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1. An integrated multi-omics analysis identifies prognostic molecular subtypes of non-muscle-invasive bladder cancer

Author

Lindskrog, Sia Viborg, Prip, Frederik, Lamy, Philippe, Taber, Ann, Groeneveld, Clarice S., Birkenkamp-Demtröder, Karin, Jensen, Jørgen Bjerggaard, Strandgaard, Trine, Nordentoft, Iver, Christensen, Emil, Sokac, Mateo, Birkbak, Nicolai J., Maretty, Lasse, Hermann, Gregers G., Petersen, Astrid C., Weyerer, Veronika, Grimm, Marc-Oliver, Horstmann, Marcus, Sjödahl, Gottfrid, Höglund, Mattias, Steiniche, Torben, Mogensen, Karin, de Reyniès, Aurélien, Nawroth, Roman, Jordan, Brian, Lin, Xiaoqi, Dragicevic, Dejan, Ward, Douglas G., Goel, Anshita, Hurst, Carolyn D., Raman, Jay D., Warrick, Joshua I., Segersten, Ulrika, Sikic, Danijel, van Kessel, Kim E. M., Maurer, Tobias, Meeks, Joshua J., DeGraff, David J., Bryan, Richard T., Knowles, Margaret A., Simic, Tatjana, Hartmann, Arndt, Zwarthoff, Ellen C., Malmström, Per-Uno, Malats, Núria, Real, Francisco X., and Dyrskjøt, Lars

Published
2021
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2. Abstract 6075: Comprehensive genomic characterization of early-stage bladder cancer from 438 patients by whole genome- and exome sequencing

Author

Prip, Frederik, primary, Lamy, Philippe, additional, Nordentoft, Iver, additional, Lindskrog, Sia Viborg, additional, Strandgaard, Trine, additional, Birkenkamp-Demtröder, Karin, additional, Hermann, Gregers G., additional, Petersen, Astrid C., additional, Bahlinger, Veronika, additional, Grimm, Marc-Oliver, additional, Horstmann, Marcus, additional, Mogensen, Karin, additional, Nawroth, Roman, additional, Segersten, Ulrika, additional, Sikic, Danijel, additional, van Kessel, Kim E. M, additional, Maurer, Tobias, additional, Simic, Tatjana, additional, Hartmann, Arndt, additional, Zwarthoff, Ellen C. C., additional, Malmström, Per-Uno, additional, Steiniche, Torben, additional, Jensen, Jørgen Bjerggaard, additional, Malats, Núria, additional, Real, Francisco X., additional, and Dyrskjøt, Lars, additional

Published
2023
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3. Long non-coding RNAs identify a subset of luminal muscle-invasive bladder cancer patients with favorable prognosis

Author

de Jong, Joep J., Liu, Yang, Robertson, A. Gordon, Seiler, Roland, Groeneveld, Clarice S., van der Heijden, Michiel S., Wright, Jonathan L., Douglas, James, Dall’Era, Marc, Crabb, Simon J., van Rhijn, Bas W. G., van Kessel, Kim E. M., Davicioni, Elai, Castro, Mauro A. A., Lotan, Yair, Zwarthoff, Ellen C., Black, Peter C., Boormans, Joost L., and Gibb, Ewan A.

Published
2019
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5. Using Decision Analysis to Model Cancer Surveillance

Author

van Kessel, Kim E. M., Geurts, Sandra M. E., Verbeek, André L. M., Steyerberg, Ewout W., Johnson, Frank E., editor, Maehara, Yoshihiko, editor, Browman, George P., editor, Margenthaler, Julie A., editor, Audisio, Riccardo A., editor, Thompson, John F., editor, Johnson, David Y., editor, Earle, Craig C., editor, and Virgo, Katherine S., editor

Published
2013
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7. An integrated multi-omics analysis identifies prognostic molecular subtypes of non-muscle-invasive bladder cancer

Author

Viborg Lindskrog, Sia, Prip, Frederik, Lamy, Philippe, Taber, Ann, Groeneveld, Clarice S., Birkenkamp-Demtröder, Karin, Bjerggaard Jensen, Jørgen, Strandgaard, Trine, Nordentoft, Iver, Christensen, Emil, Sokac, Mateo, Birkbak, Nicolai J., Maretty, Lasse, Hermann, Gregers G., Petersen, Astrid C., Weyerer, Veronika, Grimm, Marc-Oliver, Horstmann, Marcus, Sjödahl, Gottfrid, Höglund, Mattias, Steiniche, Torben, Mogensen, Karin, de Reyniès, Aurélien, Nawroth, Roman, Jordan, Brian, Lin, Xiaoqi, Dragicevic, Dejan, Ward, Douglas G., Goel, Anshita, Hurst, Carolyn D., Raman, Jay D., Warrick, Joshua I., Segersten, Ulrika, Sikic, Danijel, van Kessel, Kim E. M., Maurer, Tobias, Meeks, Joshua J., DeGraff, David J., Bryan, Richard T., Knowles, Margaret A., Simic, Tatjana, Hartmann, Arndt, Zwarthoff, Ellen C., Malmström, Per-Uno, Malats, Núria, Real, Francisco X., Dyrskjøt, Lars, Viborg Lindskrog, Sia, Prip, Frederik, Lamy, Philippe, Taber, Ann, Groeneveld, Clarice S., Birkenkamp-Demtröder, Karin, Bjerggaard Jensen, Jørgen, Strandgaard, Trine, Nordentoft, Iver, Christensen, Emil, Sokac, Mateo, Birkbak, Nicolai J., Maretty, Lasse, Hermann, Gregers G., Petersen, Astrid C., Weyerer, Veronika, Grimm, Marc-Oliver, Horstmann, Marcus, Sjödahl, Gottfrid, Höglund, Mattias, Steiniche, Torben, Mogensen, Karin, de Reyniès, Aurélien, Nawroth, Roman, Jordan, Brian, Lin, Xiaoqi, Dragicevic, Dejan, Ward, Douglas G., Goel, Anshita, Hurst, Carolyn D., Raman, Jay D., Warrick, Joshua I., Segersten, Ulrika, Sikic, Danijel, van Kessel, Kim E. M., Maurer, Tobias, Meeks, Joshua J., DeGraff, David J., Bryan, Richard T., Knowles, Margaret A., Simic, Tatjana, Hartmann, Arndt, Zwarthoff, Ellen C., Malmström, Per-Uno, Malats, Núria, Real, Francisco X., and Dyrskjøt, Lars

