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Human cerebrospinal fluid apolipoprotein E isoforms are apparently inefficient at complexing with synthetic Alzheimers amyloid-beta peptide (Abeta 1-40 ) in vitro.

机译：人脑脊髓液载脂蛋白E同工型在体外与合成的阿尔茨海默氏淀粉样蛋白-β肽（Aβ1-40）复合时明显无效。

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BACKGROUND: Variation at the apolipoprotein E locus on chromosome 19 plays a role in more cases of Alzheimer's disease than does any other identified genetic determinant. We have previously reported the isoform-specific interaction of native human apolipoprotein E (APOE, gene; apoE, protein) epsilon 3 with the amyloid-ss peptide, Ass(1-40), the major component of the cerebral amyloid deposits that appear to cause Alzheimer's disease. MATERIALS AND METHODS: In order to investigate the apoE: A beta interaction further, a modified assay was developed based on co-immunoprecipitation of the complex using an anti-apoE antibody (anti-apoE IP assay). RESULTS: Application of this assay demonstrated that the interaction of Ass(1-40) and apoE can be distinguished into two types: sodium dodecyl sulfate (SDS) -resistant and SDS-releasable. The SDS-resistant interaction between epsilon;3 and Ass(1-40) is apparently maximal at an Ass(1-40) concentration of approximately 75 micro M, and an Ass(1-40) /epsilon 3 molar ratio of about 250:1. The major apoE-isoform-specific difference in interaction with Ass(1-40) is the ability of Ass(1-40) to form SDS- resistant complexes with epsilon 3 but not with epsilon 4. Using the anti-apoE co-IP assay, we found that human cerebrospinal fluid (CSF) epsilon 3 can also form an SDS-resistant complex with Ass(1-40) but human CSF epsilon;4 cannot. However, when compared with apoE epsilon;3 collected from the conditioned medium of APOE epsilon 3-transfected cells, the competence of equal concentrations of CSF apoE epsilon 3 to form SDS-resistant complexes with Ass(1-40) is apparently diminished. A 1:1 mixture of CSF plus apoE epsilon 3-containing conditioned medium is associated with diminished Ass(1-40) /epsilon;3 complex formation to a greater extent than that observed when an identical volume of phosphate-buffered saline is added to apoE epsilon;3 medium. CONCLUSIONS: These results suggest the presence in CSF of factors that interfere with the formation of complexes between synthetic Ass(1-40) and apoE epsilon 3.

机译：背景：与其他已确定的遗传决定因素相比，第19号染色体上载脂蛋白E基因座的变异在阿尔茨海默氏病病例中的作用更大。我们以前曾报道过天然人类载脂蛋白E（APOE，基因; apoE，蛋白质）epsilon 3与淀粉样蛋白Ss肽Ass（1-40）的同工型特异性相互作用，这似乎是脑淀粉样蛋白沉积的主要成分。引起阿尔茨海默氏病。材料和方法：为了研究apoE：进一步进行β相互作用，基于复合物的共免疫沉淀，使用抗apoE抗体开发了一种改良的检测方法（anti-apoE IP检测）。结果：该检测方法的应用表明，Ass（1-40）和apoE的相互作用可分为两种类型：耐十二烷基硫酸钠（SDS）和可释放SDS。在大约75 micro M的Ass（1-40）浓度和大约250的Ass（1-40）/ epsilon 3摩尔比下，ε3和Ass（1-40）之间的SDS抗性相互作用最大：1。与Ass（1-40）相互作用的主要apoE异构体特异性差异是Ass（1-40）与epsilon 3而不与epsilon 4形成SDS抗性复合物的能力。使用anti-apoE co-IP分析，我们发现人脑脊液（CSF）epsilon 3也可以与Ass（1-40）形成SDS耐药复合物，而人CSF epsilon; 4不能。但是，与从APOEε3转染的细胞的条件培养基中收集的apoEε3相比，等浓度的CSF apoEε3与Ass（1-40）形成SDS抗性复合物的能力明显降低。 1：1的CSF加含apoE epsilon 3的条件培养基的混合物与减少的Ass（1-40）/ epsilon; 3络合物形成相关，其程度大于在相同体积的磷酸盐缓冲盐水中添加的量。 apoE epsilon; 3培养基。结论：这些结果表明在脑脊液中存在干扰合成Ass（1-40）与载脂蛋白E epsilon 3之间复合物形成的因素。

著录项

期刊名称 Molecular Medicine
作者
Zhongmin Zhou; Norman Relkin; Jorge Ghiso; Jonathan D. Smith; Sam Gandy;
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年(卷),期 2002(8),7
年度 2002
页码 376–381
总页数 6
原文格式 PDF
正文语种
中图分类分子生物学;细胞生物学;医学史;
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专利

1. Human cerebrospinal fluid apolipoprotein E isoforms are apparently inefficient at complexing with synthetic Alzheimer's amyloid-(beta) peptide (A(beta) 1-40 ) in vitro. [J] . Zhou Z, Relkin N, Ghiso J, Molecular medicine. . 2002,第7期

机译：人脑脊液载脂蛋白E同工型在体外与合成的阿尔茨海默氏淀粉样蛋白-β肽（Aβ1-40）复合时效率低下。
2. Amyloid-beta peptide(1-40) elimination from cerebrospinal fluid involves low-density lipoprotein receptor-related protein 1 at the blood-cerebrospinal fluid barrier. [J] . Fujiyoshi M, Tachikawa M, Ohtsuki S, Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry . 2011,第3a4期

机译：从脑脊液中消除淀粉样蛋白β肽（1-40）涉及血脑脊液屏障处的低密度脂蛋白受体相关蛋白1。
3. Isoform-specific interactions of human apolipoprotein E to an intermediate conformation of human Alzheimer amyloid-beta peptide [J] . Stratman NC, Castle CK, Taylor BM, Chemistry and Physics of Lipids . 2005,第1a2期

机译：人类载脂蛋白E与人阿尔茨海默氏淀粉样β肽的中间构象的同工型特异性相互作用
4. Absolute and Relative Quantitation of Apolipoprotein E Isoform Levels in Human Cerebrospinal Fluid and Brain [C] . Alaina Baker-Nigh, Kwasi G. Mawuenyega, Vitaliy Ovod, ASMS Conference on Mass Spectrometry and Allied Topics . 2015

机译：人脑脊液中载脂蛋白E同种型水平的绝对和相对定量
5. Specific amyloid-beta oligomers in human cerebrospinal fluid. [D] . Handoko, Maureen. 2012

机译：人脑脊髓液中的特定淀粉样β低聚物。
6. Alzheimer amyloid-beta peptide forms denaturant-resistant complex with type epsilon 3 but not type epsilon 4 isoform of native apolipoprotein E. [O] . Z. Zhou, J. D. Smith, P. Greengard, 1996

机译：阿尔茨海默氏淀粉样蛋白β肽与天然载脂蛋白E形成与epsilon 3型抗性但不与epsilon 4型同工型的抗变性剂复合物。
7. Binding of human apolipoprotein E to synthetic amyloid beta peptide: isoform-specific effects and implications for late-onset Alzheimer disease. [O] . Strittmatter, W J, Weisgraber, K H, Huang, D Y, 1993

机译：人载脂蛋白E与合成淀粉样β肽的结合：同工型特异性作用及其对迟发性阿尔茨海默病的影响。

Human cerebrospinal fluid apolipoprotein E isoforms are apparently inefficient at complexing with synthetic Alzheimers amyloid-beta peptide (Abeta 1-40 ) in vitro.

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