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1. Has Active Surveillance for Prostate Cancer Become Safer? Lessons Learned from a Global Clinical Registry.

Author

Bangma, C, Doan, P, Zhu, L, Remmers, S, Nieboer, D, Helleman, J, Roobol, MJ, Sugimoto, M, Chung, BH, Lee, LS, Frydenberg, M, Klotz, L, Peacock, M, Perry, A, Bjartell, A, Rannikko, A, Van Hemelrijck, M, Dasgupta, P, Moore, C, Trock, BJ, Pavlovich, C, Steyerberg, E, Carroll, P, Koo, KC, Hayen, A, Thompson, J, Movember Foundation’s Global Action Plan Prostate Cancer Active Surveillance (GAP3) Consortium, Bangma, C, Doan, P, Zhu, L, Remmers, S, Nieboer, D, Helleman, J, Roobol, MJ, Sugimoto, M, Chung, BH, Lee, LS, Frydenberg, M, Klotz, L, Peacock, M, Perry, A, Bjartell, A, Rannikko, A, Van Hemelrijck, M, Dasgupta, P, Moore, C, Trock, BJ, Pavlovich, C, Steyerberg, E, Carroll, P, Koo, KC, Hayen, A, Thompson, J, and Movember Foundation’s Global Action Plan Prostate Cancer Active Surveillance (GAP3) Consortium

Abstract

BACKGROUND AND OBJECTIVE: Active surveillance (AS) has evolved into a widely applied treatment strategy for many men around the world with low-risk prostate cancer (or in selected cases intermediate-risk disease). Here, we report on the safety and acceptability of AS, and treatment outcomes for low- and intermediate-risk tumours over time in 14 623 men with follow-up of over 6 yr. METHODS: Clinical data from 26 999 men on AS from 25 cohorts in 15 countries have been collected in an international database from 2000 onwards. KEY FINDINGS AND LIMITATIONS: Across our predefined four time periods of 4 yr each (covering the period 2000-2016), there was no significant change in overall survival (OS). However, metastasis-free survival (MFS) rates have improved since the second period and were excellent (>99%). Treatment-free survival rates for earlier periods showed a slightly more rapid shift to radical treatment. Over time, there was a constant proportion of 5% of men for whom anxiety was registered as the reason for treatment alteration. There was, however, also a subset of 10-15% in whom treatment was changed, for which no apparent reason was available. In a subset of men (10-15%), tumour progression was the trigger for treatment. In men who opted for radical treatment, surgery was the most common treatment modality. In those men who underwent radical treatment, 90% were free from biochemical recurrence at 5 yr after treatment. CONCLUSIONS AND CLINICAL IMPLICATIONS: Our study confirms that AS was a safe management option over the full duration in this large multicentre cohort with long-term follow-up, given the 84.1% OS and 99.4% MFS at 10 yr. The probability of treatment at 10 yr was 20% in men with initial low-risk tumours and 31% in men with intermediate-risk tumours. New diagnostic modalities may improve the acceptability of follow-up using individual risk assessments, while safely broadening the use of AS in higher-risk tumours. PATIENT SUMMARY: Active surveillance

Published
2024

2. Understanding the barriers to prostate cancer population-based early detection programs: The PRAISE-U BEST survey

Author

Beyer, K., primary, Leenen, R., additional, Venderbos, L.D.F., additional, Helleman, J., additional, Denijs, F., additional, Gomez Rivas, J., additional, Vasilyeva, V., additional, Briers, E., additional, Chloupkova, R., additional, Májek, O., additional, Frese, T., additional, Vilaseca, J., additional, Vinker, S., additional, Vynckier, P., additional, Annemans, L., additional, Basu, P., additional, Chandran, A., additional, Van Den Bergh, R.C.N., additional, Collen, S., additional, Van Poppel, H., additional, and Roobol, M.J., additional

Published
2024
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3. Why is there a need to re-think prostate cancer early detection?

Author

Beyer, K., primary, Leenen, R., additional, Venderbos, L.D.F., additional, Denijs, F., additional, Helleman, J., additional, Chloupkova, R., additional, Májek, O., additional, Briers, E., additional, Vasilyeva, V., additional, Gomez Rivas, J., additional, Annemans, L., additional, Vynckier, P., additional, Basu, P., additional, Chandran, A., additional, Van Den Bergh, R.C.N., additional, Collen, S., additional, Stenzl, A., additional, Van Poppel, H., additional, and Roobol, M.J., additional

Published
2024
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5. Molecular characterization of upper urinary tract urothelial carcinoma and paired bladder cancer recurrences

Author

Nakauma-González, J.A., primary, Bahlinger, V., additional, Van Doeveren, T., additional, Van De Werken, H.J.G., additional, Helleman, J., additional, Pasanisi, J., additional, Masliah Planchon, J., additional, Bieche, I., additional, Wilhelm, T., additional, Lara, M.F., additional, García-Morales, L., additional, Eckstein, M., additional, Stöhr, R., additional, Sikic, D., additional, García Munoz, I., additional, Prieto Cuadra, J.D., additional, Lozano, M.J., additional, Álvarez, M., additional, Matas-Rico, E., additional, Hartmann, A., additional, Herrera-Imbroda, B., additional, Allory, Y., additional, and Boormans, J.L., additional

Published
2024
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6. Impact of the COVID-19 pandemic on surgical care in the Netherlands

Author

De Graaff, Michelle R, Hogenbirk, Rianne N M, Janssen, Yester F, Elfrink, Arthur K E, Liem, Ronald S L, Nienhuijs, Simon W, De Vries, Jean Paul P M, Elshof, Jan Willem, Verdaasdonk, Emiel, Melenhorst, Jarno, Van Westreenen, H L, Besselink, Marc G H, Ruurda, Jelle P, Van Berge Henegouwen, Mark I, Klaase, Joost M, Den Dulk, Marcel, Van Heijl, Mark, Hegeman, Johannes H, Braun, Jerry, Voeten, Daan M, Würdemann, Franka S, Warps, Anne Loes K, Alberga, Anna J, Suurmeijer, J Annelie, Akpinar, Erman O, Wolfhagen, Nienke, Van Den Boom, Anne Loes, Bolster-van Eenennaam, Marieke J, Van Duijvendijk, Peter, Heineman, David J, Wouters, Michel W J M, Kruijff, Schelto, Helleman, J N, Koningswoud-terhoeve, C L, Belt, E, Van Der Hoeven, J A B, Marres, G M H, Tozzi, F, Von Meyenfeldt, E M, Coebergh, R R J, Van Den Braak, H.P., Rijken, A M, Balm, R, Daams, F, Dickhoff, C, Eshuis, W J, Gisbertz, S S, Zandbergen, H R, Geelkerken, R H, Halfwerk, F R, Biomedical Signals and Systems, TechMed Centre, Multi-Modality Medical Imaging, Biomechanical Engineering, Engineering Organ Support Technologies, Digital Society Institute, RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, Surgery, MUMC+: MA Heelkunde (9), RS: NUTRIM - R2 - Liver and digestive health, Cardiothoracic Surgery, Dermatology, Cancer Center Amsterdam, Cardio-thoracic surgery, Obstetrics and gynaecology, Amsterdam Reproduction & Development (AR&D), CCA - Cancer Treatment and Quality of Life, CCA - Imaging and biomarkers, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, Graduate School, ​Robotics and image-guided minimally-invasive surgery (ROBOTICS), Groningen Institute for Organ Transplantation (GIOT), Value, Affordability and Sustainability (VALUE), and Guided Treatment in Optimal Selected Cancer Patients (GUTS)

Subjects
COMPLICATIONS, HIP, SDG 3 - Good Health and Well-being, DUTCH INSTITUTE, MULTICENTER, Surgery, COHORT
Abstract