Abstract

The molecular landscape in non-muscle-invasive bladder cancer (NMIBC) is characterized by large biological heterogeneity with variable clinical outcomes. Here, we perform an integrative multi-omics analysis of patients diagnosed with NMIBC (n=834). Transcriptomic analysis identifies four classes (1, 2a, 2b and 3) reflecting tumor biology and disease aggressiveness. Both transcriptome-based subtyping and the level of chromosomal instability provide independent prognostic value beyond established prognostic clinicopathological parameters. High chromosomal instability, p53-pathway disruption and APOBEC-related mutations are significantly associated with transcriptomic class 2a and poor outcome. RNA-derived immune cell infiltration is associated with chromosomally unstable tumors and enriched in class 2b. Spatial proteomics analysis confirms the higher infiltration of class 2b tumors and demonstrates an association between higher immune cell infiltration and lower recurrence rates. Finally, the independent prognostic value of the transcriptomic classes is documented in 1228 validation samples using a single sample classification tool. The classifier provides a framework for biomarker discovery and for optimizing treatment and surveillance in next-generation clinical trials.

Published
2021
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8. Evaluation of the New American Urological Association Guidelines Risk Classification for Hematuria

Author

Woldu, Solomon L., primary, Ng, Casey K., additional, Loo, Ronald K., additional, Slezak, Jeff M., additional, Jacobsen, Steven J., additional, Tan, Wei Shen, additional, Kelly, John D., additional, Lough, Tony, additional, Darling, David, additional, van Kessel, Kim E. M., additional, de Jong, Joep J., additional, van Criekinge, Wim, additional, Shariat, Shahrokh F., additional, Hiar, Andrew, additional, Brown, Sarah, additional, Boorjian, Stephen A., additional, Barocas, Daniel A., additional, Svatek, Robert S., additional, and Lotan, Yair, additional

Published
2021
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10. Reply by Authors

Author

van Kessel, Kim E. M., primary, de Jong, Joep J., additional, Ziel-van der Made, Angelique C. J., additional, Roshani, Hossain, additional, Haensel, Stefan M., additional, Wolterbeek, Josien H., additional, Boevé, Egbert R., additional, Oomens, Eric H. G. M., additional, van Casteren, Niels J., additional, Krispin, Manuel, additional, Boormans, Joost L., additional, Steyerberg, Ewout W., additional, van Criekinge, Wim, additional, and Zwarthoff, Ellen C., additional

Published
2020
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11. A Urine Based Genomic Assay to Triage Patients with Hematuria for Cystoscopy

Author

van Kessel, Kim E. M., primary, de Jong, Joep J., additional, Ziel-van der Made, Angelique C. J., additional, Roshani, Hossain, additional, Haensel, Stefan M., additional, Wolterbeek, Josien H., additional, Boevé, Egbert R., additional, Oomens, Eric H. G. M., additional, van Casteren, Niels J., additional, Krispin, Manuel, additional, Boormans, Joost L., additional, Steyerberg, Ewout W., additional, van Criekinge, Wim, additional, and Zwarthoff, Ellen C., additional

Published
2020
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13. Molecular Markers Increase Precision of the European Association of Urology Non-Muscle-Invasive Bladder Cancer Progression Risk Groups

Author

van Kessel, Kim E. M., van der Keur, Kirstin A., Dyrskjot, Lars, Algaba, Ferran, Welvaart, Naeromy Y. C., Beukers, Willemien, Segersten, Ulrika, Keck, Bastian, Maurer, Tobias, Simic, Tatjana, Horstmann, Marcus, Grimm, Marc-Oliver, Hermann, Gregers G., Mogensen, Karin, Hartmann, Arndt, Harving, Niels, Petersen, Astrid C., Jensen, Jorgen B., Junker, Kerstin, Boormans, Joost L., Real, Francisco X., Malats, Nuria, Malmström, Per-Uno, Orntoft, Torben F., Zwarthoff, Ellen C., van Kessel, Kim E. M., van der Keur, Kirstin A., Dyrskjot, Lars, Algaba, Ferran, Welvaart, Naeromy Y. C., Beukers, Willemien, Segersten, Ulrika, Keck, Bastian, Maurer, Tobias, Simic, Tatjana, Horstmann, Marcus, Grimm, Marc-Oliver, Hermann, Gregers G., Mogensen, Karin, Hartmann, Arndt, Harving, Niels, Petersen, Astrid C., Jensen, Jorgen B., Junker, Kerstin, Boormans, Joost L., Real, Francisco X., Malats, Nuria, Malmström, Per-Uno, Orntoft, Torben F., and Zwarthoff, Ellen C.

