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首页> 外文期刊>British Journal of Cancer >Tumour markers for prediction of survival and monitoring of remission in small cell lung cancer
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Tumour markers for prediction of survival and monitoring of remission in small cell lung cancer

机译:预测小细胞肺癌生存率和监测缓解的肿瘤标志物

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Levels of the tumour markers neurone specific enolase (NSE), lactate dehydrogenase (LDH), chromogranin A (ChrA) and carcinoembryonic antigen (CEA) were measured in serum taken at presentation and during treatment, remission and relapse from 154 patients who received chemotherapy for small cell lung cancer at a single centre over a 6 year period. At presentation NSE was the most frequently elevated marker, being raised in 81% of patients and significantly higher in extensive as opposed to limited disease, as were LDH and ChrA. The response rate to therapy was best correlated with presentation level of ChrA, being 79% for those whose levels were within twice the upper limit of normal and 51% above (P < 0.01). Multivariate regression analysis showed NSE, performance status and albumin at presentation to be the best independent predictors of survival. Patients with NSE below twice the upper limit of normal, Karnofsky performance status of 80 or above and albumin 35 g l-1 or above had a median survival of 15 months with 25% alive at 2 years, whilst those with NSE above twice normal, Karnofsky below 80 and albumin less that 35 g l-1 had all died by 8 months. Changes in marker levels during therapy were of low predictive value for outcome although the finding of rising NSE during chemotherapy after an initial fall correlated with significantly reduced duration of remission. There was a strong inverse correlation between the NSE level at the time of response and duration of remission (P < 0.0001). Prediction of relapse was most reliable with ChrA, 52% of patients having rising levels before clinical evidence of disease recurrence.
机译:在呈报时以及在治疗,缓解和复发期间从154例接受过化疗的患者中获取的血清中测量了肿瘤标志物神经元特异性烯醇化酶(NSE),乳酸脱氢酶(LDH),嗜铬粒蛋白A(ChrA)和癌胚抗原(CEA)的水平。在6年内在单个中心接受小细胞肺癌治疗。演讲时,NSE是最常见的升高标志物,在81%的患者中升高,与LDH和ChrA一样,在有限的疾病中,NSE显着升高。对治疗的反应率与ChrA的呈递水平最相关,对于那些处于正常上限的两倍以内且高于正常值的51%的患者,其应答率为79%(P <0.01)。多元回归分析表明,NSE,表现状态和白蛋白是生存的最佳独立预测因子。 NSE低于正常上限两倍的患者,Karnofsky机能状态为80或更高,白蛋白为35 g l-1或更高,中位生存期为15个月,存活2年时存活率为25%,而NSE高于正常值两倍的患者80岁以下的卡诺夫斯基和小于35 g l-1的白蛋白在8个月内全部死亡。治疗期间标志物水平的变化对结局的预测价值较低,尽管最初跌倒后化疗期间NSE升高的发现与缓解时间的明显减少有关。响应时的NSE水平与缓解时间之间存在很强的负相关关系(P <0.0001)。对于ChrA,复发的预测是最可靠的,有52%的患者在疾病复发的临床证据之前水平升高。

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