During the COVID-19 pandemic, a 13.6 per cent reduction in the number of surgical procedures performed was observed in 2020. Despite great pressure on healthcare, the COVID-19 pandemic did not cause an increase in adverse surgical outcomes, and oncological surgery-related duration of hospital and ICU stay were significantly shorter.Background The COVID-19 pandemic caused disruption of regular healthcare leading to reduced hospital attendances, repurposing of surgical facilities, and cancellation of cancer screening programmes. This study aimed to determine the impact of COVID-19 on surgical care in the Netherlands. Methods A nationwide study was conducted in collaboration with the Dutch Institute for Clinical Auditing. Eight surgical audits were expanded with items regarding alterations in scheduling and treatment plans. Data on procedures performed in 2020 were compared with those from a historical cohort (2018-2019). Endpoints included total numbers of procedures performed and altered treatment plans. Secondary endpoints included complication, readmission, and mortality rates. Results Some 12 154 procedures were performed in participating hospitals in 2020, representing a decrease of 13.6 per cent compared with 2018-2019. The largest reduction (29.2 per cent) was for non-cancer procedures during the first COVID-19 wave. Surgical treatment was postponed for 9.6 per cent of patients. Alterations in surgical treatment plans were observed in 1.7 per cent. Time from diagnosis to surgery decreased (to 28 days in 2020, from 34 days in 2019 and 36 days in 2018; P < 0.001). For cancer-related procedures, duration of hospital stay decreased (5 versus 6 days; P < 0.001). Audit-specific complications, readmission, and mortality rates were unchanged, but ICU admissions decreased (16.5 versus 16.8 per cent; P < 0.001). Conclusion The reduction in the number of surgical operations was greatest for those without cancer. Where surgery was undertaken, it appeared to be delivered safely, with similar complication and mortality rates, fewer admissions to ICU, and a shorter hospital stay.Lay Summary COVID-19 has had a significant impact on healthcare worldwide. Hospital visits were reduced, operating facilities were used for COVID-19 care, and cancer screening programmes were cancelled. This study describes the impact of the COVID-19 pandemic on Dutch surgical healthcare in 2020. Patterns of care in terms of changed or delayed treatment are described for patients who had surgery in 2020, compared with those who had surgery in 2018-2019. The study found that mainly non-cancer surgical treatments were cancelled during months with high COVID-19 rates. Outcomes for patients undergoing surgery were similar but with fewer ICU admissions and shorter hospital stay. These data provide no insight into the burden endured by patients who had postponed or cancelled operations.

Published
2022
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7. Association of Hospital Volume with Perioperative Mortality of Endovascular Repair of Complex Aortic Aneurysms: A Nationwide Cohort Study

Author

Alberga, Anna J., von Meijenfeldt, Gerdine C. I., Rastogi, Vinamr, de Bruin, Jorg L., Wever, Jan J., van Herwaarden, Joost A., Hamming, Jaap F., Hazenberg, Constantijn E. V. B., van Schaik, Jan, Mees, Barend M. E., van der Laan, Maarten J., Zeebregts, Clark J., Schurink, Geert W. H., Verhagen, Hence J. M., van den Akker, P. J., Akkersdijk, G. P., Akkersdijk, W. L., van Andringa de Kempenaer, M. G., Arts, C. H. P., Avontuur, A. M., Bakker, O. J., Balm, R., Barendregt, W. B., Bekken, J. A., Bender, M. H. M., Bendermacher, B. L. W., van den Berg, M., Beuk, R. J., Blankensteijn, J. D., Bode, A. S., Bodegom, M. E., van der Bogt, K. E. A., Boll, A. P. M., Booster, M. H., Borger van der Burg, B. L. S., de Borst, G. J., Bos-van Rossum, W. T. G. J., Bosma, J., Botman, J. M. J., Bouwman, L. H., Brehm, V., de Bruijn, M. T., de Bruin, J. L., Brummel, P., van Brussel, J. P., Buijk, S. E., Buimer, M. G., Buscher, H. C. J. L., Cancrinus, E., Castenmiller, P. H., Cazander, G., Cuypers, P. W. M., Daemen, J. H. C., Dawson, I., Dierikx, J. E., Dijkstra, M. L., Diks, J., Dinkelman, M. K., Dirven, M., Dolmans, D. E. J. G. J., van Dortmont, L. M. C., Drouven, J. W., van der Eb, M. M., Eefting, D., van Eijck, G. J. W. M., Elshof, J. W. M., Elsman, A. H. P., van der Elst, A., van Engeland, M. I. A., van Eps, G. S., Faber, M. J., de Fijter, W. M., Fioole, B., Fritschy, W. M., Fung Kon Jin, P. H. P., Geelkerken, R. H., van Gent, W. B., Glade, G. J., Govaert, B., Groenendijk, R. P. R., de Groot, H. G. W., van den Haak, R. F. F., de Haan, E. F. A., Hajer, G. F., Hamming, J. F., van Hattum, E. S., Hazenberg, C. E. V. B., Hedeman Joosten, P. P. A., Helleman, J. N., van der Hem, L. G., Hendriks, J. M., van Herwaarden, J. A., Heyligers, J. M. M., Hinnen, J. W., Hissink, R. J., Ho, G. H., den Hoed, P. T., Hoedt, M. T. C., van Hoek, F., Hoencamp, R., Hoffmann, W. H., Hoksbergen, A. W. J., Hollander, E. J. F., Huisman, L. C., Hulsebos, R. G., Huntjens, K. M. B., Idu, M. M., Jacobs, M. J. H. M., van der Jagt, M. F. P., Jansbeken, J. R. H., Janssen, R. J. L., Jiang, H. H. L., de Jong, S. C., Jongbloed-Winkel, T. A., Jongkind, V., Kapma, M. R., Keller, B. P. J. A., Jahrome, A. Khodadade, Kievit, J. K., Klemm, P. L., Klinkert, P., Koedam, N. A., Koelemaij, M. J. W., Kolkert, J. L. P., Koning, G. G., Koning, O. H. J., Konings, R., Krasznai, A. G., Kropman, R. H. J., Kruse, R. R., van der Laan, L., van der Laan, M. J., van Laanen, J. H. H., van Lammeren, G. W., Lamprou, D. A. A., Lardenoije, J. H. P., Lauret, G. J., Leenders, B. J. M., Legemate, D. A., Leij-Dekkers, V. J., Lemson, M. S., Lensvelt, M. M. A., Lijkwan, M. A., van der Linden, F. T. P. M., Lung, P. F. L., Loos, M. J. A., Loubert, M. C., van de Luijtgaarden, K. M., Mahmoud, D. E. A. K., Manshanden, C. G., Mat-Tens, E. C. J. L., Meerwaldt, R., Mees, B. M. E., Menting, T. P., Metz, R., de Mol van Otterloo, J. C. A., Molegraaf, M. J., Montauban van Swijn-Dregt, Y. C. A., Morak, M. J. M., van de Mortel, R. H. W., Mulder, W., Nagesser, S. K., Naves, C. C. L. M., Nederhoed, J. H., Nevenzel, A. M., de Nie, A. J., Nieuwenhuis, D. H., van Nieuwenhuizen, R. C., Nieuwenhui-Zen, J., Nio, D., Oomen, A. P. A., Oranen, B. I., Oskam, J., Palamba, H. W., Peppelenbosch, A. G., van Petersen, A. S., Petri, B. J., Pierie, M. E. N., Ploeg, A. J., Pol, R. A., Ponfoort, E. D., Poyck, P. P. C., Prent, A., ten Raa, S., Raymakers, J. T. F. J., Reichmann, B. L., Reijnen, M. M. P. J., de Ridder, J. A. M., Rijbroek, A., van Rijn, M. J. E., de Roo, R. A., Rouwet, E. V., Saleem, B. R., van Sambeek, M. R. H. M., Samyn, M. G., van't Sant, H. P., van Schaik, J., van Schaik, P. M., Scharn, D. M., Scheltinga, M. R. M., Schepers, A., Schlejen, P. M., Schlösser, F. J. V., Schol, F. P. G., Scholtes, V. P. W., Schouten, O., Schreve, M. A., Schurink, G. W. H., Sikkink, C. J. J. M., te Slaa, A., Smeets, H. J., Smeets, L., Smeets, R. R., de Smet, A. A. E. A., Smit, P. C., Smits, T. M., Snoeijs, M. G. J., Sondakh, A. O., Speijers, M. J., van der Steenhoven, T. J., van Sterkenburg, S. M. M., Stigter, D. A. A., Stokmans, R. A., Strating, R. P., Stultiëns, G. N. M., Sybrandy, J. E. M., Teijink, J. A. W., Telgenkamp, B. J., Testroote, M. J. G., Tha-in, T., The, R. M., Thijsse, W. J., Thomassen, I., Tielliu, I. F. J., van Tongeren, R. B. M., Toorop, R. J., Tournoij, E., Truijers, M., Türkcan, K., Nolthenius, R. P. Tutein, Ünlü, C., Vaes, R. H. D., Vahl, A. C., Veen, E. J., Veger, H. T. C., Veldman, M. G., Verhagen, H. J. M., Verhoeven, B. A. N., Vermeulen, C. F. W., Vermeulen, E. G. J., Vierhout, B. P., van der Vijver-Coppen, R. J., Visser, M. J. T., van der Vliet, J. A., van Vlijmen-van Keulen, C. J., van der Vorst, J. R., Vos, A. W. F., Vos, C. G., Vos, G. A., de Vos, B., Voûte, M. T., Vriens, B. H. R., Vriens, P. W. H. E., de Vries, D. K., de Vries, J. P. P. M., de Vries, M., de Vries, A. C., van der Waal, C., Waasdorp, E. J., de Vries, B. M. Wallis, van Walraven, L. A., van Wanroi, J. L., Warlé, M. C., van Weel, V., van Well, A. M. E., Welten, G. M. J. M., Wever, J. J., Wiersema, A. M., Wikkeling, O. R. M., Willaert, W. I. M., Wille, J., Willems, M. C. M., Willigendael, E. M., Wilschut, E. D., Wisselink, W., Witte, M. E., Wittens, C. H. A., Wong, C. Y., Yazar, O., Yeung, K. K., Zeebregts, C. J. A. M., van Zeeland, M. L. P., Physiology, ACS - Pulmonary hypertension & thrombosis, Surgery, ACS - Atherosclerosis & ischemic syndromes, ACS - Microcirculation, VU University medical center, AII - Inflammatory diseases, APH - Digital Health, Medical Biochemistry, ACS - Diabetes & metabolism, AII - Infectious diseases, and AGEM - Amsterdam Gastroenterology Endocrinology Metabolism