Abstract

Purpose: The European Association of Urology (EAU) guidelines for non-muscle-invasive bladder cancer (NMIBC) recommend risk stratification based on clinicopathologic parameters. Our aim was to investigate the added value of biomarkers to improve risk stratification of NMIBC. Experimental Design: We prospectively included 1,239 patients in follow-up for NMIBC in six European countries. Fresh-frozen tumor samples were analyzed for GATA2, TBX2, TBX3, and ZIC4 methylation and FGFR3, TERT, PIK3CA, and RAS mutation status. Cox regression analyses identified markers that were significantly associated with progression to muscle-invasive disease. The progression incidence rate (PIR = rate of progression per 100 patient-years) was calculated for subgroups. Results: In our cohort, 276 patients had a low, 273 an intermediate, and 555 a high risk of tumor progression based on the EAU NMIBC guideline. Fifty-seven patients (4.6%) progressed to muscle-invasive disease. The limited number of progressors in this large cohort compared with older studies is likely due to improved treatment in the past two decades. Overall, wild-type FGFR3 and methylation of GATA2 and TBX3 were significantly associated with progression (HR = 0.34, 2.53, and 2.64, respectively). The PIR for EAU high-risk patients was 4.25. On the basis of FGFR3 mutation status and methylation of GATA2, this cohort could be reclassified into a good class (PIR = 0.86, 26.2% of patients), a moderate class (PIR = 4.32, 49.7%), and a poor class (PIR = 7.66, 24.0%). Conclusions: We conclude that the addition of selected biomarkers to the EAU risk stratification increases its accuracy and identifies a subset of NMIBC patients with a very high risk of progression. (C) 2018 AACR.

Published
2018
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14. Validation of a DNA Methylation-Mutation Urine Assay to Select Patients with Hematuria for Cystoscopy

Author

van Kessel, Kim E. M., Beukers, Willemien, Lurkin, Irene, Ziel-van der Made, Angelique, van der Keur, Kirstin A., Boormans, Joost L., Dyrskjot, Lars, Marquez, Mirari, Orntoft, Torben F., Real, Francisco X., Segersten, Ulrika, Malats, Nuria, Malmström, Per-Uno, Van Criekinge, Wim, Zwarthoff, Ellen C., van Kessel, Kim E. M., Beukers, Willemien, Lurkin, Irene, Ziel-van der Made, Angelique, van der Keur, Kirstin A., Boormans, Joost L., Dyrskjot, Lars, Marquez, Mirari, Orntoft, Torben F., Real, Francisco X., Segersten, Ulrika, Malats, Nuria, Malmström, Per-Uno, Van Criekinge, Wim, and Zwarthoff, Ellen C.

Abstract

Purpose: Only 3% to 28% of patients referred to the urology clinic for hematuria are diagnosed with bladder cancer. Cystoscopy leads to high diagnostic costs and a high patient burden. Therefore, to improve the selection of patients for cystoscopy and reduce costs and over testing we aimed to validate a recently developed diagnostic urine assay. Materials and Methods: Included in study were 200 patients from a total of 3 European countries who underwent cystoscopy for hematuria, including 97 with bladder cancer and 103 with nonmalignant findings. Voided urine samples were collected prior to cystoscopy. DNA was extracted and analyzed for mutations in FGFR3, TERT and HRAS, and methylation of OTX1, ONECUT2 and TWIST1. Logistic regression was used to analyze the association between predictor variables and bladder cancer. Results: Combining the methylation and mutation markers with age led to an AUC of 0.96 (95% CI 0.92e0.99) with 93% sensitivity and 86% specificity, and an optimism corrected AUC of 0.95. The AUC was higher for T1 or greater tumors compared to Ta tumors (0.99 vs 0.93). The AUC was also higher for high grade tumors compared to low grade tumors (1.00 vs 0.93). Overall negative predictive value was 99% based on the 5% to 10% prevalence of bladder cancer in patients with hematuria. This would lead to a 77% reduction in diagnostic cystoscopy. Conclusions: Analyzing hematuria patients for the risk of bladder cancer using novel molecular markers may lead to a reduction in diagnostic cystoscopy. Combining methylation analysis (OTX1, ONECUT2 and TWIST1) with mutation analysis (FGFR3, TERT and HRAS) and patient age resulted in a validated accurate prediction model.

