首页> 美国卫生研究院文献>British Journal of Cancer >Tumour marker concentration at the start of chemotherapy is a stronger predictor of treatment failure than marker half-life: a study in patients with disseminated non-seminomatous testicular cancer.
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Tumour marker concentration at the start of chemotherapy is a stronger predictor of treatment failure than marker half-life: a study in patients with disseminated non-seminomatous testicular cancer.

机译:化疗开始时的肿瘤标志物浓度比标志物半衰期更能预示治疗失败:这项针对散播性非精原细胞性睾丸癌患者的研究。

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摘要

We investigated the prognostic value of the serum half-life of human chorionic gonadotrophin (HCG) and alpha-fetoprotein (AFP) during induction chemotherapy and the relative prognostic importance of initial marker concentrations and marker half-life. Marker half-lives were calculated using two abnormal values observed between day 8 and day 22 of the first chemotherapy cycle. Moreover, analyses were carried out using day 43 as the second measurement point. Treatment failure at any time was chosen as the end point. The relative prognostic influence of marker half-lives and initial marker concentrations was tested in univariate and multivariate analyses. Half-lives were considered to be prolonged if > 3 days for HCG and > 6 days for AFP. In addition, we separated patients into those with half-lives > 6 days for HCG and those with half-lives > 10 days for AFP to examine whether these long half-lives were associated with a poor prognosis. A group of 669 patients treated with cisplatin combination chemotherapy was studied. Forty-two per cent of the patients had normal HCG and 37% had normal AFP at the start of chemotherapy. At day 22, HCG was still elevated in 138 patients and AFP in 211. At day 43, the numbers of these patients were 35 and 80 respectively. Based on the measurements obtained on day 8 and day 22, a half-life of HCG > 3 days or > 6 days and/or a half-life AFP > 6 days or > 10 days did not accurately predict treatment failure (P=0.413 and P=0.851, respectively; values obtained using tests for trend). However, initial marker concentrations of HCG and/or AFP > 1000 IU l(-1) were highly significant prognosticators for treatment failure (P=0.001 and P < 0.001 respectively), independent of half-life values. Half-lives calculated with the values obtained on day 43 did not contribute to the accuracy of the prediction of treatment failure. We conclude that half-lives of HCG and AFP during induction chemotherapy are inaccurate parameters for the prediction of treatment failure. In contrast, initial serum concentrations of HCG and AFP are highly significant in the prediction of unfavourable treatment outcome.
机译:我们调查了人绒毛膜促性腺激素(HCG)和甲胎蛋白(AFP)血清半衰期在诱导化疗中的预后价值以及初始标志物浓度和标志物半衰期的相对预后重要性。使用在第一个化疗周期的第8天和第22天之间观察到的两个异常值计算标记的半衰期。此外,使用第43天作为第二测量点进行分析。随时选择治疗失败作为终点。在单变量和多变量分析中测试了标志物半衰期和初始标志物浓度的相对预后影响。如果HCG> 3天,AFP> 6天,则认为半衰期延长。此外,我们将HCG的半衰期> 6天的患者和AFP的半衰期> 10天的患者分为两组,以检查这些长的半衰期是否与不良预后相关。研究了一组669例顺铂联合化疗的患者。在化疗开始时,有42%的患者HCG正常,而37%的AFP正常。在第22天,138例患者的HCG仍升高,在211例中的AFP仍升高。在第43天,这些患者的人数分别为35和80。根据在第8天和第22天获得的测量结果,HCG的半衰期> 3天或> 6天和/或AFP的半衰期> 6天或> 10天不能准确预测治疗失败(P = 0.413和P = 0.851;分别使用趋势测试获得的值)。但是,HCG和/或AFP的初始标志物浓度> 1000 IU l(-1)是治疗失败的高度重要预后因素(分别为P = 0.001和P <0.001),与半衰期值无关。根据第43天获得的值计算的半衰期不会有助于预测治疗失败的准确性。我们得出结论,诱导化疗期间HCG和AFP的半衰期对于预测治疗失败是不准确的参数。相反,HCG和AFP的初始血清浓度在不良治疗结果的预测中非常重要。

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