基于人群队列中细胞周期调控基因的表达与前列腺癌预后
Expression of cell cycle-regulated genes and prostate cancer prognosis in a population-based cohort.
作者信息
Rubicz Rohina, Zhao Shanshan, April Craig, Wright Jonathan L, Kolb Suzanne, Coleman Ilsa, Lin Daniel W, Nelson Peter S, Ostrander Elaine A, Feng Ziding, Fan Jian-Bing, Stanford Janet L
机构信息
Division of Public Health Sciences, Fred Hutchinson Cancer Research Center, Seattle, Washington.
Illumina, Inc., San Diego, California.
出版信息
Prostate. 2015 Sep;75(13):1354-62. doi: 10.1002/pros.23016. Epub 2015 May 18.
BACKGROUND
Prostate cancer (PCa) is clinically and biologically heterogeneous, making it difficult to predict at detection whether it will take an indolent or aggressive disease course. Cell cycle-regulated genes may be more highly expressed in actively dividing cells, with transcript levels reflecting tumor growth rate. Here, we evaluated expression of cell cycle genes in relation to PCa outcomes in a population-based cohort.
METHODS
Gene expression data were generated from tumor tissues obtained at radical prostatectomy for 383 population-based patients (12.3-years average follow-up). The overall mean and individual transcript levels of 30 selected cell cycle genes was compared between patients with no evidence of recurrence (73%) and those who recurred (27%) or died (7%) from PCa.
RESULTS
The multivariate adjusted hazard ratio (HR) for a change from the 25th to 75th percentile of mean gene expression level (range 8.02-10.05) was 1.25 (95%CI 0.96-1.63; P = 0.10) for PCa recurrence risk, and did not vary substantially by Gleason score, TMPRSS2-ERG fusion status, or family history of PCa. For lethal PCa, the HR for a change (25th to 75th percentile) in mean gene expression level was 2.04 (95%CI 1.26-3.31; P = 0.004), adjusted for clinicopathological variables. The ROC curve for mean gene expression level alone (AUC = 0.740) did not perform as well as clinicopathological variables alone (AUC = 0.803) for predicting lethal PCa, and the addition of mean gene expression to clinicopathological variables did not substantially improve prediction (AUC = 0.827; P = 0.18). Higher TK1 expression was strongly associated with both recurrent (P = 6.7 × 10(-5)) and lethal (P = 6.4 × 10(-6)) PCa.
CONCLUSIONS
Mean expression level for 30 selected cell cycle-regulated genes was unrelated to recurrence risk, but was associated with a twofold increase in risk of lethal PCa. However, gene expression had less discriminatory accuracy than clinical variables alone for predicting lethal events. Transcript levels for several genes in the panel were significantly overexpressed in lethal versus non-recurrent PCa.
背景
前列腺癌(PCa)在临床和生物学上具有异质性,这使得在检测时难以预测其疾病进程是惰性还是侵袭性。细胞周期调控基因可能在活跃分裂的细胞中表达更高,转录水平反映肿瘤生长速率。在此,我们在一个基于人群的队列中评估了细胞周期基因的表达与PCa预后的关系。
方法
从383例基于人群的患者(平均随访12.3年)根治性前列腺切除术中获取的肿瘤组织中生成基因表达数据。比较了无复发证据的患者(73%)与复发(27%)或死于PCa(7%)的患者中30个选定细胞周期基因的总体平均和个体转录水平。
结果
对于PCa复发风险,平均基因表达水平从第25百分位数变化到第75百分位数(范围8.02 - 10.05)的多变量调整风险比(HR)为1.25(95%CI 0.96 - 1.63;P = 0.10),并且在Gleason评分、TMPRSS2-ERG融合状态或PCa家族史方面没有显著差异。对于致命性PCa,在调整临床病理变量后,平均基因表达水平变化(第25百分位数到第75百分位数)的HR为2.04(95%CI 1.26 - 3.31;P = 0.004)。仅平均基因表达水平的ROC曲线(AUC = 仅平均基因表达水平的ROC曲线(AUC = 0.740)在预测致命性PCa方面不如单独的临床病理变量(AUC = 0.803),并且将平均基因表达添加到临床病理变量中并没有显著改善预测(AUC = 0.827;P = 0.18)。较高的TK1表达与复发性(P = 6.7×10⁻⁵)和致命性(P = 6.4×10⁻⁶)PCa均密切相关。
结论
30个选定的细胞周期调控基因的平均表达水平与复发风险无关,但与致命性PCa风险增加两倍相关。然而,在预测致命事件方面,基因表达的判别准确性低于单独的临床变量。在致命性PCa与非复发性PCa中,该基因面板中几个基因的转录水平显著过表达。
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