Published
2017
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16. Comprehensive Transcriptional Analysis of Early-Stage Urothelial Carcinoma

Author

Hedegaard, Jakob, Lamy, Philippe, Nordentoft, Iver, Algaba, Ferran, Hoyer, Soren, Ulhoi, Benedicte Parm, Vang, Soren, Reinert, Thomas, Hermann, Gregers G., Mogensen, Karin, Thomsen, Mathilde Borg Houlberg, Nielsen, Morten Muhlig, Marquez, Mirari, Segersten, Ulrika, Aine, Mattias, Hoglund, Mattias, Birkenkamp-Demtroder, Karin, Fristrup, Niels, Borre, Michael, Hartmann, Arndt, Stoehr, Robert, Wach, Sven, Keck, Bastian, Seitz, Anna Katharina, Nawroth, Roman, Maurer, Tobias, Tulic, Cane, Simic, Tatjana, Junker, Kerstin, Horstmann, Marcus, Harving, Niels, Petersen, Astrid Christine, Luz Calle, M., Steyerberg, Ewout W., Beukers, Willemien, van Kessel, Kim E. M., Jensen, Jorgen Bjerggaard, Pedersen, Jakob Skou, Malmström, Per-Uno, Malats, Nuria, Real, Francisco X., Zwarthoff, Ellen C., Orntoft, Torben Falck, Dyrskjot, Lars, Hedegaard, Jakob, Lamy, Philippe, Nordentoft, Iver, Algaba, Ferran, Hoyer, Soren, Ulhoi, Benedicte Parm, Vang, Soren, Reinert, Thomas, Hermann, Gregers G., Mogensen, Karin, Thomsen, Mathilde Borg Houlberg, Nielsen, Morten Muhlig, Marquez, Mirari, Segersten, Ulrika, Aine, Mattias, Hoglund, Mattias, Birkenkamp-Demtroder, Karin, Fristrup, Niels, Borre, Michael, Hartmann, Arndt, Stoehr, Robert, Wach, Sven, Keck, Bastian, Seitz, Anna Katharina, Nawroth, Roman, Maurer, Tobias, Tulic, Cane, Simic, Tatjana, Junker, Kerstin, Horstmann, Marcus, Harving, Niels, Petersen, Astrid Christine, Luz Calle, M., Steyerberg, Ewout W., Beukers, Willemien, van Kessel, Kim E. M., Jensen, Jorgen Bjerggaard, Pedersen, Jakob Skou, Malmström, Per-Uno, Malats, Nuria, Real, Francisco X., Zwarthoff, Ellen C., Orntoft, Torben Falck, and Dyrskjot, Lars

Abstract

Non-muscle-invasive bladder cancer (NMIBC) is a heterogeneous disease with widely different outcomes. We performed a comprehensive transcriptional analysis of 460 early-stage urothelial carcinomas and showed that NMIBC can be subgrouped into three major classes with basal-and luminal-like characteristics and different clinical outcomes. Large differences in biological processes such as the cell cycle, epithelial-mesenchymal transition, and differentiation were observed. Analysis of transcript variants revealed frequent mutations in genes encoding proteins involved in chromatin organization and cytoskeletal functions. Furthermore, mutations in well-known cancer driver genes (e.g., TP53 and ERBB2) were primarily found in high-risk tumors, together with APOBEC-related mutational signatures. The identification of subclasses in NMIBC may offer better prognostication and treatment selection based on subclass assignment.

Published
2016
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17. A urine based assay to select patients for initial cystoscopy

Author

van Kessel, Kim E. M., Beukers, Willemien, Lurkin, Irene, van der Keur, Kirstin A., Dyrskjot, Lars, Segersten, Ulrika, Orntoft, Torben F., Malats, Nuria, Malmstrom, Per-Uno, Real, Francisco X., Bangma, Chris H., Zwarthoff, Ellen C., van Kessel, Kim E. M., Beukers, Willemien, Lurkin, Irene, van der Keur, Kirstin A., Dyrskjot, Lars, Segersten, Ulrika, Orntoft, Torben F., Malats, Nuria, Malmstrom, Per-Uno, Real, Francisco X., Bangma, Chris H., and Zwarthoff, Ellen C.

Abstract

Meeting Abstract: 549

Published
2015
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19. Assessment of Predictive Genomic Biomarkers for Response to Cisplatin-based Neoadjuvant Chemotherapy in Bladder Cancer.

Author

Gil-Jimenez A, van Dorp J, Contreras-Sanz A, van der Vos K, Vis DJ, Braaf L, Broeks A, Kerkhoven R, van Kessel KEM, Ribal MJ, Alcaraz A, Wessels LFA, Seiler R, Wright JL, Mengual L, Boormans J, van Rhijn BWG, Black PC, and van der Heijden MS

Subjects
Humans, Neoadjuvant Therapy, Retrospective Studies, Biomarkers, Tumor genetics, Cystectomy, Genomics, Neoplasm Invasiveness, Xeroderma Pigmentosum Group D Protein, Cisplatin, Urinary Bladder Neoplasms pathology
Abstract