Subjects
volume-outcome, complex AAA, endovascular, mortality
Abstract

Objective: We evaluate nationwide perioperative outcomes of complex EVAR and assess the volume-outcome association of complex EVAR. Summary of Background Data: Endovascular treatment with fenestrated (FEVAR) or branched (BEVAR) endografts is progressively used for excluding complex aortic aneurysms (complex AAs). It is unclear if a volumeoutcome association exists in endovascular treatment of complex AAs (complex EVAR). Methods: All patients prospectively registered in the Dutch Surgical Aneurysm Audit who underwent complex EVAR (FEVAR or BEVAR) between January 2016 and January 2020 were included. The effect of annual hospital volume on perioperative mortality was examined using multivariable logistic regression analyses. Patients were stratified into quartiles based on annual hospital volume to determine hospital volume categories. Results: We included 694 patients (539 FEVAR patients, 155 BEVAR patients). Perioperative mortality following FEVAR was 4.5% and 5.2% following BEVAR. Postoperative complication rates were 30.1% and 48.7%, respectively. The first quartile hospitals performed

Published
2023
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8. Comparison of outcomes of different biopsy schedules among men on active surveillance for prostate cancer: An analysis of the G.A.P.3 global consortium database

Author

Beckmann, KR, Bangma, CH, Helleman, J, Bjartell, A, Carroll, PR, Morgan, T, Nieboer, D, Santaolalla, A, Trock, BJ, Valdagni, R, Roobol, MJ, and Global Action Plan Active Surveillance Prostate Cancer [G.A.P.3] Consortium

Subjects
Male, Urologic Diseases, Aging, treatment, 1103 Clinical Sciences, 1112 Oncology and Carcinogenesis, 1114 Paediatrics and Reproductive Medicine, Biopsy, Prevention, Prostate Cancer, active surveillance, Clinical Sciences, Oncology and Carcinogenesis, Prostate, Prostatic Neoplasms, Global Action Plan Active Surveillance Prostate Cancer [G.A.P.3] Consortium, Prostate-Specific Antigen, Paediatrics and Reproductive Medicine, Clinical Research, biopsy schedule, Disease Progression, Humans, Oncology & Carcinogenesis, Neoplasm Grading, Watchful Waiting, upgrading, Cancer
Abstract

BACKGROUND: The optimal interval for repeat biopsy during active surveillance (AS) for prostate cancer is yet to be defined. This study examined whether risk of upgrading (to grade group ≥ 2) or risk of converting to treatment varied according to intensity of repeat biopsy using data from the GAP3 consortium's global AS database. MATERIALS AND METHODS: Intensity of surveillance biopsy schedules was categorized according to centers' protocols: (a) Prostate Cancer Research International Active Surveillance project (PRIAS) protocols with biopsies at years 1, 4, and 7 (10 centers; 7532 men); (b) biennial biopsies, that is, every other year (8 centers; 4365 men); and (c) annual biopsy schedules (4 centers; 1602 men). Multivariable Cox regression was used to compare outcomes according to biopsy intensity. RESULTS: Out of the 13,508 eligible participants, 56% were managed according to PRIAS protocols (biopsies at years 1, 4, and 7), 32% via biennial biopsy, and 12% via annual biopsy. After adjusting for baseline characteristics, risk of converting to treatment was greater for those on annual compared with PRIAS biopsy schedules (hazard ratio [HR] = 1.66; 95% confidence interval [CI] = 1.51-1.83; p

Published
2022

9. Prostate Cancer Patients Under Active Surveillance with a Suspicious Magnetic Resonance Imaging Finding Are at Increased Risk of Needing Treatment: Results of the Movember Foundation's Global Action Plan Prostate Cancer Active Surveillance (GAP3) Consortium.

Author

Olivier, J, Li, W, Nieboer, D, Helleman, J, Roobol, M, Gnanapragasam, V, Frydenberg, M, Sugimoto, M, Carroll, P, Morgan, TM, Valdagni, R, Rubio-Briones, J, Robert, G, Stricker, P, Hayen, A, Schoots, I, Haider, M, Moore, CM, Denton, B, Villers, A, Movember Foundation's Global Action Plan Prostate Cancer Active Surveillance GAP3 Consortium, Olivier, J, Li, W, Nieboer, D, Helleman, J, Roobol, M, Gnanapragasam, V, Frydenberg, M, Sugimoto, M, Carroll, P, Morgan, TM, Valdagni, R, Rubio-Briones, J, Robert, G, Stricker, P, Hayen, A, Schoots, I, Haider, M, Moore, CM, Denton, B, Villers, A, and Movember Foundation's Global Action Plan Prostate Cancer Active Surveillance GAP3 Consortium

