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An explorative study on the clinical utility of baseline and serial serum tumour marker measurements in advanced upper gastrointestinal cancer.

机译:在晚期上消化道癌中基线和系列血清肿瘤标志物测定的临床效用的探索性研究。

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The value of early tumour marker changes during palliative chemotherapy in patients with upper gastrointestinal adenocarcinoma (UGIA) is unclear. Seventy-three patients with advanced UGIA were randomised to receive 45 mg/m2 docetaxel or 180 mg/m2 irinotecan with 5-FU/leucovorin. After every 2nd course the patients were crossed over to the other regimen. Serum was sampled before start of chemotherapy and every 2nd week during 8 weeks for CEA, TPA, TPS, CA72-4, CA19-9 and CA242 measurements. Eighteen patients (25%) had partial response (PR) and 21 patients had stable disease for at least 4 months (SD4). All baseline marker levels, except CA72-4, correlated with time to progression and survival. Patients with normal levels, except CA72-4, also had more clinical responses (PR+SD4) than patients with elevated values. Tumour marker changes early during treatment provided modest predictive information for tumour response and survival. A model combining baseline level, the change and the interaction between them gave the best prediction of outcome, however, insignificantly better than baseline level for all markers except CA242. Baseline tumour marker levels provide prognostic information for patients with UGIA on palliative chemotherapy. Early changes generally failed to provide accurate information for tumour response and survival.
机译:目前尚不清楚上消化道腺癌(UGIA)患者姑息化疗期间早期肿瘤标志物改变的价值。 73例晚期UGIA患者被随机分配接受45 mg / m2多西他赛或180 mg / m2伊立替康与5-FU /亚叶酸钙的联合治疗。每第二个疗程结束后,将患者转移至另一种疗程。在开始化疗之前以及在8周中的每2周进行一次血清采样,以进行CEA,TPA,TPS,CA72-4,CA19-9和CA242测量。 18名患者(25%)有部分缓解(PR),21名患者病情稳定至少4个月(SD4)。除CA72-4外,所有基线标记物水平均与进展时间和生存时间相关。除CA72-4水平正常外,患者的临床反应(PR + SD4)也高于升高值的患者。治疗早期的肿瘤标志物变化为肿瘤反应和生存提供了适度的预测信息。结合基线水平,变化和它们之间的相互作用的模型给出了最佳的结局预测,但是,除CA242以外,所有指标均优于基线水平。基线肿瘤标志物水平可为UGIA姑息化疗患者提供预后信息。早期变化通常无法为肿瘤反应和生存提供准确的信息。

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