Cisplatin-based neoadjuvant chemotherapy (NAC) followed by radical cystectomy is recommended for patients with muscle-invasive bladder cancer (MIBC). It has been shown that somatic deleterious mutations in ERCC2, gain-of-function mutations in ERBB2, and alterations in ATM, RB1, and FANCC are correlated with pathological response to NAC in MIBC. The objective of this study was to validate these genomic biomarkers in pretreatment transurethral resection material from an independent retrospective cohort of 165 patients with MIBC who subsequently underwent NAC and radical surgery. Patients with ypT0/Tis/Ta/T1N0 disease after surgery were defined as responders. Somatic deleterious mutations in ERCC2 were found in nine of 68 (13%) evaluable responders and two of 95 (2%) evaluable nonresponders (p = 0.009; FDR = 0.03). No correlation was observed between response and alterations in ERBB2 or in ATM, RB1, or FANCC alone or in combination. In an exploratory analysis, no additional genomic alterations discriminated between responders and nonresponders to NAC. No further associations were identified between the aforementioned biomarkers and pathological complete response (ypT0N0) after surgery. In conclusion, we observed a positive association between deleterious mutations in ERCC2 and pathological response to NAC, but not overall survival or recurrence-free survival. Other previously reported genomic biomarkers were not validated. PATIENT SUMMARY: It is currently unknown which patients will respond to chemotherapy before definitive surgery for bladder cancer. Previous studies described several gene mutations in bladder cancer that correlated with chemotherapy response. This study confirmed that patients with bladder cancer with a mutation in the ERCC2 gene often respond to chemotherapy., (Copyright © 2022 European Association of Urology. Published by Elsevier B.V. All rights reserved.)

Published
2023
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20. A Urine-based Genomic Assay Improves Risk Stratification for Patients with High-risk Hematuria Stratified According to the American Urological Association Guidelines.

Author

de Jong JJ, Pijpers OM, van Kessel KEM, Boormans JL, Van Criekinge W, Zwarthoff EC, and Lotan Y

Subjects
Humans, Hematuria diagnosis, Hematuria genetics, Hematuria epidemiology, Prospective Studies, Biomarkers, Tumor genetics, Genomics, Risk Assessment, Transcription Factors, Homeodomain Proteins, Otx Transcription Factors, Urinary Bladder Neoplasms diagnosis, Urinary Bladder Neoplasms genetics, Urinary Bladder Neoplasms complications, Carcinoma, Transitional Cell
Abstract

Background: According to the recent American Urological Association (AUA) guideline on hematuria, patients are stratified into groups with low, intermediate, and high risk of urothelial carcinoma (UC). These risk groups are based on clinical factors and do not incorporate urine-based tumor markers., Objective: To evaluate whether a urine-based genomic assay improves the redefined AUA risk stratification for hematuria., Design, Setting, and Participants: We selected patients with complete biomarker status, as assessed on urinary DNA, from a previously collected prospective Dutch hematuria cohort (n = 838). Patients were stratified into the AUA risk categories on the basis of sex, age, and type of hematuria. Biomarker status included mutation status for the FGFR3, TERT, and HRAS genes, and methylation status for the OTX1, ONECUT2, and TWIST1 genes., Outcome Measurements and Statistical Analysis: The primary endpoint was the diagnostic model performance for different hematuria risk groups. Further analyses assessed the pretest and post-test UC probability in the hematuria subgroups using a Fagan nomogram., Results and Limitations: Overall, 65 patients (7.8%) were classified as low risk, 106 (12.6%) as intermediate risk, and 667 (79.6%) as high risk. The UC incidence differed significantly between the gross hematuria (21%, 98/457) and microscopic hematuria (4%, 14/381) groups (p < 0.001). All cancer cases were in the high-risk group, which had UC incidence of 16.8% (112/667). Application of the diagnostic model revealed robust performance among all risk groups (area under the receiver operating characteristic curve 0.929-0.971). Depending on the risk group evaluated, a negative urine assay was associated with post-test UC probability of 0.3-2%, whereas a positive urine assay was associated with post-test UC probability of 31-42%., Conclusions: This study shows the value that a urine-based genomic assay adds to the AUA guideline stratification for patients with hematuria. It seems justified to safely withhold cystoscopy for patients with AUA low risk who have a negative urine assay. In addition, evaluation should be expedited for patients with AUA intermediate or high risk and a positive urine assay., Patient Summary: Patients who have blood in their urine (hematuria) can be classified as having low, intermediate, or high risk of having cancer in their urinary tract. We found that use of a urine-based genetic test improves the accuracy of predicting which patients are most likely to have cancer. Patients with a negative test may be able to avoid invasive tests, while further tests could be prioritized for patients with a positive test., (Copyright © 2022. Published by Elsevier B.V.)

Published
2023
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21. Recommendations for follow-up of muscle-invasive bladder cancer patients: A consensus by the international bladder cancer network.

Author

Zuiverloon TCM, van Kessel KEM, Bivalacqua TJ, Boormans JL, Ecke TH, Grivas PD, Kiltie AE, Liedberg F, Necchi A, van Rhijn BW, Roghmann F, Sanchez-Carbayo M, Schmitz-Dräger BJ, Wezel F, and Kamat AM

Subjects
Consensus, Disease Management, Female, Humans, Male, Urinary Bladder Neoplasms pathology, Follow-Up Studies, Urinary Bladder Neoplasms therapy
Abstract

Rationale: Several guidelines exist that address treatment of patients with nonmetastatic muscle-invasive bladder cancer (MIBC). However, most only briefly mention follow-up strategies for patients and hence the treating physician is often left to infer on what the preferred follow-up schema would be for an individual patient. Herein, we aim to synthesize recommendations for follow-up of patients with MIBC for easy reference., Methods: A multidisciplinary MIBC expert panel from the International Bladder Cancer Network was assembled to critically assess currently available major guidelines on surveillance of MIBC patients. Recommendations for follow-up were extracted and critically evaluated. Important considerations for guideline assessment included both aspects of oncological and functional follow-up-frequency of visits, the use of different imaging modalities, the role of cytology and molecular markers, and the duration of follow-up., Outcome: An International Bladder Cancer Network expert consensus recommendation was constructed for the follow-up of patients with MIBC based on the currently available evidence-based data., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published
2018
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22. Molecular Markers Increase Precision of the European Association of Urology Non-Muscle-Invasive Bladder Cancer Progression Risk Groups.

