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Autoantibodies as diagnostic biomarkers for lung cancer: A systematic review

机译:自身抗体作为肺癌的诊断生物标记物:系统评价

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摘要

Lung cancer (LC) accounts for the largest number of tumor-related deaths worldwide. As the overall 5-year survival rate of LC is associated with its stages at detection, development of a cost-effective and noninvasive cancer screening method is necessary. We conducted a systematic review to evaluate the diagnostic values of single and panel tumor-associated autoantibodies (TAAbs) in patients with LC. This review included 52 articles with 64 single TAAbs and 19 with 20 panels of TAAbs. Enzyme-linked immunosorbent assays (ELISA) were the most common detection method. The sensitivities of single TAAbs for all stages of LC ranged from 3.1% to 92.9% (mean: 45.2%, median: 37.1%), specificities from 60.6% to 100% (mean: 88.1%, median: 94.9%), and AUCs from 0.416 to 0.990 (mean: 0.764, median: 0.785). The single TAAb with the most significant diagnostic value was the autoantibody against human epididymis secretory protein (HE4) with the maximum sensitivity 91% for NSCLC. The sensitivities of the panel of TAAbs ranged from 30% to 94.8% (mean: 76.7%, median: 82%), specificities from 73% to 100% (mean: 86.8%, median: 89.0%), and AUCs from 0.630 to 0.982 (mean: 0.821, median: 0.820), and the most significant AUC value in a panel (M13 Phage 908, 3148, 1011, 3052, 1000) was 0.982. The single TAAb with the most significant diagnostic calue for early stage LC, was the autoantibody against Wilms tumor protein 1 (WT1) with the maximum sensitivity of 90.3% for NSCLC and its sensitivity and specificity in a panel (T7 Phage 72, 91, 96, 252, 286, 290) were both above 90.0%. Single or TAAbs panels may be useful biomarkers for detecting LC patients at all stages or an early-stage in high-risk populations or health people, but the TAAbs panels showed higher detection performance than single TAAbs. The diagnostic value of the panel of six TAAbs, which is higher than the panel of seven TAAbs, may be used as potential biomarkers for the early detection of LC and can probably be used in combination with low-dose CT in the clinic.
机译:肺癌(LC)占全球与肿瘤相关的死亡人数最多。由于LC的总体5年生存率与其检测阶段有关,因此有必要开发一种经济有效的无创性癌症筛查方法。我们进行了系统的评估,以评估单个和小组肿瘤相关自身抗体(TAAb)在LC患者中的诊断价值。这篇综述包括52篇文章,其中包含64种单一TAAb,19篇文章中包含20种TAAb。酶联免疫吸附测定(ELISA)是最常见的检测方法。单个TAAb对LC所有阶段的敏感性为3.1%至92.9%(平均值:45.2%,中位数:37.1%),特异性从60.6%至100%(平均值:88.1%,中位数:94.9%)和AUC从0.416到0.990(平均值:0.764,中位数:0.785)。诊断价值最高的单个TAAb是抗人附睾分泌蛋白(HE4)的自身抗体,对NSCLC的敏感性最高为91%。 TAAb的敏感性范围为30%至94.8%(平均值:76.7%,中位数:82%),特异性范围为73%至100%(平均值:86.8%,中位数:89.0%)和AUC范围为0.630至0.982(平均值:0.821,中位数:0.820),面板中最显着的AUC值(M13噬菌体908、3148、1011、3052、1000)为0.982。早期LC诊断最重要的单一TAAb是抗Wilms肿瘤蛋白1(WT1)的自身抗体,其对NSCLC的最大敏感性为90.3%,其敏感性和特异性在面板中均有效(T7 Phage 72、91、96 (252、286、290)均高于90.0%。单一或TAAbs面板可能是检测高危人群或健康人群中所有阶段或早期LC患者的有用的生物标志物,但TAAbs面板显示出比单个TAAb更高的检测性能。六种TAAb的组的诊断价值高于七种TAAb的组的诊断价值,可以用作早期检测LC的潜在生物标志物,并且可能与临床中的低剂量CT结合使用。

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