Genomic profile of urine has high diagnostic sensitivity compared to cytology in non‐invasive urothelial bladder cancer

Hirotsu, Yosuke; Yokoyama, Hitoshi; Amemiya, Kenji; Hagimoto, Takashi; Daimon, Hironori; Hosaka, Kyoko; Oyama, Toshio; Mochizuki, Hitoshi; Omata, Masao

doi:10.1111/cas.14155

Cited by 26 publications

(25 citation statements)

References 38 publications

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“…Recent studies have shown that the concentration of cfDNA in urine is even higher than that in blood. For example, Yosuke et al conducted gene detection tests on urine supernatants, urine precipitate, and blood samples from patients with BC, cystitis, and benign tumors 21 . Half of the somatic mutations present in tumors were detected in urine samples (53% in urine supernatant and 48% in urine precipitate), while 2% were detected in the blood plasma.…”

Section: Components Of Urine Biopsymentioning

confidence: 99%

Urine biopsy technologies: Cancer and beyond

Chen¹,

Liao²,

Li³

et al. 2020

Theranostics

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Since the discovery of circulating tumor cells in 1869, technological advances in the study of biomarkers from liquid biopsy have made it possible to diagnose disease in a less invasive way. Although blood-based liquid biopsy has been used extensively for the detection of solid tumors and immune diseases, the potential of urine-based liquid biopsy has not been fully explored. Advancements in technologies for the harvesting and analysis of biomarkers are providing new opportunities for the characterization of other disease types. Liquid biopsy markers such as exfoliated bladder cancer cells, cell-free DNA (cfDNA), and exosomes have the potential to change the nature of disease management and care, as they allow a cost-effective and convenient mode of patient monitoring throughout treatment. In this review, we addressed the advancement of research in the field of disease detection for the key liquid biopsy markers such as cancer cells, cfDNA, and exosomes, with an emphasis on urine-based liquid biopsy. First, we highlighted key technologies that were widely available and used extensively for clinical urine sample analysis. Next, we presented recent technological developments in cell and genetic research, with implications for the detection of other types of diseases, besides cancer. We then concluded with some discussions on these areas, emphasizing the role of microfluidics and artificial intelligence in advancing point-of-care applications. We believe that the benefits of urine biopsy provide diagnostic development potential, which will pave opportunities for new ways to guide treatment selections and facilitate precision disease therapies.

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Section: Components Of Urine Biopsymentioning

confidence: 99%

Urine biopsy technologies: Cancer and beyond

Chen¹,

Liao²,

Li³

et al. 2020

Theranostics

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“…Besides ctDNA, urothelial tumors have close contact with urine, thus, urinary biomarkers are highly promising as noninvasive tools. Somatic mutations are reliably detected in urinary cell-pellet DNA and cfDNA [75][76][77][78][79][80], and the level of cfDNA in urine supernatants was associated with pathologic features and disease progression, which makes urine tumor DNA have great potential in clinical detection, especially in the early stages of BC [81,82,80,79,83,84]. Current research on the clinical significance of UcfDNA detection for BC is increasing ( Table 2).…”

Section: Ta B L Ementioning

confidence: 99%

“…Increased levels of FGFR3 and Phosphatidylinositol-4,5bisphosphate 3-kinase catalytic subunit alpha (PIK3CA) mutated DNA in urine and plasma are indicative of later progression and metastasis in BC. Hirotsu et al [81] compared detection rates of 71 UC commonly mutated genes in urine supernatants, urine precipitation, and plasma from 25 BC patients and 5 patients with cystitis and benign tumor. The diagnostic sensitivity of the genetic analysis was higher in urine DNA (67%-78%) compared to cfDNA or conventional cytology (22%) in NMIBC.…”

Section: Ta B L Ementioning

confidence: 99%

Tumor heterogeneity and the potential role of liquid biopsy in bladder cancer

Huang

2020

Cancer Communications

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Bladder cancer (BC) is a heterogeneous disease that characterized by genomic instability and a high mutation rate. Heterogeneity in tumor may partially explain the diversity of responses to targeted therapies and the various clinical outcomes. A combination of cytology and cystoscopy is the standard methodology for BC diagnosis, prognosis, and disease surveillance. However, genomics analyses of single tumor-biopsy specimens may underestimate the mutational burden of heterogeneous tumors. Liquid biopsy, as a promising technology, enables analysis of tumor components in the bodily fluids, such as blood and urine, at multiple time points and provides a minimally invasive approach that can track the evolutionary dynamics and monitor tumor heterogeneity. In this review, we describe the multiple faces of BC heterogeneity at the genomic and transcriptional levels and how they affect clinical care and outcomes. We also summarize the outcomes of liquid biopsy in BC, which plays a potential role in revealing tumor heterogeneity. Finally, we discuss the challenges that must be addressed before liquid biopsy can be widely used in clinical treatment.

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“…We searched TCGA data and literature (5,(16)(17)(18)(19)(20)(21)(22) and selected 71 genes related to urological cancer (kidney cancer, prostate cancer, and BC) as described previously (23). A total of 3,652 primer pairs were designed by Ion AmpliSeq Designer contained within this panel (covering 365.34 kb) (23). Library preparation was conducted by amplicon-based multiplex PCR with Ion AmpliSeq Plus Kit (Thermo Fisher Scientific) as described previously (24)(25)(26).…”

Section: Gene Selection and Targeted Sequencingmentioning

confidence: 99%

Genomic Profiling Identified ERCC2 E606Q Mutation in Helicase Domain Respond to Platinum-Based Neoadjuvant Therapy in Urothelial Bladder Cancer

et al. 2020

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Genomic profiling of tumors enables therapeutic decisions, and identifying drugmatched mutations will prolong survival and prognosis. Here, we generated a custom panel for detecting genetic alterations in 19 patients with urothelial bladder cancer. This panel targeted 71 genes associated with urological cancer. Targeted sequencing was performed on formalin-fixed paraffin-embedded tumor tissues. Paired patient-matched tumor and blood samples were subjected to this analysis. A total of 142 somatic mutations were detected in 19 tumor tissues. At least one non-synonymous mutation was detected in all tumor tissues, and KDM6A, KMT2D, TP53, KMT2C, PIK3CA, and ERCC2 were recurrently mutated. Chromatin remodeling and epigenetic modifier genes are frequently mutated. Of 142 mutations, 69 mutations (49%) were annotated to have oncogenic potential. Furthermore, 74% of patients were expected to receive targeted therapy due to drug-matched mutations being identified in their tumors. Among this cohort, a patient harbored an ERCC2 helicase domain mutation and would be expected to respond to platinum-based therapy. As expected, the patient received carboplatin-containing neoadjuvant therapy with a remarkable response. Furthermore, tumor-derived mutations in urine were rapidly decreased after neoadjuvant therapy. These results suggested targeted sequencing could help to detect drug-matched somatic mutations and indicate single or combination therapy for cancer patients.

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Genomic profile of urine has high diagnostic sensitivity compared to cytology in non‐invasive urothelial bladder cancer

Cited by 26 publications

References 38 publications

Urine biopsy technologies: Cancer and beyond

Urine biopsy technologies: Cancer and beyond

Tumor heterogeneity and the potential role of liquid biopsy in bladder cancer

Genomic Profiling Identified ERCC2 E606Q Mutation in Helicase Domain Respond to Platinum-Based Neoadjuvant Therapy in Urothelial Bladder Cancer

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