Author

van Kessel KEM, van der Keur KA, Dyrskjøt L, Algaba F, Welvaart NYC, Beukers W, Segersten U, Keck B, Maurer T, Simic T, Horstmann M, Grimm MO, Hermann GG, Mogensen K, Hartmann A, Harving N, Petersen AC, Jensen JB, Junker K, Boormans JL, Real FX, Malats N, Malmström PU, Ørntoft TF, and Zwarthoff EC

Subjects
Adult, Aged, Aged, 80 and over, Biomarkers, Tumor genetics, Disease Progression, Europe, Female, GATA2 Transcription Factor genetics, GATA2 Transcription Factor metabolism, Humans, Male, Middle Aged, Mutation genetics, Neoplasm Invasiveness genetics, Prospective Studies, Receptor, Fibroblast Growth Factor, Type 3 genetics, Receptor, Fibroblast Growth Factor, Type 3 metabolism, Risk Factors, Urinary Bladder Neoplasms genetics, Urology methods, Young Adult, Biomarkers, Tumor metabolism, Neoplasm Invasiveness pathology, Urinary Bladder Neoplasms metabolism, Urinary Bladder Neoplasms pathology
Abstract

Purpose: The European Association of Urology (EAU) guidelines for non-muscle-invasive bladder cancer (NMIBC) recommend risk stratification based on clinicopathologic parameters. Our aim was to investigate the added value of biomarkers to improve risk stratification of NMIBC. Experimental Design: We prospectively included 1,239 patients in follow-up for NMIBC in six European countries. Fresh-frozen tumor samples were analyzed for GATA2, TBX2, TBX3 , and ZIC4 methylation and FGFR3, TERT, PIK3CA , and RAS mutation status. Cox regression analyses identified markers that were significantly associated with progression to muscle-invasive disease. The progression incidence rate (PIR = rate of progression per 100 patient-years) was calculated for subgroups. Results: In our cohort, 276 patients had a low, 273 an intermediate, and 555 a high risk of tumor progression based on the EAU NMIBC guideline. Fifty-seven patients (4.6%) progressed to muscle-invasive disease. The limited number of progressors in this large cohort compared with older studies is likely due to improved treatment in the past two decades. Overall, wild-type FGFR3 and methylation of GATA2 and TBX3 were significantly associated with progression (HR = 0.34, 2.53, and 2.64, respectively). The PIR for EAU high-risk patients was 4.25. On the basis of FGFR3 mutation status and methylation of GATA2 , this cohort could be reclassified into a good class (PIR = 0.86, 26.2% of patients), a moderate class (PIR = 4.32, 49.7%), and a poor class (PIR = 7.66, 24.0%). Conclusions: We conclude that the addition of selected biomarkers to the EAU risk stratification increases its accuracy and identifies a subset of NMIBC patients with a very high risk of progression. Clin Cancer Res; 24(7); 1586-93. ©2018 AACR ., (©2018 American Association for Cancer Research.)

Published
2018
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23. Validation of a DNA Methylation-Mutation Urine Assay to Select Patients with Hematuria for Cystoscopy.

Author

van Kessel KE, Beukers W, Lurkin I, Ziel-van der Made A, van der Keur KA, Boormans JL, Dyrskjøt L, Márquez M, Ørntoft TF, Real FX, Segersten U, Malats N, Malmström PU, Van Criekinge W, and Zwarthoff EC

Subjects
Adult, Aged, Aged, 80 and over, Diagnostic Tests, Routine, Female, Humans, Male, Middle Aged, Neoplasm Grading, Netherlands, Patient Selection, Predictive Value of Tests, Prospective Studies, Sensitivity and Specificity, Spain, Sweden, Biomarkers, Tumor genetics, Biomarkers, Tumor urine, Cystoscopy, DNA Methylation, DNA Mutational Analysis, Hematuria genetics, Hematuria urine, Urinary Bladder Neoplasms genetics, Urinary Bladder Neoplasms urine
Abstract

