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Quantification of clusterin in paired cerebrospinal fluid and plasma samples

机译:配对脑脊液和血浆样品中簇蛋白的定量

摘要

Background: Clusterin (ApoJ) is an amyloid-associated protein and plays an important role in Alzheimer's disease (AD) pathology. Recent genome-wide association studies have indicated that certain genetic variants increase the risk of developing AD. To determine if the expression of clusterin is different in AD patients, both systemically and locally in the brain, differs between (subgroups of) AD patients and non-AD cases, an assay available that detects clusterin in both plasma and cerebrospinal fluid (CSF) with equal sensitivity would be helpful. Methods: We compared four different commercially available antibodies in their ability to detect recombinant clusterin and immune-purified human clusterin. Specificity was tested on western blot and in ELISA systems, and selection was based on the ability to detect clusterin in CSF and plasma. A sandwich ELISA was developed and validated with monoclonal antibody G7 as capture, and rabbit polyclonal (Alexis) antibodies for detection. Results: Our ELISA measured clusterin concentrations in plasma and CSF with dynamic ranges of 2-70 mg/L and 0.5-40 mg/L, respectively. The assays showed 99.8% recovery in CSF and 97% recovery in plasma. Intra-assay coefficient of variation was 1.4% and inter-assay 8.8%. The assay shows no cross-reactivity with related apolipoproteins. Clusterin quantification is dependent on the type of storage for plasma samples. A single freeze/thaw cycle caused fluctuations of clusterin concentrations in plasma, while clusterin in CSF is stable for up to five cycles. Conclusions: We have successfully developed a clusterin ELISA that reliably measures CSF and plasma clusterin concentrations. In a pilot study, all samples gave results that were well within the dynamic range of the assay, with low variations. Freshly stored plasma samples are crucial for accurate clusterin quantification. © The Author(s) 2013 Reprints and permissions: sagepub.co.uk/journalsPermissions.nav.
机译:背景:Clusterin(ApoJ)是一种淀粉样蛋白相关蛋白,在阿尔茨海默氏病(AD)病理学中起着重要作用。最近的全基因组关联研究表明,某些遗传变异会增加罹患AD的风险。为了确定在系统性和局部性AD患者中,AD患者(亚组)和非AD患者之间的簇蛋白表达是否不同,一种可用的检测血浆和脑脊液(CSF)中簇蛋白的方法具有相同的敏感性将是有帮助的。方法:我们比较了四种不同的市售抗体检测重组簇蛋白和免疫纯化人簇蛋白的能力。在Western印迹法和ELISA系统中测试了特异性,选择的基础是检测CSF和血浆中簇蛋白的能力。开发了夹心ELISA,并用单克隆抗体G7作为捕获抗体和兔多克隆(Alexis)抗体进行了验证,以进行检测。结果:我们的ELISA测定血浆和CSF中的簇蛋白浓度分别在2-70 mg / L和0.5-40 mg / L的动态范围内。该测定显示脑脊液中99.8%的回收率和血浆中97%的回收率。批内变异系数为1.4%,批间变异为8.8%。该测定显示与相关载脂蛋白无交叉反应。簇蛋白的定量取决于血浆样品的储存类型。单个冷冻/解冻循环会导致血浆中簇蛋白浓度波动,而脑脊液中的簇蛋白最多可稳定五个周期。结论:我们已经成功开发了一种clusterin ELISA,可以可靠地测量CSF和血浆中clusterin的浓度。在一项前期研究中,所有样品的结果均在测定的动态范围内,且变化很小。新鲜储存的血浆样品对于准确的簇蛋白定量至关重要。 ©作者2013转载和许可:sagepub.co.uk/journalsPermissions.nav。

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