构的差异。与匹配的神经正常标本 (N=4) 相比,HD SVZ (N=4) 的脂质组学特征表现为髓鞘层中硫酸脑苷脂和甘油三酯的丢失,在该层中观察到鞘磷脂和神经酰胺-1-磷酸的异位和局灶性积累。在室管膜层也观察到脂质组学模式的明显丢失,其中 HD 中局部磷酸肌醇的丰度显著降低。对人类 HD SVZ 的全面空间分辨脂质组学分析确定了脂质结构的改变,这可能有助于了解 SVZ 对 HD 神经退行性变的反应机制。开放科学:本文获得了开放材料徽章。有关更多信息,请参见:https://cos.io/our-services/open-science-badges/。

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