Abstract

BACKGROUND: The inclusion criterion for active surveillance (AS) is low- or intermediate-risk prostate cancer. The predictive value of the presence of a suspicious lesion at magnetic resonance imaging (MRI) at the time of inclusion is insufficiently known. OBJECTIVE: To evaluate the percentage of patients needing active treatment stratified by the presence or absence of a suspicious lesion at baseline MRI. DESIGN SETTING AND PARTICIPANTS: A retrospective analysis of the data from the multicentric AS GAP3 Consortium database was conducted. The inclusion criteria were men with grade group (GG) 1 or GG 2 prostate cancer combined with prostate-specific antigen <20 ng/ml. We selected a subgroup of patients who had MRI at baseline and for whom MRI results and targeted biopsies were used for AS eligibility. Suspicious MRI was defined as an MRI lesion with Prostate Imaging Reporting and Data System (PI-RADS)/Likert ≥3 and for which targeted biopsies did not exclude the patient for AS. OUTCOME MEASUREMENTS AND STATISTICAL ANALYSIS: The primary outcome was treatment free survival (FS). The secondary outcomes were histological GG progression FS and continuation of AS (discontinuation FS). RESULTS AND LIMITATIONS: The study cohort included 2119 patients (1035 men with nonsuspicious MRI and 1084 with suspicious MRI) with a median follow-up of 23 (12-43) mo. For the whole cohort, 3-yr treatment FS was 71% (95% confidence interval [CI]: 69-74). For nonsuspicious MRI and suspicious MRI groups, 3-yr treatment FS rates were, respectively, 80% (95% CI: 77-83) and 63% (95% CI: 59-66). Active treatment (hazard ratio [HR] = 2.0, p < 0.001), grade progression (HR = 1.9, p < 0.001), and discontinuation of AS (HR = 1.7, p < 0.001) were significantly higher in the suspicious MRI group than in the nonsuspicious MRI group. CONCLUSIONS: The risks of switching to treatment, histological progression, and AS discontinuation are higher in cases of suspicious MRI at inclusion. PATIENT SUMMARY: Among

Published
2022

10. Treatment Outcome Trends for Non-Ruptured Abdominal Aortic Aneurysms: A Nationwide Prospective Cohort Study

Author

Alberga, Anna J., Karthaus, Eleonora G., Wilschut, Janneke A., de Bruin, Jorg L., Akkersdijk, George P., Geelkerken, Robert H., Hamming, Jaap F., Wever, Jan J., Verhagen, Hence J. M., van den Akker, P. J., Akkersdijk, G. P., Akkersdijk, W. L., van Andringa de Kempenaer, M. G., Arts, C. H. P., Avontuur, A. M., Bakker, O. J., Balm, R., Barendregt, W. B., Bekken, J. A., Bender, M. H. M., Bendermacher, B. L. W., van den Berg, M., Beuk, R. J., Blankensteijn, J. D., Bode, A. S., Bodegom, M. E., van der Bogt, K. E. A., Boll, A. P. M., Booster, M. H., Borger van der Burg, B. L. S., de Borst, G. J., Bos-van Rossum, W. T. G. J., Bosma, J., Botman, J. M. J., Bouwman, L. H., Brehm, V., de Bruijn, M. T., de Bruin, J. L., Brummel, P., van Brussel, J. P., Buijk, S. E., Buimer, M. G., Buscher, H. C. J. L., Cancrinus, E., Castenmiller, P. H., Cazander, G., Cuypers, P. H. W. M., Daemen, J. H. C., Dawson, I., Dierikx, J. E., Dijkstra, M. L., Diks, J., Dinkelman, M. K., Dirven, M., Dolmans, D. E. J. G. J., van Dortmont, L. M. C., Drouven, J. W., van der Eb, M. M., Eefting, D., van Eijck, G. J. W. M., Elshof, J. W. M., Elsman, B. H. P., van der Elst, A., van Engeland, M. I. A., van Eps, G. S., Faber, M. J., de Fijter, W. M., Fioole, B., Fritschy, W. M., Jin, P. H. P. F. K., Geelkerken, R. H., van Gent, W. B., Glade, G. J., Govaert, B., Groenendijk, R. P. R., de Groot, H. G. W., van den Haak, R. F. F., de Haan, E. F. A., Hajer, G. F., Hamming, J. F., van Hattum, E. S., Hazenberg, C. E. V. B., Hedeman Joosten, P. P. H. A., Helleman, J. N., van der Hem, L. G., Hendriks, J. M., van Herwaarden, J. A., Heyligers, J. M. M., Hinnen, J. W., Hissink, R. J., Ho, G. H., den Hoed, P. T., Hoedt, M. T. C., van Hoek, F., Hoencamp, R., Hoffmann, W. H., Hoksbergen, A. W. J., Hollander, E. J. F., Huisman, L. C., Hulsebos, R. G., Huntjens, K. M. B., Idu, M. M., Jacobs, M. J. H. M., van der Jagt, M. F. P., Jansbeken, J. R. H., Janssen, R. J. L., Jiang, H. H. L., de Jong, S. C., Jongbloed-Winkel, T. A., Jongkind, V., Kapma, M. R., Keller, B. P. J. A., Jahrome, A. K., Kievit, J. K., Klemm, P. L., Klinkert, P., Koedam, N. A., Koelemaij, M. J. W., Kolkert, J. L. P., Koning, G. G., Koning, O. H. J., Konings, R., Krasznai, A. G., Kropman, R. H. J., Kruse, R. R., van der Laan, L., van der Laan, M. J., van Laanen, J. H. H., van Lammeren, G. W., Lamprou, D. A. A., Lardenoije, J. H. P., Lauret, G. J., Leenders, B. J. M., Legemate, D. A., Leijdekkers, V. J., Lemson, M. S., Lensvelt, M. M. A., Lijkwan, M. A., van der Linden, F. T. H. P. M., Lung, P. F. Liqui, Loos, M. J. A., Loubert, M. C., van de Luijtgaarden, K. M., Mahmoud, D. E. A. K., Manshanden, C. G., Mattens, E. C. J. L., Meerwaldt, R., Mees, B. M. E., Menting, T. P., Metz, R., de Mol van Otterloo, J. C. A., Molegraaf, M. J., Montauban van Swijndregt, Y. C. A., Morak, M. J. M., van de Mortel, R. H. W., Mulder, W., Nagesser, S. K., Naves, C. C. L. M., Nederhoed, J. H., Nevenzel, A. M., de Nie, A. J., Nieuwenhuis, D. H., van Nieuwenhuizen, R. C., Nieuwenhuizen, J., Nio, D., Oomen, A. P. A., Oranen, B. I., Oskam, J., Palamba, H. W., Peppelenbosch, A. G., van Petersen, A. S., Petri, B. J., Pierie, M. E. N., Ploeg, A. J., Pol, R. A., Ponfoort, E. D., Poyck, P. P. C., Prent, A., Raa, S. ten, Raymakers, J. T. F. J., Reichmann, B. L., Reijnen, M. M. P. J., de Ridder, J. A. M., Rijbroek, A., van Rijn, M. J. E., de Roo, R. A., Rouwet, E. V., Saleem, B. R., van Sambeek, M. R. H. M., Samyn, M. G., van ’t Sant, H. P., van Schaik, J., van Schaik, P. M., Scharn, D. M., Scheltinga, M. R. M., Schepers, A., Schlejen, P. M., Schlösser, F. J. V., Schol, F. P. G., Scholtes, V. P. W., Schouten, O., Schreve, M. A., Schurink, G. W. H., Sikkink, C. J. J. M., Slaa, A. te, Smeets, H. J., Smeets, L., Smeets, R. R., de Smet, A. A. E. A., Smit, P. C., Smits, T. M., Snoeijs, M. G. J., Sondakh, A. O., Speijers, M. J., van der Steenhoven, T. J., van Sterkenburg, S. M. M., Stigter, D. A. A., Stokmans, R. A., Strating, R. P., Stultiëns, G. N. M., Sybrandy, J. E. M., Teijink, J. A. W., Telgenkamp, B. J., Testroote, M. J. G., Tha-in, T., The, R. M., Thijsse, W. J., Thomassen, I., Tielliu, I. F. J., van Tongeren, R. B. M., Toorop, R. J., Tournoij, E., Truijers, M., Türkcan, K., Tutein Nolthenius, R. P., Ünlü, C., Vaes, R. H. D., Vahl, A. C., Veen, E. J., Veger, H. T. C., Veldman, M. G., Verhagen, H. J. M., Verhoeven, B. A. N., Vermeulen, C. F. W., Vermeulen, E. G. J., Vierhout, B. P., van der Vijver-Coppen, R. J., Visser, M. J. T., van der Vliet, J. A., van Vlijmen - van Keulen, C. J., van der Vorst, J. R., Vos, A. W. F., Vos, C. G., Vos, G. A., de Vos, B., Voûte, M. T., Vriens, B. H. R., Vriens, P. W. H. E., de Vries, D. K., de Vries, J. P. P. M., de Vries, M., de Vries, A. C., van der Waal, C., Waasdorp, E. J., Wallis de Vries, B. M., van Walraven, L. A., van Wanroi, J. L., Warlé, M. C., van Weel, V., van Well, A. M. E., Welten, G. M. J. M., Wever, J. J., Wiersema, A. M., Wikkeling, O. R. M., Willaert, W. I. M., Wille, J., Willems, M. C. M., Willigendael, E. M., Wilschut, E. D., Wisselink, W., Witte, M. E., Wittens, C. H. A., Wong, C. Y., Yazar, O., Yeung, K. K., Zeebregts, C. J. A. M., van Zeeland, M. L. P., ACS - Microcirculation, Anesthesiology, Physiology, ACS - Pulmonary hypertension & thrombosis, Surgery, ACS - Atherosclerosis & ischemic syndromes, VU University medical center, ACS - Diabetes & metabolism, TechMed Centre, Multi-Modality Medical Imaging, Medical Biochemistry, and AGEM - Amsterdam Gastroenterology Endocrinology Metabolism

