Oncimmune Ltd.
Division of Breast Surgery, University of Nottingham, Clinical Sciences Building, Nottingham City Hospital, Nottingham, UK.
Ann Oncol. 2010 Aug;21(8):1687-1693. doi: 10.1093/annonc/mdp606. Epub 2010 Feb 2.
Publications on autoantibodies to tumour-associated antigens (TAAs) have failed to show either calibration or reproducibility data. The validation of a panel of six TAAs to which autoantibodies have been described is reported here.
Three separate groups of patients with newly diagnosed lung cancer were identified, along with control individuals, and their samples used to validate an enzyme-linked immunosorbant assay. Precision, linearity, assay reproducibility and antigen batch reproducibility were all assessed.
For between-replicate error, samples with higher signals gave coefficients of variation (CVs) in the range 7%-15%. CVs for between-plate variation were only 1%-2% higher. For between-run error, CVs were in the range 15%-28%. In linearity studies, the slope was close to 1.0 and correlation coefficient values were generally >0.8. The sensitivity and specificity of individual batches of antigen varied slightly between groups of patients; however, the sensitivity and specificity of the panel of antigens as a whole remained constant. The validity of the calibration system was demonstrated.
A calibrated six-panel assay of TAAs has been validated for identifying nearly 40% of primary lung cancers via a peripheral blood test. Levels of reproducibility, precision and linearity would be acceptable for an assay used in a regulated clinical setting.
关于肿瘤相关抗原(TAA)自身抗体的出版物未能显示校准或重现性数据。本文报告了一组已描述自身抗体的六个 TAA 面板的验证情况。
确定了三组新诊断的肺癌患者以及对照组个体,并使用其样本验证酶联免疫吸附测定法。评估了精密度、线性、测定重复性和抗原批重复性。
对于重复间误差,信号较高的样本的变异系数(CV)在 7%-15%范围内。板间变异的 CV 仅高出 1%-2%。对于运行间误差,CV 在 15%-28%范围内。在线性研究中,斜率接近 1.0,相关系数值通常>0.8。单个批次抗原的敏感性和特异性在患者组之间略有差异;然而,作为一个整体的抗原面板的敏感性和特异性保持不变。校准系统的有效性得到了证明。
通过外周血检测,经过校准的六重 TAA 检测试剂盒已验证可识别近 40%的原发性肺癌。在监管临床环境中使用的测定中,可接受的重现性、精密度和线性度水平。
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