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肿瘤相关抗原自身抗体与异常甲胎蛋白联合增强对肝细胞癌的免疫诊断。

Autoantibodies to tumor-associated antigens combined with abnormal alpha-fetoprotein enhance immunodiagnosis of hepatocellular carcinoma.

机构信息

Department of Biological Sciences, The University of Texas at El Paso, El Paso, TX 79968, USA.

出版信息

Cancer Lett. 2010 Mar 1;289(1):32-9. doi: 10.1016/j.canlet.2009.07.016. Epub 2009 Aug 15.

Abstract

The identification and characterization of tumor-associated antigens (TAAs) and their use in antigen mini-arrays for cancer immunodiagnosis has been of interest recently as an approach to cancer detection. In this study, autoantibodies in sera from a patient with HCC were used as probes to immunoscreen a HepG2 cDNA expression library for the identification of TAAs involved in malignant liver transformation. Recombinant proteins from two genes identified in this manner, Sui1 and RalA were expressed, purified and used as antigens in immunoassays to detect the presence of antibodies in sera from 77 patients with HCC, 30 with chronic hepatitis (CH), 30 with liver cirrhosis (LC) and 82 normal human sera (NHS). The prevalence of antibody to Sui1 and RalA in HCC were 11.7% (9/77) and 19.5% (15/77), respectively, which were significantly higher than prevalence in liver cirrhosis (3.3% and 3.3%), chronic hepatitis (0% and 0%) and normal human sera (0% and 0%). When Sui1 and RalA were added to a panel of eight other TAAs used in a previous study, the final cumulative prevalence of anti-TAA antibodies in HCC to the 10 TAA array was raised to 66.2% (51/77). The specificity for HCC compared with LC, CH and NHS, was 66.7%, 80.0%, and 87.8%, respectively. When anti-TAA was added to abnormal serum AFP as combined diagnostic markers, it raised the diagnostic sensitivity from 66.2% to 88.7%. AFP and anti-TAA were independent markers and the simultaneous use of these two markers significantly resulted in the increased sensitivity of HCC detection.

摘要

最近,人们对鉴定和描述肿瘤相关抗原(TAA)及其在癌症免疫诊断中的应用产生了浓厚的兴趣,将其作为癌症检测的一种方法。在这项研究中,我们利用一名 HCC 患者血清中的自身抗体作为探针,对 HepG2 cDNA 表达文库进行免疫筛选,以鉴定参与恶性肝转化的 TAA。以这种方式鉴定出的两个基因(Sui1 和 RalA)的重组蛋白被表达、纯化,并作为抗原用于免疫检测,以检测 77 例 HCC 患者、30 例慢性肝炎(CH)患者、30 例肝硬化(LC)患者和 82 例正常人血清(NHS)中抗体的存在。Sui1 和 RalA 抗体在 HCC 中的阳性率分别为 11.7%(9/77)和 19.5%(15/77),明显高于肝硬化(3.3%和 3.3%)、慢性肝炎(0%和 0%)和正常人血清(0%和 0%)。当 Sui1 和 RalA 与之前研究中使用的其他 8 个 TAA 组合成一个 panel 时,对 10 个 TAA 组合的 HCC 患者抗 TAA 抗体的最终累积阳性率提高到 66.2%(51/77)。与 LC、CH 和 NHS 相比,对 HCC 的特异性分别为 66.7%、80.0%和 87.8%。当将抗-TAA 与异常血清 AFP 联合作为诊断标志物时,其诊断敏感性从 66.2%提高到 88.7%。AFP 和抗-TAA 是独立的标志物,同时使用这两种标志物可显著提高 HCC 的检测灵敏度。

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