Subjects
Male, Time Factors, Operative procedure, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], Risk Assessment, Blood Vessel Prosthesis Implantation, Postoperative Complications, Risk Factors, Humans, Hospital Mortality, Prospective Studies, Registries, Treatment outcome, Aged, Netherlands, Retrospective Studies, Aged, 80 and over, Endovascular Procedures, Quality of care, Middle Aged, Endovascular procedure, Abdominal aortic aneurysm, Surgery, Female, Trends, Cardiology and Cardiovascular Medicine, Aortic Aneurysm, Abdominal
Abstract

Contains fulltext : 251573.pdf (Publisher’s version ) (Open Access) OBJECTIVE: The Dutch Surgical Aneurysm Audit (DSAA) initiative was established in 2013 to monitor and improve nationwide outcomes of aortic aneurysm surgery. The objective of this study was to examine whether outcomes of surgery for intact abdominal aortic aneurysms (iAAA) have improved over time. METHODS: Patients who underwent primary repair of an iAAA by standard endovascular (EVAR) or open surgical repair (OSR) between 2014 and 2019 were selected from the DSAA for inclusion. The primary outcome was peri-operative mortality trend per year, stratified by OSR and EVAR. Secondary outcomes were trends per year in major complications, textbook outcome (TbO), and characteristics of treated patients. The trends per year were evaluated and reported in odds ratios per year. RESULTS: In this study, 11 624 patients (74.8%) underwent EVAR and 3 908 patients (25.2%) underwent OSR. For EVAR, after adjustment for confounding factors, there was no improvement in peri-operative mortality (aOR [adjusted odds ratio] 1.06, 95% CI 0.94 - 1.20), while major complications decreased (2014: 10.1%, 2019: 7.0%; aOR 0.91, 95% CI 0.88 - 0.95) and the TbO rate increased (2014: 68.1%, 2019: 80.9%; aOR 1.13, 95% CI 1.10 - 1.16). For OSR, the peri-operative mortality decreased (2014: 6.1%, 2019: 4.6%; aOR 0.89, 95% CI 0.82 - 0.98), as well as major complications (2014: 28.6%, 2019: 23.3%; aOR 0.95, 95% CI 0.91 - 0.99). Furthermore, the proportion of TbO increased (2014: 49.1%, 2019: 58.3%; aOR 1.05, 95% CI 1.01 - 1.10). In both the EVAR and OSR group, the proportion of patients with cardiac comorbidity increased. CONCLUSION: Since the establishment of this nationwide quality improvement initiative (DSAA), all outcomes of iAAA repair following EVAR and OSR have improved, except for peri-operative mortality following EVAR which remained unchanged.

Published
2022
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12. A0861 - Molecular characterization of upper urinary tract urothelial carcinoma and paired bladder cancer recurrences

Author

Nakauma-González, J.A., Bahlinger, V., Van Doeveren, T., Van De Werken, H.J.G., Helleman, J., Pasanisi, J., Masliah Planchon, J., Bieche, I., Wilhelm, T., Lara, M.F., García-Morales, L., Eckstein, M., Stöhr, R., Sikic, D., García Munoz, I., Prieto Cuadra, J.D., Lozano, M.J., Álvarez, M., Matas-Rico, E., Hartmann, A., Herrera-Imbroda, B., Allory, Y., and Boormans, J.L.

Published
2024
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18. Adverse pathological findings in deferred radical prostatectomy in men under active surveillance for very low and low risk prostate cancers: Results from GAP3 active surveillance cohorts

Author

Marenghi, C., primary, Qiu, Z., additional, Nicolai, N., additional, Helleman, J., additional, Nieboer, D., additional, Rubio-Briones, J., additional, Carroll, P.R., additional, Cowan, J.E., additional, Lee, L.S., additional, Boutros, P.C., additional, and Valdagni, R., additional

Published
2021
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19. Outcomes after introducing intraoperative NeuroSAFE technique in robot-assisted radical prostatectomy

Author

van der Slot, M.A., primary, Den Bakker, M.A., additional, Kweldam, C.F., additional, Remmers, S., additional, Tan, T., additional, Klaver, O.S., additional, Kliffen, M., additional, Busstra, M.B., additional, Rietbergen, J.B.W., additional, Gan, M., additional, Hamoen, K.E., additional, Budel, L.M., additional, Goemaere, N.T., additional, Bangma, C.H., additional, Helleman, J., additional, Roobol, M.J., additional, and Van Leenders, G.J.L.H., additional

Published
2021
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21. Intraoperative NeuroSAFE enables more frequent nerve-sparing radical prostatectomies

Author

van der Slot, M.A., primary, Den Bakker, M.A., additional, Klaver, O.S., additional, Kliffen, M., additional, Busstra, M.B., additional, Rietbergen, J.B.W., additional, Gan, M., additional, Hamoen, K.E., additional, Budel, L.M., additional, Goemaere, N.T., additional, Kweldam, C.F., additional, Bangma, C., additional, Helleman, J., additional, Roobol, M.J., additional, and Van Leenders, G.J.L.H., additional

Published
2020
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24. Predicting Biopsy Outcomes During Active Surveillance for Prostate Cancer: External Validation of the Canary Prostate Active Surveillance Study Risk Calculators in Five Large Active Surveillance Cohorts

Author

Drost, FJH, Nieboer, D, Morgan, TM, Carroll, PR, Roobol, MJ, Trock, B, Ehdaie, B, Carroll, P, Filson, C, Kim, J, Logothetis, C, Morgan, T, Klotz, L, Pickles, T, Hyndman, E, Moore, CM, Gnanapragasam, V, Van Hemelrijck, M, Dasgupta, P, Bangma, C, Roobol, M, Villers, A, Rannikko, A, Valdagni, R, Perry, A, Hugosson, J, Rubio-Briones, J, Bjartell, A, Hefermehl, L, Shiong, LL, Frydenberg, M, Kakehi, Y, Chung, BH, van der Kwast, T, van der Linden, W, Hulsen, T, de Jonge, C, Kattan, M, Xinge, J, Muir, K, Lophatananon, A, Fahey, M, Steyerberg, E, Zhang, L, Beckmann, K, Denton, B, Hayen, A, Boutros, P, Guo, W, Benfante, N, Cowan, J, Patil, D, Tolosa, E, Kim, TK, Mamedov, A, Lapointe, V, Crump, T, Kimberly-Duffell, J, Santaolalla, A, Olivier, J, Rancati, T, Ahlgren, H, Mascarós, J, Löfgren, A, Lin, CH, Hirama, H, Lee, KS, Jenster, G, Auvinen, A, Haider, M, van Bochove, K, Carter, B, Gledhill, S, Buzza, M, Bruinsma, S, and Helleman, J

Subjects
Urology & Nephrology
Abstract

© 2019 European Association of Urology Two active surveillance risk calculators to predict disease reclassification on prostate biopsy are externally validated by the Movember Foundation's Global Action Plan (GAP3) consortium. They proved to be clinically useful and could reduce unnecessary biopsies, but need recalibration to local settings.