Purpose: Only 3% to 28% of patients referred to the urology clinic for hematuria are diagnosed with bladder cancer. Cystoscopy leads to high diagnostic costs and a high patient burden. Therefore, to improve the selection of patients for cystoscopy and reduce costs and over testing we aimed to validate a recently developed diagnostic urine assay., Materials and Methods: Included in study were 200 patients from a total of 3 European countries who underwent cystoscopy for hematuria, including 97 with bladder cancer and 103 with nonmalignant findings. Voided urine samples were collected prior to cystoscopy. DNA was extracted and analyzed for mutations in FGFR3, TERT and HRAS, and methylation of OTX1, ONECUT2 and TWIST1. Logistic regression was used to analyze the association between predictor variables and bladder cancer., Results: Combining the methylation and mutation markers with age led to an AUC of 0.96 (95% CI 0.92-0.99) with 93% sensitivity and 86% specificity, and an optimism corrected AUC of 0.95. The AUC was higher for T1 or greater tumors compared to Ta tumors (0.99 vs 0.93). The AUC was also higher for high grade tumors compared to low grade tumors (1.00 vs 0.93). Overall negative predictive value was 99% based on the 5% to 10% prevalence of bladder cancer in patients with hematuria. This would lead to a 77% reduction in diagnostic cystoscopy., Conclusions: Analyzing hematuria patients for the risk of bladder cancer using novel molecular markers may lead to a reduction in diagnostic cystoscopy. Combining methylation analysis (OTX1, ONECUT2 and TWIST1) with mutation analysis (FGFR3, TERT and HRAS) and patient age resulted in a validated accurate prediction model., (Copyright © 2017 American Urological Association Education and Research, Inc. Published by Elsevier Inc. All rights reserved.)

Published
2017
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24. Elevated Derived Neutrophil-to-Lymphocyte Ratio Corresponds With Poor Outcome in Patients Undergoing Pre-Operative Chemotherapy in Muscle-Invasive Bladder Cancer.

Author

van Kessel KE, de Haan LM, Fransen van de Putte EE, van Rhijn BW, de Wit R, van der Heijden MS, Zwarthoff EC, and Boormans JL

Abstract

Background: Platinum-based pre-operative chemotherapy (POC) for muscle-invasive bladder cancer (MIBC) increases the complete pathological response rate at cystectomy and improves overall survival. However, 60% of MIBC patients still has muscle-invasive disease at cystectomy despite POC. Therefore, accurate prediction of response to POC is an important clinical need. We hypothesized that an elevated neutrophil-to-lymphocyte ratio (NLR) corresponds with adverse outcome in patients undergoing POC and radical cystectomy. Objective: To explore the correlation between the NLR and outcome in MIBC patients treated by POC and radical cystectomy. Methods: In 123 MIBC patients (urothelial carcinoma) who were treated by platinum-based POC and radical cystectomy, the derived NLR (dNLR) was retrospectively calculated by dividing the neutrophil count by the difference between leukocytes and neutrophil counts, prior to the start of chemotherapy. The correlation of the dNLR with pathological response at cystectomy and survival was analyzed by logistic regression analysis or the Kaplan-Meier method. Results: The complete pathological response (ypT0N0Mx) rate was 28.5%, 8.9% obtained a partial response (ypTa/T1/TisN0Mx), and 62.6% were non-responders (stage ≥ ypT2 and/or N+). An elevated dNLR (>2.21) correlated with non-response to POC (OR 2.70, 95% confidence interval: 1.15-6.38, p  = 0.02) but this effect was nullified when corrected for clinically node-positive disease and clinical T stage. Patients with an elevated dNLR had shorter progression-free and overall survival albeit non-significant ( p  = 0.42, and p  = 0.45, respectively). Conclusions: An elevated dNLR corresponded with poor outcome in terms of survival and non-response to POC in MIBC patients undergoing radical surgery. However, after correction for well-known prognostic factors, such as positive lymph node status at diagnostic imaging and clinical T stage, the correlation for the dNLR was nullified. Therefore, we conclude that the dNLR is insufficient to predict response to POC in this heterogeneous patient population.

Published
2016
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25. Comprehensive Transcriptional Analysis of Early-Stage Urothelial Carcinoma.

Author

Hedegaard J, Lamy P, Nordentoft I, Algaba F, Høyer S, Ulhøi BP, Vang S, Reinert T, Hermann GG, Mogensen K, Thomsen MBH, Nielsen MM, Marquez M, Segersten U, Aine M, Höglund M, Birkenkamp-Demtröder K, Fristrup N, Borre M, Hartmann A, Stöhr R, Wach S, Keck B, Seitz AK, Nawroth R, Maurer T, Tulic C, Simic T, Junker K, Horstmann M, Harving N, Petersen AC, Calle ML, Steyerberg EW, Beukers W, van Kessel KEM, Jensen JB, Pedersen JS, Malmström PU, Malats N, Real FX, Zwarthoff EC, Ørntoft TF, and Dyrskjøt L

Subjects
APOBEC Deaminases genetics, Cluster Analysis, Female, Gene Expression Regulation, Neoplastic, Genetic Predisposition to Disease, Humans, Male, Neoplasm Staging, RNA, Long Noncoding genetics, Survival Analysis, Biomarkers, Tumor genetics, Gene Expression Profiling methods, Mutation, Sequence Analysis, RNA methods, Urinary Bladder Neoplasms genetics, Urinary Bladder Neoplasms pathology
Abstract

Non-muscle-invasive bladder cancer (NMIBC) is a heterogeneous disease with widely different outcomes. We performed a comprehensive transcriptional analysis of 460 early-stage urothelial carcinomas and showed that NMIBC can be subgrouped into three major classes with basal- and luminal-like characteristics and different clinical outcomes. Large differences in biological processes such as the cell cycle, epithelial-mesenchymal transition, and differentiation were observed. Analysis of transcript variants revealed frequent mutations in genes encoding proteins involved in chromatin organization and cytoskeletal functions. Furthermore, mutations in well-known cancer driver genes (e.g., TP53 and ERBB2) were primarily found in high-risk tumors, together with APOBEC-related mutational signatures. The identification of subclasses in NMIBC may offer better prognostication and treatment selection based on subclass assignment., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published
2016
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26. Evaluation of an Epigenetic Profile for the Detection of Bladder Cancer in Patients with Hematuria.

