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The value of tumour markers in lung cancer

机译:肿瘤标志物在肺癌中的价值

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The pre-treatment serum levels of neuron-specific enolase (NSE), phosphohexose isomerase (PHI) and circulating immune complexes (CC) as tumour markers were compared to measurements of standard haematology and biochemical indices in 73 patients with lung cancer, as an aid to differentiation of tumour type, estimating disease extent, predicting response to therapy and prognosis. Elevated NSE greater than or equal to 12.5 ng ml-1, PHI greater than or equal to 55 mgl-1 levels were observed in 55% of cases for NSE, 90% for PHI and 49% for CC. NSE was significantly elevated in 61% (25/41) of patients with SCLC (P less than 0.005) compared to 41% (13/32) with NSCLC. CC levels were significantly raised in 72% (23/32) of patients with NSCLC (P less than 0.05) compared to 32% with SCLC. The levels of NSE and PHI were not related to tumour stage but CC was significantly raised in limited compared to extensive disease in SCLC (P less than 0.05). Serum albumin was significantly lower in NSCLC compared to SCLC, and median values of alkaline phosphatase, gamma-glutamyltranspeptidase and aminoaspartate transferase were significantly higher in patients with extensive disease. The pre-treatment serum values of NSE, PHI, and CC did not predict the response to therapy or prognosis in the 73 patients with lung cancer. The most important prognostic factor was the number of abnormal routine laboratory parameters (greater than 4) in this group of patients.
机译:将治疗前血清神经元特异性烯醇化酶(NSE),磷酸己糖异构酶(PHI)和循环免疫复合物(CC)的水平作为肿瘤标志物与73例肺癌患者的标准血液学和生化指标进行了比较,作为一项辅助手段区分肿瘤类型,估计疾病程度,预测对治疗的反应和预后。在55%的NSE患者,90%的PHI患者和49%的CC患者中观察到NSE高于或等于12.5 ng ml-1,PHI高于或等于55 mgl-1。 SCLC患者中有61%(25/41)的NSE显着升高(P小于0.005),而NSCLC患者的NSE则有41%(13/32)。 NSCLC患者中CC水平显着升高(72/23)(P小于0.05),而SCLC患者为32%。 NSC和PHI的水平与肿瘤的分期无关,但与SCLC中的广泛性疾病相比,CC在有限的程度上显着升高(P小于0.05)。与小细胞肺癌相比,非小细胞肺癌患者的血清白蛋白水平显着降低,而广泛性疾病患者的碱性磷酸酶,γ-谷氨酰转肽酶和氨基天冬氨酸转移酶的中位值显着更高。 NSE,PHI和CC的治疗前血清值不能预测73例肺癌患者对治疗或预后的反应。最重要的预后因素是这组患者中常规实验室参数异常(大于4)的数量。

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