Published
2019

25. Intraoperative assessment and reporting of radical prostatectomy specimens to guide nerve-sparing surgery in prostate cancer patients (NeuroSAFE)

Author

van, M.A. (Margaretha A.), der Slot, (), Bakker, M.A. (Michael) den, Klaver, S. (Sjoerd), Kliffen, M. (Mike), Busstra, M. (Martijn), Rietbergen, J.B. (John), Gan, M. (Melanie), Hamoen, K.E. (Karen E.), Budel, L.M. (Leo M.), Goemaere, N.N.T. (Natascha), Bangma, C.H. (Chris), Helleman, J. (Jozien), Roobol-Bouts, M.J. (Monique), Leenders, G.J.H.L. (Geert), van, M.A. (Margaretha A.), der Slot, (), Bakker, M.A. (Michael) den, Klaver, S. (Sjoerd), Kliffen, M. (Mike), Busstra, M. (Martijn), Rietbergen, J.B. (John), Gan, M. (Melanie), Hamoen, K.E. (Karen E.), Budel, L.M. (Leo M.), Goemaere, N.N.T. (Natascha), Bangma, C.H. (Chris), Helleman, J. (Jozien), Roobol-Bouts, M.J. (Monique), and Leenders, G.J.H.L. (Geert)

Abstract

AIMS: Radical prostatectomy for prostate cancer is frequently complicated by urinary incontinence and erectile dysfunction. Nerve-sparing surgery reduces the risk of post-operative complications and can be optimized using intraoperative frozen sections of the adjacent neurovascular structure (NeuroSAFE). The aim of th

Published
2020
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26. Cribriform architecture in radical prostatectomies predicts oncological outcome in Gleason score 8 prostate cancer patients

Author

Hollemans, E. (Eva), Verhoef, E.I. (Esther), Bangma, C.H. (Chris), Rietbergen, J.B. (John), Osanto, S. (Susanne), Pelger, R.C.M. (R. C M), Wezel, T. (Tom) van, Poel, H.G. (Henk) van der, Bekers, E.M. (Elise), Helleman, J. (Jozien), Roobol-Bouts, M.J. (Monique), Leenders, G.J.H.L. (Geert), Hollemans, E. (Eva), Verhoef, E.I. (Esther), Bangma, C.H. (Chris), Rietbergen, J.B. (John), Osanto, S. (Susanne), Pelger, R.C.M. (R. C M), Wezel, T. (Tom) van, Poel, H.G. (Henk) van der, Bekers, E.M. (Elise), Helleman, J. (Jozien), Roobol-Bouts, M.J. (Monique), and Leenders, G.J.H.L. (Geert)

Abstract

The Gleason score is an important parameter for clinical outcome in prostate cancer patients. Gleason score 8 is a heterogeneous disease including Gleason score 3 + 5, 4 + 4, and 5 + 3 tumors, and encompasses a broad range of tumor growth patterns. Our objective was to characterize individual growth patterns and identify prognostic parameters in Gleason score 8 prostate cancer patients. We reviewed 1064 radical prostatectomy specimens, recorded individual Gleason 4 and 5 growth patterns as well as presence of intraductal carcinoma, and evaluated biochemical recurrence- and metastasis-free survival. Gleason score 8 disease was identified in 140 (13%) patients, of whom 76 (54%) had Gleason score 3 + 5, 46 (33%) 4 + 4, and 18 (13%) 5 + 3 disease. Invasive cribriform and/or intraductal carcinoma (n = 87, 62%) was observed more frequently in Gleason score 4 + 4 (93%) than 3 + 5 (47%; P < 0.001) and 5 + 3 (44%; P < 0.001) patients. Gleason pattern 5 was present in 110 (79%) men: as single cells and/or cords in 99 (90%) and solid fields in 32 (29%) cases. Solid field pattern 5 coexisted with cribriform architecture (23/32, 72%) more frequently than nonsolid pattern 5 cases (36/78, 46%, P = 0.02). In multivariable analysis including age, prostate-specific antigen, pT-stage, surgical margin status, and lymph node metastases, presence of cribriform architecture was an independent parameter for biochemical recurrence-free (hazard ratio (HR) 2.0, 95% confidence interval (CI) 1.0–3.7; P = 0.04) and metastasis-free (HR 3.5, 95% CI 1.0–12.3; P = 0.05) survival. In conclusion, invasive cribriform and/or intraductal carcinoma occurs more frequently in Gleason score 4 + 4 prostate cancer patients than in Gleason score 3 + 5 and 5 + 3, and is an independent parameter for biochemical recurrence and metastasis. Therefore, cribriform architecture has added value in risk stratification of Gleason score 8 prostate cancer patients.

Published
2020
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27. Clinical outcome comparison of Grade Group 1 and Grade Group 2 prostate cancer with and without cribriform architecture at the time of radical prostatectomy

Author

Hollemans, E. (Eva), Verhoef, E.I. (Esther), Bangma, C.H. (Chris), Rietbergen, J.B. (John), Roobol-Bouts, M.J. (Monique), Helleman, J. (Jozien), Leenders, G.J.H.L. (Geert), Hollemans, E. (Eva), Verhoef, E.I. (Esther), Bangma, C.H. (Chris), Rietbergen, J.B. (John), Roobol-Bouts, M.J. (Monique), Helleman, J. (Jozien), and Leenders, G.J.H.L. (Geert)

Abstract

Aims: Invasive cribriform and intraductal carcinoma are associated with aggressive disease in Grade Group 2 (GG2) prostate cancer patients. However, the characteristics and clinical outcome of patients with GG2 prostate cancer without cribriform architecture (GG2−) as compared with those with Grade Group 1 (GG1) prostate cancer are unknown. The aim of this study was to investigate the clinical and pathological characteristics of GG1 and GG2− prostate cancer in radical prostatectomy specimens. Methods and results: We reviewed 835 radical prostatectomy specimens for Grade Group, pT stage, surgical margin status, and the presence of cribriform architecture. Biochemical recurrence-free survival and metastasis were used as clinical outcomes. GG1 prostate cancer was seen in 207 patients, and GG2 prostate cancer was seen in 420 patients, of whom 228 (54%) showed cribriform architecture (GG2+) and 192 (46%) did not. GG2− patients had higher prostate-specific antigen levels (9.4 ng/ml versus 7.0 ng/ml; P < 0.001), more often had extraprostatic extension (36% versus 11%; P < 0.001) and had more positive surgical margins (27% versus 17%; P = 0.01) than GG1 patients. GG2− patients had

Published
2020
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28. TP53 Mutations in Serum Circulating Cell-Free Tumor DNA As Longitudinal Biomarker for High-Grade Serous Ovarian Cancer

Author

Vitale, S.R. (Silvia), Groenendijk, F.H. (Floris H.), Marion, R. (Ronald) van, Beaufort, C.M. (Corine M.), Helmijr, J. (Jean), Jan Dubbink, H. (Hendrikus), N M Dinjens, W. (Winand), Ewing, P.C. (Patricia), Smolders, R. (Ramon), van Doorn, H.C. (Helena C.), Boere, I.A. (Ingrid), Berns, P.M.J.J. (Els), Helleman, J. (Jozien), Jansen, M.P.H.M. (Maurice), Vitale, S.R. (Silvia), Groenendijk, F.H. (Floris H.), Marion, R. (Ronald) van, Beaufort, C.M. (Corine M.), Helmijr, J. (Jean), Jan Dubbink, H. (Hendrikus), N M Dinjens, W. (Winand), Ewing, P.C. (Patricia), Smolders, R. (Ramon), van Doorn, H.C. (Helena C.), Boere, I.A. (Ingrid), Berns, P.M.J.J. (Els), Helleman, J. (Jozien), and Jansen, M.P.H.M. (Maurice)

