Manley Brandon J, Reznik Ed, Ghanaat Mazyar, Kashan Mahyar, Becerra Maria F, Casuscelli Jozefina, Tennenbaum Daniel, Redzematovic Almedina, Carlo Maria I, Sato Yusuke, Arcila Maria, Voss Martin H, Feldman Darren R, Motzer Robert J, Russo Paul, Coleman Jonathan, Hsieh James J, Hakimi Ari A
Department of Genitourinary Oncology, Moffitt Cancer Center, Tampa, FL.
Department of Medicine, Molecular Oncology, Siteman Cancer Center, Washington University School of Medicine, St. Louis, MO.
Urol Oncol. 2019 Jan;37(1):12-17. doi: 10.1016/j.urolonc.2017.10.012. Epub 2017 Nov 11.
Small renal masses (SRMs) with evidence of clear cell renal cell carcinoma (ccRCC) are understudied. Current algorithms for the management of SRMs include surgical resection, ablation, and active surveillance. We sought to identify genomic biomarkers that could potentially refine the management of ccRCC in SRMs, especially in patients being evaluated for active surveillance.
We identified patients who had SRMs (4cm or less) at time of surgery, had sequencing performed on their primary tumor and had a diagnosis of ccRCC. Patients were selected from 3 publicly available cohorts, The Cancer Genome Atlas (n = 110), University of Tokyo (n = 37), The International Cancer Genome Consortium (n = 31), and from our own institutional prospective database (n = 25). Among this cohort we analyzed mutations present in at least 5% of tumors, assessing for the enrichment of mutations and progression-free survival using the composite endpoint of recurrence or death of disease. Analysis was adjusted for multiple testing. A Cox regression model was used to assess clinical variables with significant mutations.
In total, 203 patients were available for analysis. Median follow-up was 43.1 months among survivors. Mutations in VHL, PBRM1, SETD2, BAP1, KDM5C, and MTOR were present in more than 5% of tumors. Twenty-three patients (11.3%) had recurrence or died of their disease. Mutations in KDM5C were associated with inferior survival from either recurrence or death from disease, adjusted P 0.033.
We identified mutations in SRMs in ccRCC that are associated with recurrence and lethality. The strongest association was seen in those with KDM5C mutations. Use of these genomic biomarkers may improve stratification of patients with SRMs and for those who may be appropriate for active surveillance. Prospective evaluation of these markers is needed.
有透明细胞肾细胞癌(ccRCC)证据的小肾肿块(SRM)研究不足。目前SRM的管理算法包括手术切除、消融和主动监测。我们试图确定基因组生物标志物,以潜在地优化SRM中ccRCC的管理,特别是在接受主动监测评估的患者中。
我们确定了手术时患有SRM(4厘米或更小)、对其原发性肿瘤进行了测序且诊断为ccRCC的患者。患者选自3个公开可用的队列,即癌症基因组图谱(n = 110)、东京大学(n = 37)、国际癌症基因组联盟(n = 31)以及我们自己机构的前瞻性数据库(n = 25)。在这个队列中,我们分析了至少5%的肿瘤中存在的突变,使用疾病复发或死亡的复合终点评估突变的富集情况和无进展生存期。分析针对多重检验进行了调整。使用Cox回归模型评估具有显著突变的临床变量。
总共203名患者可供分析。幸存者的中位随访时间为43.1个月。超过5%的肿瘤中存在VHL、PBRM1、SETD2、BAP1、KDM5C和MTOR的突变。23名患者(11.3%)疾病复发或死亡。KDM5C的突变与疾病复发或死亡导致的较差生存率相关,校正后P值为0.033。
我们在ccRCC的SRM中确定了与复发和致死性相关的突变。在KDM5C突变者中观察到最强的关联。使用这些基因组生物标志物可能会改善SRM患者以及可能适合主动监测的患者的分层。需要对这些标志物进行前瞻性评估。