Author

van Kessel KE, Van Neste L, Lurkin I, Zwarthoff EC, and Van Criekinge W

Subjects
Adult, Aged, Aged, 80 and over, Epigenomics, Female, Gene Expression Profiling, Hematuria etiology, Humans, Male, Middle Aged, Multivariate Analysis, Mutation, Sensitivity and Specificity, Urinary Bladder Neoplasms complications, Urinary Bladder Neoplasms urine, Young Adult, Urinary Bladder Neoplasms diagnosis, Urinary Bladder Neoplasms genetics
Abstract

Purpose: Many patients enter the care cycle with gross or microscopic hematuria and undergo cystoscopy to rule out bladder cancer. Sensitivity of this invasive examination is limited, leaving many patients at risk for undetected cancer. To improve current clinical practice more sensitive and noninvasive screening methods should be applied., Materials and Methods: A total of 154 urine samples were collected from patients with hematuria, including 80 without and 74 with bladder cancer. DNA from cells in the urine was epigenetically profiled using 2 independent assays. Methylation specific polymerase chain reaction was performed on TWIST1. SNaPshot™ methylation analysis was done for different loci of OTX1 and ONECUT2. Additionally all samples were analyzed for mutation status of TERT (telomerase reverse transcriptase), PIK3CA, FGFR3 (fibroblast growth factor receptor 3), HRAS, KRAS and NRAS., Results: The combination of TWIST1, ONECUT2 (2 loci) and OTX1 resulted in the best overall performing panel. Logistic regression analysis on these methylation markers, mutation status of FGFR3, TERT and HRAS, and patient age resulted in an accurate model with 97% sensitivity, 83% specificity and an AUC of 0.93 (95% CI 0.88-0.98). Internal validation led to an optimism corrected AUC of 0.92. With an estimated bladder cancer prevalence of 5% to 10% in a hematuria cohort the assay resulted in a 99.6% to 99.9% negative predictive value., Conclusions: Epigenetic profiling using TWIST1, ONECUT2 and OTX1 results in a high sensitivity and specificity. Accurate risk prediction might result in less extensive and invasive examination of patients at low risk, thereby reducing unnecessary patient burden and health care costs., (Copyright © 2016 American Urological Association Education and Research, Inc. Published by Elsevier Inc. All rights reserved.)

Published
2016
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27. FGFR3 mutation analysis in voided urine samples to decrease cystoscopies and cost in nonmuscle invasive bladder cancer surveillance: a comparison of 3 strategies.

Author

van Kessel KE, Kompier LC, de Bekker-Grob EW, Zuiverloon TC, Vergouwe Y, Zwarthoff EC, and Steyerberg EW

Subjects
Adult, Aged, Aged, 80 and over, Carcinoma, Transitional Cell diagnosis, Carcinoma, Transitional Cell economics, Carcinoma, Transitional Cell genetics, Carcinoma, Transitional Cell urine, Cost-Benefit Analysis, Female, Humans, Male, Middle Aged, Retrospective Studies, Urinary Bladder Neoplasms diagnosis, Urinary Bladder Neoplasms economics, Cystoscopy statistics & numerical data, Receptor, Fibroblast Growth Factor, Type 3 genetics, Urinary Bladder Neoplasms genetics, Urinary Bladder Neoplasms urine
Abstract

Purpose: We determined whether FGFR3 mutation analysis of voided urine samples would be cost-effective to partly replace cystoscopy in the surveillance of patients treated for nonmuscle invasive urothelial carcinoma., Materials and Methods: In this decision analytical study we analyzed data on 70 Dutch patients with FGFR3 positive primary tumors and a median followup of 8.8 years. Surveillance strategies were compared in a Markov model. Modified surveillance consisted of FGFR3 mutation analysis of voided urine samples every 3 months, and cystoscopy at 3, 12 and 24 months. Standard surveillance was defined as cystoscopy every 3 months and minimal surveillance was defined as cystoscopy at 3, 12 and 24 months. Analysis was stratified for 3 risk profiles, including surveillance after 1) the primary tumor, 2) the first to third recurrence and 3) the fourth recurrence or more. Sensitivity analysis was performed to evaluate the impact of variations in cost, sensitivity and specificity., Results: The probability of no recurrence after 2 years of surveillance after a primary tumor was higher for modified surveillance than for standard and minimal surveillance, eg after primary tumors (95.7% vs 95.0% and 93.9%, respectively). The total cost of surveillance after the primary tumor was lower for minimal and modified surveillance (€2,254 and €2,558, respectively) than for standard surveillance (€5,861). Results were robust to changing inputs over plausible ranges and consistent for each of the 3 risk profiles., Conclusions: Surveillance in which cystoscopy is partly replaced by FGFR3 mutation analysis of urine seems a safe, effective and cost-effective surveillance strategy. Further validation in larger cohorts is required., (Copyright © 2013 American Urological Association Education and Research, Inc. Published by Elsevier Inc. All rights reserved.)

Published
2013
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