Abstract

The aim of this study was to determine an optimal workflow to detect TP53 mutations in baseline and longitudinal serum cell free DNA (cfDNA) from high-grade serous ovarian carcinomas (HGSOC) patients and to define whether TP53 mutations are suitable as biomarker for disease. TP53 was investigated in tissue and archived serum from 20 HGSOC patients by a next-generation sequencing (NGS) workflow alone or combined with digital PCR (dPCR). AmpliSeq™-focused NGS panels and customized dPCR assays were used for tissue DNA and longitudinal cfDNAs, and Oncomine NGS panel with molecular barcoding was used for baseline cfDNAs. TP53 missense mutations were observed in 17 tissue specimens and in baseline cfDNA for 4/8 patients by AmpliSeq, 6/9 patients by Oncomine, and 4/6 patients by dPCR. Mutations in cfDNA were detected in 4/6 patients with residual disease and 3/4 patients with disease progression within six months, compared to 5/11 patients with no residual disease and 6/13 patients with progression after six months. Finally, mutations were detected at progression in 5/6 patients, but not during chemotherapy. NGS with molecular barcoding and dPCR were most optimal workflows to detect TP53 mutations in baseline and longitudinal serum cfDNA, respectively. TP53 mutations were undetectable in cfDNA during treatment but re-appeared at disease progression, illustrating its promise as a biomarker for disease monitoring.

Published
2020
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29. Adherence to Active Surveillance Protocols for Low-risk Prostate Cancer: Results of the Movember Foundation's Global Action Plan Prostate Cancer Active Surveillance Initiative.

Author

Harkin T., Bangma C.H., Steyerberg E.W., Helleman J., Frydenberg M., Roobol M.J., Kalapara A.A., Verbeek J.F.M., Nieboer D., Fahey M., Gnanapragasam V., Van Hemelrijck M., Lee L.S., Harkin T., Bangma C.H., Steyerberg E.W., Helleman J., Frydenberg M., Roobol M.J., Kalapara A.A., Verbeek J.F.M., Nieboer D., Fahey M., Gnanapragasam V., Van Hemelrijck M., and Lee L.S.

Abstract

Background: Active surveillance (AS) enrolment criteria and follow-up schedules for low-risk prostate cancer vary between institutions. However, uncertainty remains about adherence to these protocols. Objective(s): To determine adherence to institution-specific AS inclusion criteria and follow-up schedules within the Movember Foundation's Global Action Plan Prostate Cancer Active Surveillance (GAP3) initiative. Design, setting, and participants: We retrospectively assessed the data of 15 101 patients from 25 established AS cohorts worldwide between 2014 and 2016. Outcome measurements and statistical analysis: Adherence to individual AS inclusion criteria was rated on a five-point Likert scale ranging from poor to excellent. Nonadherence to follow-up schedules was defined as absence of repeat biopsy 1 yr after the scheduled date. Cohorts were pooled into annual and Prostate Cancer Research International: Active Surveillance (PRIAS)-based biopsy schedules, and a generalised linear mixed model was constructed to test for nonadherence. Results and limitations: Serum prostate-specific antigen (PSA) inclusion criteria were followed in 92%, Gleason score (GS) criteria were followed in 97%, and the number of positive biopsy cores was followed in 94% of men. Both age and tumour stage (T stage) criteria had 99% adherence overall. Pooled nonadherence rates increased over time-8%, 16%, and 34% for annual schedules and 11%, 30%, and 29% for PRIAS-based schedules at 1, 4, and 7 yr, respectively-and did not differ between biopsy schedules. A limitation is that our results do not consider the use of multiparametric magnetic resonance imaging. Conclusion(s): In on-going development of evidence-based AS protocols, variable adherence to PSA and GS inclusion criteria should be considered. Repeat biopsy adherence reduces with increased duration of surveillance, independent of biopsy frequency. This emphasises the importance of risk stratification at the commencement of AS. Patient Summa

Published
2020

31. Consistent Biopsy Quality and Gleason Grading Within the Global Active Surveillance Global Action Plan 3 Initiative: A Prerequisite for Future Studies.

Author

Rannikko A., Moore C.M., Gnanapragasam V., Van Hemelrijck M., Dasgupta P., Bangma C., Villers A., Valdagni R., Perry A., Hugosson J., Rubio-Briones J., Bjartell A., Hefermehl L., Shiong L.L., Frydenberg M., Kakehi Y., Chung B.H., Obbink H., van der Linden W., Hulsen T., de Jonge C., Kattan M., Xinge J., Muir K., Lophatananon A., Fahey M., Steyerberg E., Zhang L., Guo W., Benfante N., Cowan J., Patil D., Tolosa E., Kim T.-K., Mamedov A., Lapointe V., Crump T., Kimberly-Duffell J., Santaolalla A., Olivier J., Rancati T., Ahlgren H., Mascaros J., Lofgren A., Lehmann K., Lin C.H., Hirama H., Lee K.S., Jenster G., Auvinen A., Haider M., van Bochove K., Carter B., Gledhill S., Buzza M., van der Kwast T.H., Helleman J., Nieboer D., Bruinsma S.M., Roobol M.J., Trock B., Ehdaie B., Carroll P., Filson C., Kim J., Logothetis C., Morgan T., Klotz L., Pickles T., Hyndman E., Rannikko A., Moore C.M., Gnanapragasam V., Van Hemelrijck M., Dasgupta P., Bangma C., Villers A., Valdagni R., Perry A., Hugosson J., Rubio-Briones J., Bjartell A., Hefermehl L., Shiong L.L., Frydenberg M., Kakehi Y., Chung B.H., Obbink H., van der Linden W., Hulsen T., de Jonge C., Kattan M., Xinge J., Muir K., Lophatananon A., Fahey M., Steyerberg E., Zhang L., Guo W., Benfante N., Cowan J., Patil D., Tolosa E., Kim T.-K., Mamedov A., Lapointe V., Crump T., Kimberly-Duffell J., Santaolalla A., Olivier J., Rancati T., Ahlgren H., Mascaros J., Lofgren A., Lehmann K., Lin C.H., Hirama H., Lee K.S., Jenster G., Auvinen A., Haider M., van Bochove K., Carter B., Gledhill S., Buzza M., van der Kwast T.H., Helleman J., Nieboer D., Bruinsma S.M., Roobol M.J., Trock B., Ehdaie B., Carroll P., Filson C., Kim J., Logothetis C., Morgan T., Klotz L., Pickles T., and Hyndman E.

Abstract

Within the Movember Foundation's Global Action Plan Prostate Cancer Active Surveillance (GAP3) initiative, 25 centers across the globe collaborate to standardize active surveillance (AS) protocols for men with low-risk prostate cancer (PCa). A centralized PCa AS database, comprising data of more than 15 000 patients worldwide, was created. Comparability of the histopathology between the different cohorts was assessed by a centralized pathology review of 445 biopsies from 15 GAP3 centers. Grade group 1 (Gleason score 6) in 85% and grade group >=2 (Gleason score >=7) in 15% showed 89% concordance at review with moderate agreement (kappa = 0.56). Average biopsy core length was similar among the analyzed cohorts. Recently established highly adverse pathologies, including cribriform and/or intraductal carcinoma, were observed in 3.6% of the reviewed biopsies. In conclusion, the centralized pathology review of 445 biopsies revealed comparable histopathology among the 15 GAP3 centers with a low frequency of high-risk features. This enables further data analyses-without correction-toward uniform global AS guidelines for men with low-risk PCa. Patient Summary: Movember Foundation's Global Action Plan Prostate Cancer Active Surveillance (GAP3) initiative combines data from 15 000 men with low-risk prostate cancer (PCa) across the globe to standardize active surveillance protocols. Histopathology review confirmed that the histopathology was consistent with low-risk PCa in most men and comparable between different centers. A centralized pathological review showed consistent biopsy quality and Gleason grading within the global active surveillance Global Action Plan 3 initiative, a prerequisite for future studies toward uniform global guidelines for active surveillance of men with low-risk prostate cancer.Copyright © 2018

Published
2019

32. Reasons for Discontinuing Active Surveillance: Assessment of 21 Centres in 12 Countries in the Movember GAP3 Consortium.

