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联合富集人黑质致密部组织中的神经黑色素颗粒和突触体用于蛋白质组学分析。

Combined enrichment of neuromelanin granules and synaptosomes from human substantia nigra pars compacta tissue for proteomic analysis.

机构信息

Department of Functional Proteomics, Medizinisches Proteom-Center, Ruhr-Universität Bochum, Bochum, Germany.

Department of Cytology, Institute of Anatomy, Ruhr-Universität Bochum, Bochum, Germany.

出版信息

J Proteomics. 2013 Dec 6;94:202-206. doi: 10.1016/j.jprot.2013.07.015. Epub 2013 Aug 3.

Abstract

UNLABELLED

This article gives a detailed description of a protocol using density gradient centrifugation for the enrichment of neuromelanin granules and synaptosomes from low amounts (≥0.15g) of human substantia nigra pars compacta tissue. This has a great advantage compared to already existing methods as it allows for the first time (i) a combined enrichment of neuromelanin granules and synaptosomes and (ii) just minimal amounts of tissue necessary to enable donor specific analysis. Individual specimens were classified as control or diseased according to clinical evaluation and neuropathological examination. For the enrichment of synaptosomes and neuromelanin granules from the same tissue sample density gradient centrifugations using Percoll® and Iodixanol were performed. The purity of resulting fractions was checked by transmission electron microscopy. We were able to establish a reproducible and easy to handle protocol combining two different density gradient centrifugations: using an Iodixanol gradient neuromelanin granules were enriched and in parallel, from the same sample, a fraction of synaptosomes with high purity using a Percoll® gradient was obtained. Our subfractionation strategy will enable a subsequent in depth proteomic characterization of neurodegenerative processes in the substantia nigra pars compacta in patients with Parkinson's disease and dementia with Lewy bodies compared to appropriate controls.

BIOLOGICAL SIGNIFICANCE

Key features of Parkinson's disease are the degeneration of dopaminergic neurons in the substantia nigra pars compacta, an associated loss of the brain pigment neuromelanin and a resulting impairment of the neuronal network. The accumulation of iron binding neuromelanin granules is age- and disease-dependent and disease specific alterations could affect the neuronal iron homeostasis leading to oxidative stress induced cell death. The focus of the described method is the analysis of neuromelanin granules as well as axonal cell-endings of nerve cells (synaptosomes) of individual donors (control and diseased). It is the basis for the identification of disease-relevant changes in the iron homeostasis and the generation of new insight into altered protein compositions or regulations which might lead to disturbed communications between nerve cells resulting in pathogenic processes.

摘要

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本文详细描述了一种使用密度梯度离心从低量(≥0.15g)人黑质致密部组织中富集神经黑色素颗粒和突触体的方案。与现有的方法相比,这具有很大的优势,因为它首次允许(i)同时富集神经黑色素颗粒和突触体,以及(ii)仅需要最少的组织量就可以进行供体特异性分析。根据临床评估和神经病理学检查,将个体标本分类为对照或患病。为了从同一组织样品中富集突触体和神经黑色素颗粒,进行了使用 Percoll®和碘克沙醇的密度梯度离心。通过透射电子显微镜检查了所得级分的纯度。我们成功建立了一种可重复且易于处理的方案,该方案结合了两种不同的密度梯度离心:使用碘克沙醇梯度,神经黑色素颗粒被富集,同时,从同一样品中,使用 Percoll®梯度获得了具有高纯度的突触体级分。我们的亚分级策略将使我们能够对帕金森病和路易体痴呆患者黑质致密部中的神经退行性过程进行深入的蛋白质组学特征分析,与适当的对照相比。

生物学意义

帕金森病的主要特征是黑质致密部多巴胺能神经元的退化,与脑色素神经黑色素的丢失以及由此导致的神经元网络功能障碍相关。铁结合神经黑色素颗粒的积累与年龄和疾病有关,并且疾病特异性改变可能会影响神经元铁稳态,导致氧化应激诱导的细胞死亡。所描述方法的重点是分析个体供体(对照和患病)的神经黑色素颗粒以及轴突细胞末端(突触体)。这是鉴定铁稳态中与疾病相关的变化以及产生新的见解的基础,这些变化可能导致神经元之间的通讯中断,从而导致致病过程。

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