Batista, Rui and Vinagre, João and Prazeres, Hugo and Sampaio, Cristina and Peralta, Pedro and Conceição, Paulo and Sismeiro, Amílcar and Leão, Ricardo and Gomes, Andreia and Furriel, Frederico and Oliveira, Carlos and Torres, João Nuno and Eufrásio, Pedro and Azinhais, Paulo and Almeida, Fábio and Gonzalez, Edwin Romero and Bidovanets, Bohdan and Ecke, Thorsten and Stinjs, Pascal and Pascual, Álvaro Serrano and Abdelmalek, Rabehi and Villafruela, Ainara and Beardo-Villar, Pastora and Fidalgo, Nuno and Öztürk, Hakan and Gonzalez-Enguita, Carmen and Monzo, Juan and Lopes, Tomé and Álvarez-Maestro, Mario and Servan, Patricia Parra and De La Cruz, Santiago Moreno Perez and Perez, Mario Pual Sanchez and Máximo, Valdemar and Soares, Paula (2019) Validation of a Novel, Sensitive, and Specific Urine-Based Test for Recurrence Surveillance of Patients With Non-Muscle-Invasive Bladder Cancer in a Comprehensive Multicenter Study. Frontiers in Genetics, 10. ISSN 1664-8021
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Abstract
Bladder cancer (BC), the most frequent malignancy of the urinary system, is ranked the sixth most prevalent cancer worldwide. Of all newly diagnosed patients with BC, 70–75% will present disease confined to the mucosa or submucosa, the non-muscle-invasive BC (NMIBC) subtype. Of those, approximately 70% will recur after transurethral resection (TUR). Due to high rate of recurrence, patients are submitted to an intensive follow-up program maintained throughout many years, or even throughout life, resulting in an expensive follow-up, with cystoscopy being the most cost-effective procedure for NMIBC screening. Currently, the gold standard procedure for detection and follow-up of NMIBC is based on the association of cystoscopy and urine cytology. As cystoscopy is a very invasive approach, over the years, many different noninvasive assays (both based in serum and urine samples) have been developed in order to search genetic and protein alterations related to the development, progression, and recurrence of BC. TERT promoter mutations and FGFR3 hotspot mutations are the most frequent somatic alterations in BC and constitute the most reliable biomarkers for BC. Based on these, we developed an ultra-sensitive, urine-based assay called Uromonitor®, capable of detecting trace amounts of TERT promoter (c.1-124C > T and c.1-146C > T) and FGFR3 (p.R248C and p.S249C) hotspot mutations, in tumor cells exfoliated to urine samples. Cells present in urine were concentrated by the filtration of urine through filters where tumor cells are trapped and stored until analysis, presenting long-term stability. Detection of the alterations was achieved through a custom-made, robust, and highly sensitive multiplex competitive allele-specific discrimination PCR allowing clear interpretation of results. In this study, we validate a test for NMIBC recurrence detection, using for technical validation a total of 331 urine samples and 41 formalin-fixed paraffin-embedded tissues of the primary tumor and recurrence lesions from a large cluster of urology centers. In the clinical validation, we used 185 samples to assess sensitivity/specificity in the detection of NMIBC recurrence vs. cystoscopy/cytology and in a smaller cohort its potential as a primary diagnostic tool for NMIBC. Our results show this test to be highly sensitive (73.5%) and specific (93.2%) in detecting recurrence of BC in patients under surveillance of NMIBC.
Item Type: | Article |
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Subjects: | Afro Asian Library > Medical Science |
Depositing User: | Unnamed user with email support@afroasianlibrary.com |
Date Deposited: | 04 Feb 2023 09:04 |
Last Modified: | 31 Jul 2024 13:42 |
URI: | http://classical.academiceprints.com/id/eprint/166 |