一种用于预测局限性肾细胞癌手术后复发的 16 基因检测:开发和验证研究。
A 16-gene assay to predict recurrence after surgery in localised renal cell carcinoma: development and validation studies.
机构信息
Cleveland Clinic, Cleveland, OH, USA.
Genomic Health Inc, Redwood City, CA, USA.
出版信息
Lancet Oncol. 2015 Jun;16(6):676-85. doi: 10.1016/S1470-2045(15)70167-1. Epub 2015 May 12.
BACKGROUND
The likelihood of tumour recurrence after nephrectomy in localised clear cell renal cell carcinoma is well characterised by clinical and pathological parameters. However, these assessments can be improved and personalised by the addition of molecular characteristics of each patient's tumour. We aimed to develop and validate a prognostic multigene signature to improve prediction of recurrence risk in clear cell renal cell carcinoma.
METHODS
In the development stage, we investigated the association between expression of 732 genes, measured by reverse-transcription PCR, and clinical outcome in 942 patients with stage I-III clear cell renal cell carcinoma who had undergone a nephrectomy at the Cleveland Clinic (OH, USA). 516 genes were associated with recurrence-free interval. 11 of these genes were selected by further statistical analyses, and were combined with five reference genes (ie, 16 genes in total), from which a recurrence score algorithm was developed. The recurrence score was then validated in an independent cohort of 626 patients from France with stage I-III clear cell renal cell carcinoma who had also undergone nephrectomy. The association between the recurrence score and the risk of recurrence and cancer-specific survival in the first 5 years after surgery was assessed using Cox proportional hazard regression, stratified by tumour stage (stage I vs stage II vs III).
FINDINGS
In our primary univariate analysis, the continuous recurrence score (median 37, IQR 31-45) was significantly associated with recurrence-free interval (hazard ratio 3·91 [95% CI 2·63-5·79] for a 25-unit increase in score, p<0·0001). In multivariable analyses, the recurrence score was significantly associated with the risk of tumour recurrence (hazard ratio per 25-unit increase in the score 3·37 [95% CI 2·23-5·08], p<0·0001) after stratification by stage and adjustment for tumour size, grade, or Leibovich score. The recurrence score was able to identify a clinically significant number of both high-risk stage I and low-risk stage II-III patients. A heterogeneity study on separate samples showed little to no intratumoural variability among the 16 genes.
INTERPRETATION
Our findings validate the recurrence score as a predictor of clinical outcome in patients with stage I-III clear cell renal cell carcinoma, providing a more accurate and individualised risk assessment beyond existing clinical and pathological parameters.
FUNDING
Genomic Health Inc and Pfizer Inc.
背景
在局限性肾透明细胞癌患者中,肾切除术后肿瘤复发的可能性可以通过临床和病理参数很好地描述。然而,通过添加每位患者肿瘤的分子特征,可以改善和个性化这些评估。我们旨在开发和验证一种预后多基因标记物,以提高对肾透明细胞癌复发风险的预测。
方法
在开发阶段,我们通过逆转录 PCR 测量了 942 例 I-III 期肾透明细胞癌患者的 732 个基因的表达,这些患者在克利夫兰诊所(美国俄亥俄州)接受了肾切除术,并调查了这些基因表达与无复发生存期之间的关联。516 个基因与无复发生存期相关。通过进一步的统计分析选择了其中 11 个基因,并结合 5 个参考基因(即总共 16 个基因),由此开发了一个复发评分算法。然后在法国的一个具有 I-III 期肾透明细胞癌且接受肾切除术的 626 例患者的独立队列中验证了复发评分。使用 Cox 比例风险回归评估手术后 5 年内复发评分与复发风险和癌症特异性生存率之间的关系,按肿瘤分期(I 期与 II 期与 III 期)分层。
发现
在我们的初步单变量分析中,连续的复发评分(中位数 37,IQR 31-45)与无复发生存期显著相关(评分增加 25 个单位时的危险比为 3.91[95%CI 2.63-5.79],p<0.0001)。在多变量分析中,复发评分与肿瘤复发的风险显著相关(评分每增加 25 个单位,风险比为 3.37[95%CI 2.23-5.08],p<0.0001),分层后按肿瘤大小、分级或 Leibovich 评分进行调整。复发评分能够识别出具有临床意义的高风险 I 期和低风险 II-III 期患者。在单独样本的异质性研究中,16 个基因之间的肿瘤内变异性很小或几乎没有。
解释
我们的研究结果验证了复发评分作为 I-III 期肾透明细胞癌患者临床结局的预测因子,提供了比现有临床和病理参数更准确和个体化的风险评估。
资金来源
基因组健康公司和辉瑞公司。
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