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Detection of Circulating Tumour Cells in Urothelial Cancers and Clinical Correlations: Comparison of Two Methods

机译:尿路上癌症中循环肿瘤细胞的检测及临床相关性:两种方法的比较

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摘要

Circulating tumour cells (CTC) are identified exploiting their protein/gene expression patterns or distinct size compared to blood cells. Data on CTC in bladder cancer (BC) are still scarce. We comparatively analyzed CTC enrichment by AdnaTest ProstateCancerSelect (AT) and ScreenCell®Cyto (SC) kits, combined with identification by EPCAM, MUC1, and ERBB2 expression and by cytological criteria, respectively, in 19 nonmetastatic (M0) and 47 metastatic (M+) BC patients, at baseline (T0) and during treatment (T1). At T0, CTC positivity rates by AT were higher in M+ compared to M0 cases (57.4% versus 25%, p = 0.041). EPCAM was detected in 75% of CTC-positive samples by AT, showing increasing expression levels from T0 to T1 (median (interquartile range, IQR): 0.18 (0.07–0.42) versus 0.84 (0.33–1.84), p=0.005) in M+ cases. Overall, CTC positivity by SC was around 80% regardless of clinical setting and time point of analysis, except for a lower occurrence at T1 in M0 cases. At T0, circulating tumour microemboli were more frequently (25% versus 8%) detected and more numerous in M+ compared to M0 patients. The approach used for CTC detection impacts the outcome of CTC studies. Further investigations are required to clarify the clinical validity of AT and SC in specific BC clinical contexts.
机译:与血细胞相比,鉴定循环肿瘤细胞(CTC)利用其蛋白质/基因表达模式或明显的大小。膀胱癌(BC)的CTC数据仍然稀缺。我们通过ADNATEST PROSTATECACCERECT(AT)和ScreenCell®Cyto(SC)试剂盒相比分析了CTC富集,与EPCAM,MUC1和ERBB2表达的鉴定和通过细胞学标准,在19个非容性(M0)和47转移(M +)中BC患者,在基线(T0)和治疗期间(T1)。在T0,与M0案例相比,M0 +均匀的CTC阳性率较高(57.4%,P = 0.041)。在75%的CTC阳性样品中检测到EPCAM,显示出从T0至T1的表达水平增加(中值(四分位数范围,IQR):0.18(0.07-0.42)与0.84(0.33-1.84),p = 0.005) M +病例。总体而言,无论临床环境和时间分析,SC的CTC阳性率约为80%,除了在M0案例中较低的T1发生。在T0,与M0患者相比,循环肿瘤微明率更频繁地(25%与8%)检测到,更为多于M +。用于CTC检测的方法会影响CTC研究的结果。需要进一步调查来阐明特定BC临床环境中AT和SC的临床有效性。

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