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前列腺癌患者的血清胰岛素水平、疾病分期、前列腺特异性抗原(PSA)和 Gleason 评分。

Serum insulin level, disease stage, prostate specific antigen (PSA) and Gleason score in prostate cancer.

作者信息

Lehrer S, Diamond E J, Stagger S, Stone N N, Stock R G

机构信息

Department of Radiation Oncology, Mount Sinai School of Medicine, New York and the Veterans Affairs Medical Center, Bronx, New York, NY 10029, USA.

出版信息

Br J Cancer. 2002 Sep 23;87(7):726-8. doi: 10.1038/sj.bjc.6600526.

Abstract

In the present study, we assessed the relationship of serum insulin levels and three surrogate markers of recurrence, T stage, PSA, and Gleason score, in men with localized prostate cancer. Participants in our study were found through urology and radiation oncology clinics, and all eligible patients were asked to take part. All patients were asymptomatic and had been initially diagnosed on the basis of rising PSA or abnormal physical examination. Histological confirmation of diagnosis was obtained for all subjects. Serum insulin levels were determined by chemoluminescent assay with a standard, commercially available instrument. Patients were divided into three previously defined risk groups: Low risk: PSA < or =10, stage < or =T2a, or Gleason grade < or =6. Medium risk: 10 <PSA < or =15, Gleason 7 or stage T2b. High risk: Gleason >7, tumour in seminal vesicle biopsy, PSA >15 or stage T2c or T3. One hundred and sixty-three men with prostate cancer were studied. There was a significant increase in serum insulin with risk group (P=0.003, one way anova). Tukey's multiple range test showed that the insulin levels of high risk patients were significantly higher than the insulin levels of medium and low risk patients (P=0.05) but the insulin levels of medium and low risk patients were not significantly different from one another. Multivariate linear regression, with insulin as the dependent variable, Gleason score, PSA, and T stage (T1, T2, T3) as the independent variables, was significant overall (P<0.001, r(2)=0.120). Increased T stage was independently correlated with increased serum insulin levels (P<0.001). Gleason score was negatively, insignificantly correlated with serum insulin level (P=0.059). The positive correlation of PSA and insulin level was not significant (P=0.097). To assure normal distribution of insulin and PSA values, the regression was repeated with log (insulin) as the dependent variable, log (PSA), T stage (T1, T2, T3), and Gleason score as independent variables. The regression was significant overall (P=0.002, r(2) =0.095). Increased T stage was independently correlated with increased log (insulin level) (P=0.026). Gleason score was negatively, insignificantly correlated with log (insulin) level (P=0.728). The positive correlation of log (PSA) and log (insulin) levels was significant (P=0.010). The relationship between increased insulin level and advanced tumour stage in prostate cancer we describe here is biologically quite plausible, since insulin is a growth factor. Further studies may document whether serum insulin levels might be a useful biomarker of prostate cancer stage.

摘要

在本研究中,我们评估了局限性前列腺癌男性患者血清胰岛素水平与复发的三个替代标志物、T分期、前列腺特异性抗原(PSA)和 Gleason评分之间的关系。我们通过泌尿外科和放射肿瘤学诊所招募研究参与者,所有符合条件的患者均被邀请参与。所有患者均无症状,最初是根据PSA升高或体格检查异常确诊的。所有受试者均获得了组织学确诊。血清胰岛素水平通过化学发光法使用标准的商用仪器测定。患者被分为三个先前定义的风险组:低风险:PSA≤10,分期≤T2a,或Gleason分级≤6。中风险:10<PSA≤15,Gleason 7或分期T2b。高风险:Gleason>7,精囊活检有肿瘤,PSA>15或分期T2c或T3。对163名前列腺癌男性进行了研究。血清胰岛素水平随风险组增加而显著升高(P = 0.003,单因素方差分析)。Tukey多重极差检验显示,高风险患者的胰岛素水平显著高于中低风险患者(P = 0.05),但中低风险患者的胰岛素水平彼此之间无显著差异。以胰岛素为因变量,Gleason评分、PSA和T分期(T1、T2、T3)为自变量进行多变量线性回归,总体具有显著性(P<0.001,r² = 0.120)。T分期增加与血清胰岛素水平升高独立相关(P<0.001)。Gleason评分与血清胰岛素水平呈负相关,但不显著(P = 0.059)。PSA与胰岛素水平的正相关不显著(P = 0.097)。为确保胰岛素和PSA值呈正态分布,以log(胰岛素)为因变量,log(PSA)、T分期(T1、T2、T3)和Gleason评分为自变量重复进行回归。回归总体具有显著性(P = 0.002,r² = 0.095)。T分期增加与log(胰岛素水平)升高独立相关(P = 0.026)。Gleason评分与log(胰岛素)水平呈负相关,但不显著(P = 0.728)。log(PSA)与log(胰岛素)水平的正相关具有显著性(P = 0.010)。我们在此描述的前列腺癌中胰岛素水平升高与肿瘤晚期之间的关系在生物学上相当合理,因为胰岛素是一种生长因子。进一步的研究可能会证明血清胰岛素水平是否可能是前列腺癌分期的有用生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bee8/2364268/1a0204ef2ed5/87-6600526f1.jpg

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