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通过尿核基质蛋白22和细胞学检查对膀胱肿瘤复发、分期及分级进行风险分层。

Risk stratification for bladder tumor recurrence, stage and grade by urinary nuclear matrix protein 22 and cytology.

作者信息

Shariat Shahrokh F, Casella Roberto, Wians Frank H, Ashfaq Raheela, Balko Jody, Sulser Tullio, Gasser Thomas C, Sagalowsky Arthur I

机构信息

Department of Urology, University of Texas Southwestern Medical Center, 5323 Harry Hines Boulevard, Dallas, TX 75390-9110, USA.

出版信息

Eur Urol. 2004 Mar;45(3):304-13; author reply 313. doi: 10.1016/j.eururo.2003.10.020.

Abstract

PURPOSE

To test the hypothesis that voided urinary levels of nuclear matrix protein 22 (NMP22) would add to the predictive ability of urine cytology in the diagnosis, staging and grading of bladder transitional cell carcinoma (TCC), and to evaluate the diagnostic performance of different NMP22 cut-points.

MATERIALS

NMP22 level and barbotage cytology were evaluated in voided urine specimens collected before cystoscopy from 302 subjects with a history of TCC, 32 subjects with benign urologic pathologies, and 10 healthy volunteers.

RESULTS

180 patients (52%) had bladder TCC. Higher levels of NMP22 and positive cytology were independently associated with an increased risk of TCC, invasive stage, and high grade. The NMP22 value with equal sensitivity and specificity for prediction of bladder cancer was 6.5U/ml; for prediction of grade 3 TCC it was 13.5U/ml; and for prediction of invasive tumor stage it was 17.4U/ml. The NMP22 cut-point of 6.5U/ml outperformed the 10U/ml cut-point in all pathologic stages and grades. The diagnostic sensitivity of the cytology and NMP22 combined was superior across all pathologic stages and grades to that of either marker alone. NMP22 and cytology stratified patients into groups with significantly different risk for TCC presence, invasive stage, and high grade.

CONCLUSIONS

6.5U/ml is a robust NMP22 cut-point for bladder cancer surveillance. The diagnostic sensitivities of the combined NMP22 and cytology for TCC presence, stage, and grade were significantly higher than those of single marker alone. The combination of urine cytology and NMP22 could be used to tailor the frequency of cystoscopic follow up.

摘要

目的

检验如下假设,即尿核基质蛋白22(NMP22)水平可增强尿液细胞学检查在膀胱移行细胞癌(TCC)诊断、分期及分级中的预测能力,并评估不同NMP22切点的诊断性能。

材料

对302例有TCC病史的患者、32例有良性泌尿系统疾病的患者及10名健康志愿者在膀胱镜检查前收集的晨尿标本进行NMP22水平及冲洗液细胞学检查评估。

结果

180例患者(52%)患有膀胱TCC。NMP22水平升高及细胞学检查阳性与TCC、浸润期及高级别风险增加独立相关。预测膀胱癌时具有同等敏感性和特异性的NMP22值为6.5U/ml;预测3级TCC时为13.5U/ml;预测浸润性肿瘤分期时为17.4U/ml。在所有病理分期和分级中,6.5U/ml的NMP22切点优于10U/ml的切点。在所有病理分期和分级中,细胞学检查与NMP22联合检查的诊断敏感性均优于单一标志物。NMP22和细胞学检查将患者分为TCC存在、浸润期及高级别风险显著不同的组。

结论

6.5U/ml是用于膀胱癌监测的可靠NMP22切点。联合NMP22和细胞学检查对TCC存在、分期及分级的诊断敏感性显著高于单一标志物。尿液细胞学检查与NMP22联合可用于调整膀胱镜随访频率。

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