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Non-invasive detection of urothelial cancer through the analysis of driver gene mutations and aneuploidy

机译:通过驱动基因突变和非整倍性分析无创检测尿路上皮癌

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Current non-invasive approaches for detection of urothelial cancers are suboptimal. We developed a test to detect urothelial neoplasms using DNA recovered from cells shed into urine. UroSEEK incorporates massive parallel sequencing assays for mutations in 11 genes and copy number changes on 39 chromosome arms. In 570 patients at risk for bladder cancer (BC), UroSEEK was positive in 83% of those who developed BC. Combined with cytology, UroSEEK detected 95% of patients who developed BC. Of 56 patients with upper tract urothelial cancer, 75% tested positive by UroSEEK, including 79% of those with non-invasive tumors. UroSEEK detected genetic abnormalities in 68% of urines obtained from BC patients under surveillance who demonstrated clinical evidence of recurrence. The advantages of UroSEEK over cytology were evident in low-grade BCs; UroSEEK detected 67% of cases whereas cytology detected none. These results establish the foundation for a new non-invasive approach for detection of urothelial cancer.
机译:当前用于检测尿路上皮癌的非侵入性方法是次优的。我们开发了一种检测尿道上皮肿瘤的检测方法,该检测方法是使用从尿液细胞中回收的DNA进行的。 UroSEEK结合了大规模并行测序测定法,用于11个基因的突变和39个染色体臂上的拷贝数变化。在570位有膀胱癌(BC)风险的患者中,UroSEEK在83%的BC患者中呈阳性。结合细胞学检查,UroSEEK检测出95%的患有BC的患者。在56例上尿路尿路上皮癌患者中,有75%的UroSEEK检测为阳性,其中包括79%的非浸润性肿瘤。 UroSEEK在接受监视的BC患者身上发现了68%的尿液遗传异常,这些患者表现出复发的临床证据。在低级BC中,UroSEEK优于细胞学的优势十分明显。 UroSEEK检测到67%的病例,而细胞学检测未见。这些结果为检测尿路上皮癌的新的非侵入性方法奠定了基础。

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