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Antibody validation by quantitative analysis of protein expression using expression of Met in breast cancer as a model

机译:以Met在乳腺癌中的表达为模型,通过蛋白质表达的定量分析进行抗体验证

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Expression of Met, the Hepatocyte Growth Factor receptor, has been shown to have prognostic value in numerous types of cancer including breast, gastric, cervical and head and neck carcinomas. However, traditional analyses of expression have shown variable results and a lack of reproducibility. The AQUA? system is a method of quantitative in situ analysis of protein expression that allows the assessment of reproducibility of both antibodies and assay conditions. Here, we illustrate the necessity for antibody validation when assaying the prognostic value of a potential biomarker. Using five antibodies to the intracellular domain of the Met receptor and 10 cell line controls, we quantitatively assess reproducibility of protein expression. We show that many antibodies are not reproducible at a quantitative level from lot to lot or assay to assay, suggesting new criteria for antibody validation. We also build upon past literature addressing the prognostic value of Met in a cohort of 640 cases of invasive breast cancer on a tissue microarray. We show that high levels of expression of nuclear Met, as determined by antibodies to the intracellular domain and defined as nuclear by subcellular compartmental analysis, is associated with shorter disease-specific survival in breast cancer.
机译:肝细胞生长因子受体Met的表达已显示对多种类型的癌症具有预后价值,包括乳腺癌,胃癌,宫颈癌和头颈癌。但是,传统的表达分析显示结果可变且缺乏可重复性。水族?系统是对蛋白质表达进行定量原位分析的方法,可用于评估抗体的可重复性和测定条件。在这里,我们说明了在分析潜在生物标记物的预后价值时进行抗体验证的必要性。使用五种针对Met受体的细胞内结构域的抗体和10个细胞系对照,我们定量评估了蛋白质表达的可重复性。我们显示,从批次到批次或从一种测定到另一种测定,许多抗体在定量水平上均不可再现,为抗体验证提出了新的标准。我们还基于处理Met在组织芯片上的640例浸润性乳腺癌队列中的预后价值的以往文献为基础。我们显示高水平表达的核Met,由细胞内结构域的抗体确定,并通过亚细胞区室分析定义为核,与乳腺癌中疾病特异性生存期较短有关。

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