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一种使用多种生物标志物在治疗期间确定疾病反应的定量方法:应用于乳腺癌

A quantitative approach to determining disease response during therapy using multiple biologic markers: application to carcinoma of the breast.

作者信息

Woo K B, Waalkes T P, Ahmann D L, Tormey D C, Gehrke C W, Oliverio V T

出版信息

Cancer. 1978 May;41(5):1685-703. doi: 10.1002/1097-0142(197805)41:5<1685::aid-cncr2820410507>3.0.co;2-9.

Abstract

This analytical study was undertaken in an effort to develop a model for a quantitative approach to the evaluation of multiple biological marker levels in blood and urine as a means for determining tumor changes during treatment of patients with malignant disease. The potential biologic markers measured in patients with carcinoma of the breast consist of three urinary polyamines (putrescine, spermidine and spermine), three urinary nucleosides (pseudouridine, N2, N2-dimethylguanosine and 1-methylinosine), and plasma carcinoembryonic antigen (CEA). The distribution patterns of the seven markers measured pretreatment and five weeks after initiating therapy were examined by grouping the patients into the three categories of progression, stable, or regression based on their clinical response to treatment. In addition to the individual marker measurements, the pretreatment and posttreatment values of the ratios of the polyamine levels (spermine/putrescine, spermine/spermidine, and spermidine/putrescine) and the nucleoside levels (N2, N2-dimethylguanosine/pseudouridine, 1-methylinosine/pseudouridine, and 1-methylinosine/N2, N2-dimethylguanosine) were also evaluated. In the pretreatment measurements, CEA levels were elevated for 76% of the patients and the three nucleosides were elevated for 36% of the patients and the three nucleosides were elevated for 36% to 37% of the patients. Urinary spermidine and spermine levels were abnormal for 27% and 24%, respectively, while putrescine levels were elevated for 7% of the patients. When all 14 marker measurements and the 12 ratios of these measurements were considered, the multiple regression equation evaluated the treatment results with a multiple correlation coefficient (R = 0.891; P less than 0.100) about 2.4 times higher than with the most sensitive single marker variable, N2, N2-dimethylguanosine/pseudouridine (R = 0.377; P less than 0.05), alone. Stepwise regression analysis revealed that the minimum number of multiple marker measurements and their ratios required to achieve the maximum value of the multiple correlation coefficient (R = 0.653; p = 0.010) was fifteen. These include the pre and posttreatment measurements of CEA, spermine, N2, N2-dimethylguanosine and 1-methylinosine, as well as two ratios of the polyamines and three ratios of the nucleosides in the post-treatment of the polyamines and three ratios of the nucleosides in the post-treatment measurements. These data suggest that the utilization of regression analysis to evaluate the monitoring utility of multiple marker measurements may be of clinical value.

摘要

本分析性研究旨在开发一种定量方法模型,用于评估血液和尿液中的多种生物标志物水平,以此作为确定恶性疾病患者治疗期间肿瘤变化的一种手段。在乳腺癌患者中测量的潜在生物标志物包括三种尿多胺(腐胺、亚精胺和精胺)、三种尿核苷(假尿苷、N2,N2-二甲基鸟苷和1-甲基肌苷)以及血浆癌胚抗原(CEA)。根据患者对治疗的临床反应,将其分为病情进展、稳定或缓解三类,以此检查治疗前及开始治疗五周后所测量的七种标志物的分布模式。除了对单个标志物进行测量外,还评估了多胺水平之比(精胺/腐胺、精胺/亚精胺和亚精胺/腐胺)以及核苷水平之比(N2,N2-二甲基鸟苷/假尿苷、1-甲基肌苷/假尿苷和1-甲基肌苷/N2,N2-二甲基鸟苷)的治疗前和治疗后值。在治疗前测量中,76%的患者CEA水平升高,36%的患者三种核苷水平升高。尿中亚精胺和精胺水平分别有27%和24%异常,而7%的患者腐胺水平升高。当考虑所有14项标志物测量值及其12个比值时,多元回归方程评估治疗结果的复相关系数(R = 0.891;P<0.100)比最敏感的单个标志物变量N2,N2-二甲基鸟苷/假尿苷(R = 0.377;P<0.05)单独使用时高出约2.4倍。逐步回归分析表明,要达到复相关系数的最大值(R = 0.653;p = 0.010)所需的最少多项标志物测量值及其比值数量为15个。这些包括CEA、精胺、N2,N2-二甲基鸟苷和1-甲基肌苷的治疗前和治疗后测量值,以及多胺治疗后的两个比值和核苷治疗后的三个比值。这些数据表明,利用回归分析来评估多项标志物测量的监测效用可能具有临床价值。

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