Eastern Hepatobiliary Surgery Hospital, Second Military Medical University, Shanghai 200438, PR China.
Cancer Epidemiol. 2012 Feb;36(1):82-8. doi: 10.1016/j.canep.2011.04.001. Epub 2011 Oct 21.
Hepatocellular carcinoma (HCC) is one of the most common tumors worldwide. Autoantibodies to tumor-associated proteins in the serum profile, as new biomarkers, may improve the early detection of HCC.
In this study, we interrogated a HCC cDNA T7 phage library for tumor-associated proteins using biopan enrichment techniques with HCC patient and normal sera. The enrichment of tumor-associated proteins after biopanning was tested using plaque assay and immunochemical detection. The putative tumor-associated phage clones were collected for PCR and sequencing analysis. Identities of those selected sequences were revealed through the sequence BLAST program. The identified phage-expressed proteins were then used to develop phage protein ELISA to measure matching autoantibodies using 70 HCC patients, 50 chronic hepatitis patients, and 70 normal serum samples. The logistic regression model and leave-one-out validation were used to evaluate predictive accuracies with a single marker as well as with combined markers.
Twenty-six phage-displayed proteins have sequence identity with known or putative tumor-associated proteins. Immunochemical reactivity of patient sera with phage-expressed proteins showed that the autoantibodies to phage-expressed protein CENPF, DDX3, HSPA4, HSPA5, VIM, LMNB1, and TP53 had statistical significance in HCC patients. Measurements of the seven autoantibodies combined in a logistic regression model showed that combined measurements of these autoantibodies was more predictive of disease than any single antibody alone, underscoring the importance of identifying multiple potential markers.
Autoantibody in the serum profiling is a promising approach for early detection and diagnosis of HCC. The panel of autoantibodies appears preferable to achieve superior accuracy rather than an autoantibody alone, and may have significant relevance to tumor biology, novel drug development, and immunotherapies.
肝细胞癌(HCC)是全球最常见的肿瘤之一。血清中肿瘤相关蛋白的自身抗体作为新的生物标志物,可能提高 HCC 的早期检测率。
本研究采用 HCC 患者和正常人血清的 biopan 富集技术,在 HCC cDNA T7 噬菌体文库中查询肿瘤相关蛋白。使用噬菌斑检测和免疫化学检测来测试生物淘选后肿瘤相关蛋白的富集情况。收集可能的肿瘤相关噬菌体克隆进行 PCR 和测序分析。通过序列 BLAST 程序揭示所选序列的身份。然后,使用噬菌体表达蛋白开发噬菌体蛋白 ELISA,以测量 70 例 HCC 患者、50 例慢性肝炎患者和 70 例正常人血清样本中的匹配自身抗体。使用逻辑回归模型和留一法验证,以评估单个标志物和联合标志物的预测准确性。
26 个噬菌体展示的蛋白质与已知或推测的肿瘤相关蛋白具有序列同源性。患者血清与噬菌体表达蛋白的免疫化学反应性表明,抗噬菌体表达蛋白 CENPF、DDX3、HSPA4、HSPA5、VIM、LMNB1 和 TP53 的自身抗体在 HCC 患者中具有统计学意义。在逻辑回归模型中对七种自身抗体的联合测量表明,与任何单一抗体相比,联合测量这些自身抗体对疾病的预测更为准确,这突显了识别多个潜在标志物的重要性。
血清谱中的自身抗体是 HCC 早期检测和诊断的一种很有前途的方法。与单一抗体相比,自身抗体谱似乎更能提高准确性,并且可能与肿瘤生物学、新药开发和免疫治疗有重要关系。
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