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首页> 外文期刊>Journal of proteomics >An optimized predictor panel for colorectal cancer diagnosis based on the combination of tumor-associated antigens obtained from protein and phage microarrays
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An optimized predictor panel for colorectal cancer diagnosis based on the combination of tumor-associated antigens obtained from protein and phage microarrays

机译:基于从蛋白质和噬菌体微阵列获得的肿瘤相关抗原的组合,用于大肠癌诊断的优化预测子面板

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摘要

Humoral response in cancer patients appears early in cancer progression and can be used for diagnosis, including early detection. By using human recombinant protein and T7 phage microarrays displaying colorectal cancer (CRC)-specific peptides, we previously selected 6 phages and 6 human recombinant proteins as tumor-associated antigens (TAAs) with high diagnostic value. After completing validation in biological samples, TAAs were classified according to their correlation, redundancy in reactivity patterns and multiplex diagnostic capabilities. For predictor model optimization, TAAs were reanalyzed with a new set of samples. A combination of three phages displaying peptides homologous to GRN, NHSL1 and SREBF2 and four proteins PIM1, MAPKAPK3, FGFR4 and ACVR2B, achieved an area under the curve (AUC) of 94%, with a sensitivity of 89.1% and specificity of 90.0%, to correctly predict the presence of cancer. For early colorectal cancer stages, the AUC was 90%, with a sensitivity of 88.2% and specificity of 82.6%. In summary, we have defined an optimized predictor panel, combining TAAs from different sources, with highly improved accuracy and diagnostic value for colorectal cancer. This article is part of a Special Issue entitled: Translational Proteomics.
机译:癌症患者的体液反应出现在癌症进展的早期,可用于诊断,包括早期发现。通过使用人类重组蛋白和显示结直肠癌(CRC)特异性肽的T7噬菌体微阵列,我们先前选择了6个噬菌体和6个人类重组蛋白作为具有高诊断价值的肿瘤相关抗原(TAA)。在生物样品中完成验证后,根据TAA的相关性,反应模式的冗余性和多重诊断能力对TAA进行分类。对于预测器模型优化,使用一组新样本重新分析了TAA。展示与GRN,NHSL1和SREBF2同源的三种噬菌体肽和四种蛋白PIM1,MAPKAPK3,FGFR4和ACVR2B的组合,曲线下面积(AUC)为94%,灵敏度为89.1%,特异性为90.0%,正确预测癌症的存在。对于早期大肠癌阶段,AUC为90%,敏感性为88.2%,特异性为82.6%。总而言之,我们定义了一个优化的预测器面板,将来自不同来源的TAA组合在一起,具有高度提高的准确性和对结直肠癌的诊断价值。本文是《问题蛋白质组学》特刊的一部分。

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