Buccheri Gianfranco, Torchio Pierfederico, Ferrigno Domenico
Division of Pneumology, Ospedale S. Croce e Carle, Cuneo, Italy.
Chest. 2003 Aug;124(2):622-32. doi: 10.1378/chest.124.2.622.
We have longstanding experience with tissue polypeptide antigen (TPA), a tumor marker of the cytokeratin (CK) family. In the mid-1990s, a new CK marker, CK 19 fragments (CYFRA 21-1), became popular and widely accepted. This is the first study specifically designed to compare the two markers.
Analysis of a single institution database over a 3-year period (ie, 1998 to 2000).
Community-based hospital and second referral level institution for a province of 500,000 people.
The study included 180 new consecutive patients (143 men) with pathologically documented non-small cell lung cancer (NSCLC), who were observed during and after treatment, and eventually were assessed for status.
Anthropometric, clinical, and laboratory data, including TPA and CYFRA 21-1 serum levels, were recorded prospectively. Standard nonparametric tests, Kaplan-Meyer survival analyses, Cox proportional hazards models, receiver-operating characteristic (ROC) curves, and estimates were used for statistical analysis.
A total of 1,299 twin TPA and CYFRA 21-1 serum assays (180 performed at diagnosis and 1,119 performed during or after treatment) were obtained. Intermarker correlation tests revealed incredibly high Spearman rho indexes, ranging from 0.935 at diagnosis to 0.813 to 0.921 at the different follow-up times. The substantial equivalence of the two tests explained all the other results, as follows: their similar profile of correlation with the other variables (objective treatment response: TPA rho, 0.456; CYFRA 21-1 rho, 0.463; follow-up performance status: rho range, 0.424 to 0.435); their superimposable capability to predict important clinical situations (eg, recognizing a metastatic disease at diagnosis with areas under the ROC curve of 0.742 and 0.706, respectively); their nearly identical prognostic significance (the D statistic of the goodness-of-fit of a multivariate survival model: TPA, 851.0; CYFRA 21-1, 851.6).
In most of their traditional clinical applications the two serum tests are equivalent because of their virtual identity. We strongly recommend using a CK test in the evaluation of each NSCLC patient. The choice between TPA and CYFRA 21-1 can be based on nonclinical factors, such as the laboratory experience or preference, and the cost of the two kits.
我们在组织多肽抗原(TPA)方面有着长期经验,TPA是细胞角蛋白(CK)家族的一种肿瘤标志物。在20世纪90年代中期,一种新的CK标志物,CK 19片段(CYFRA 21 - 1)开始流行并被广泛接受。这是第一项专门设计用于比较这两种标志物的研究。
对一个单一机构数据库进行为期3年(即1998年至2000年)的分析。
一所服务于50万人口省份的社区医院及二级转诊机构。
该研究纳入了180例新的连续患者(143例男性),这些患者经病理证实患有非小细胞肺癌(NSCLC),在治疗期间及之后接受观察,并最终进行状态评估。
前瞻性记录人体测量学、临床和实验室数据,包括TPA和CYFRA 21 - 1血清水平。使用标准非参数检验、Kaplan - Meyer生存分析、Cox比例风险模型、受试者操作特征(ROC)曲线及估计值进行统计分析。
共获得1299对TPA和CYFRA 21 - 1血清检测结果(180例在诊断时进行,1119例在治疗期间或之后进行)。标志物间相关性检验显示Spearman相关系数极高,从诊断时的0.935到不同随访时间的0.813至0.921不等。这两种检测的实质等效性解释了所有其他结果,如下:它们与其他变量的相关性相似(客观治疗反应:TPA相关系数为0.456;CYFRA 21 - 1相关系数为0.463;随访时的功能状态:相关系数范围为0.424至0.435);它们预测重要临床情况的能力相当(例如,诊断时识别转移性疾病,ROC曲线下面积分别为0.742和0.706);它们的预后意义几乎相同(多变量生存模型拟合优度的D统计量:TPA为(851.0);CYFRA 21 - 1为(851.6))。
由于这两种血清检测在本质上几乎相同,所以在大多数传统临床应用中它们是等效的。我们强烈建议在评估每例NSCLC患者时使用一种CK检测。在TPA和CYFRA 21 - 1之间的选择可以基于非临床因素,如实验室经验或偏好以及两种试剂盒的成本。
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