Department of Urology, Erasmus Medical Center, Rotterdam, The Netherlands.
J Urol. 2013 May;189(5):1945-51. doi: 10.1016/j.juro.2012.11.115. Epub 2012 Nov 28.
We determined a combination of markers with optimal sensitivity to detect recurrence in voided urine after resection of an incident low grade, nonmuscle invasive bladder tumor.
A total of 136 patients with G1/G2 nonmuscle invasive bladder tumor were included in the study at transurethral resection of the incident tumor. At least 3 followup urine samples were required for patient selection. DNA was extracted from the incident tumor and cell pellets of subsequently collected urine samples. We performed FGFR3, PIK3CA and RAS mutation analysis, and microsatellite and methylation analysis on tissue and urine DNA samples.
We obtained 716 urine samples. The 136 patients experienced a total of 552 recurrences during a median 3-year followup. Sensitivity for detecting a recurrent tumor varied between 66% and 68% for the molecular tests after patient stratification based on tumor DNA analysis. A combination of markers increased sensitivity but decreased the number of patients eligible for a certain test combination. Combining urine cytology with FGFR3 analysis without stratifying for FGFR3 status of the incident tumor increased sensitivity from 56% to 76%.
A combination of markers increased the percentage of patients eligible for urine based followup and the sensitivity of recurrence detection. Adding FGFR3 analysis to urine cytology could be valuable for noninvasive followup of patients with nonmuscle invasive bladder cancer.
我们确定了一组标记物,以提高检测经尿道切除低级别非肌肉浸润性膀胱肿瘤后尿脱落细胞复发的敏感性。
共纳入 136 例 G1/G2 非肌肉浸润性膀胱肿瘤患者,在经尿道切除肿瘤时进行研究。患者选择需要至少 3 次随访尿样。从肿瘤和随后收集的尿样细胞沉淀中提取 DNA。我们对组织和尿液 DNA 样本进行了 FGFR3、PIK3CA 和 RAS 突变分析,以及微卫星和甲基化分析。
我们获得了 716 个尿样。136 例患者在中位 3 年随访期间共经历了 552 次复发。根据肿瘤 DNA 分析对患者进行分层后,分子检测检测复发肿瘤的敏感性在 66%到 68%之间。标记物的组合增加了敏感性,但减少了符合特定测试组合的患者数量。在不分层 FGFR3 状态的情况下,将尿细胞学与 FGFR3 分析相结合,可将敏感性从 56%提高到 76%。
标记物的组合增加了适合基于尿液的随访的患者比例,并提高了复发检测的敏感性。将 FGFR3 分析添加到尿细胞学中可能对非肌肉浸润性膀胱癌患者的非侵入性随访有价值。