Author

Perry A., Gledhill S., Morgan T., Klotz L., Pickles T., Hyndman E., Moore C.M., Dasgupta P., Villers A., Valdagni R., Carter B., Hugosson J., Rubio-Briones J., Bjartell A., Hefermehl L., Lui Shiong L., Kakehi Y., Ha Chung B., van der Kwast T., Obbink H., Hulsen T., de Jonge C., Xinge J., Muir K., Lophatananon A., Steyerberg E., Zhang L., Santa Olalla A., Beckmann K., Denton B., Hayen A., Boutros P., Guo W., Benfante N., Cowan J., Patil D., Tolosa E., Kim T.-K., Mamedov A., La Pointe V., Crump T., Kimberly-Duffell J., Santaolalla A., Olivier J., Rancati T., Ahlgren H., Mascaros J., Lofgren A., Lehmann K., Han Lin C., Hirama H., Suk Lee K., Jenster G., Auvinen A., Haider M., van Bochove K., Buzza M., Bangma C., Bruinsma S., Fahey M., Van Hemelrijck M., Ji X., Kattan M.W., Helleman J., Roobol M.J., Nieboer D., Bangma C.H., van der Linden W., Frydenberg M., Rannikko A., Lee L.S., Gnanapragasam V.J., Trock B., Ehdaie B., Carroll P., Filson C., Kim J., Logothetis C., Perry A., Gledhill S., Morgan T., Klotz L., Pickles T., Hyndman E., Moore C.M., Dasgupta P., Villers A., Valdagni R., Carter B., Hugosson J., Rubio-Briones J., Bjartell A., Hefermehl L., Lui Shiong L., Kakehi Y., Ha Chung B., van der Kwast T., Obbink H., Hulsen T., de Jonge C., Xinge J., Muir K., Lophatananon A., Steyerberg E., Zhang L., Santa Olalla A., Beckmann K., Denton B., Hayen A., Boutros P., Guo W., Benfante N., Cowan J., Patil D., Tolosa E., Kim T.-K., Mamedov A., La Pointe V., Crump T., Kimberly-Duffell J., Santaolalla A., Olivier J., Rancati T., Ahlgren H., Mascaros J., Lofgren A., Lehmann K., Han Lin C., Hirama H., Suk Lee K., Jenster G., Auvinen A., Haider M., van Bochove K., Buzza M., Bangma C., Bruinsma S., Fahey M., Van Hemelrijck M., Ji X., Kattan M.W., Helleman J., Roobol M.J., Nieboer D., Bangma C.H., van der Linden W., Frydenberg M., Rannikko A., Lee L.S., Gnanapragasam V.J., Trock B., Ehdaie B., Carroll P., Filson C., Kim J., and Logothetis C.

Abstract

Background: Careful assessment of the reasons for discontinuation of active surveillance (AS) is required for men with prostate cancer (PCa). Objective(s): Using Movember's Global Action Plan Prostate Cancer Active Surveillance initiative (GAP3) database, we report on reasons for AS discontinuation. Design, setting, and participants: We compared data from 10 296 men on AS from 21 centres across 12 countries. Outcome measurements and statistical analysis: Cumulative incidence methods were used to estimate the cumulative incidence rates of AS discontinuation. Results and limitations: During 5-yr follow-up, 27.5% (95% confidence interval [CI]: 26.4-28.6%) men showed signs of disease progression, 12.8% (95% CI: 12.0-13.6%) converted to active treatment without evidence of progression, 1.7% (95% CI: 1.5-2.0%) continued to watchful waiting, and 1.7% (95% CI: 1.4-2.1%) died from other causes. Of the 7049 men who remained on AS, 2339 had follow-up for >5 yr, 4561 had follow-up for <5 yr, and 149 were lost to follow-up. Cumulative incidence of progression was 27.5% (95% CI: 26.4-28.6%) at 5 yr and 38.2% (95% CI: 36.7-39.9%) at 10 yr. A limitation is that not all centres were included due to limited information on the reason for discontinuation and limited follow-up. Conclusion(s): Our descriptive analyses of current AS practices worldwide showed that 43.6% of men drop out of AS during 5-yr follow-up, mainly due to signs of disease progression. Improvements in selection tools for AS are thus needed to correctly allocate men with PCa to AS, which will also reduce discontinuation due to conversion to active treatment without evidence of disease progression. Patient Summary: Our assessment of a worldwide database of men with prostate cancer (PCa) on active surveillance (AS) shows that 43.6% drop out of AS within 5 yr, mainly due to signs of disease progression. Better tools are needed to select and monitor men with PCa as part of AS. After about 5 yr, about 56% of men were still

Published
2019

33. Predicting Biopsy Outcomes During Active Surveillance for Prostate Cancer: External Validation of the Canary Prostate Active Surveillance Study Risk Calculators in Five Large Active Surveillance Cohorts.

Author

Santaolalla A., Gnanapragasam V., Van Hemelrijck M., Dasgupta P., Auvinen A., Haider M., van Bochove K., Carter B., Gledhill S., Buzza M., Bruinsma S., Helleman J., Drost F.-J.H., Nieboer D., Morgan T.M., Carroll P.R., Roobol M.J., Trock B., Ehdaie B., Carroll P., Filson C., Kim J., Logothetis C., Morgan T., Klotz L., Pickles T., Hyndman E., Bangma C., Roobol M., Villers A., Rannikko A., Valdagni R., Perry A., Hugosson J., Rubio-Briones J., Bjartell A., Hefermehl L., Shiong L.L., Frydenberg M., Kakehi Y., Chung B.H., van der Kwast T., van der Linden W., Hulsen T., de Jonge C., Kattan M., Xinge J., Muir K., Lophatananon A., Fahey M., Steyerberg E., Zhang L., Beckmann K., Denton B., Hayen A., Boutros P., Guo W., Benfante N., Cowan J., Patil D., Tolosa E., Kim T.-K., Mamedov A., Lapointe V., Crump T., Kimberly-Duffell J., Olivier J., Rancati T., Ahlgren H., Mascaros J., Lofgren A., Lin C.H., Hirama H., Lee K.S., Moore C.M., Jenster G., Santaolalla A., Gnanapragasam V., Van Hemelrijck M., Dasgupta P., Auvinen A., Haider M., van Bochove K., Carter B., Gledhill S., Buzza M., Bruinsma S., Helleman J., Drost F.-J.H., Nieboer D., Morgan T.M., Carroll P.R., Roobol M.J., Trock B., Ehdaie B., Carroll P., Filson C., Kim J., Logothetis C., Morgan T., Klotz L., Pickles T., Hyndman E., Bangma C., Roobol M., Villers A., Rannikko A., Valdagni R., Perry A., Hugosson J., Rubio-Briones J., Bjartell A., Hefermehl L., Shiong L.L., Frydenberg M., Kakehi Y., Chung B.H., van der Kwast T., van der Linden W., Hulsen T., de Jonge C., Kattan M., Xinge J., Muir K., Lophatananon A., Fahey M., Steyerberg E., Zhang L., Beckmann K., Denton B., Hayen A., Boutros P., Guo W., Benfante N., Cowan J., Patil D., Tolosa E., Kim T.-K., Mamedov A., Lapointe V., Crump T., Kimberly-Duffell J., Olivier J., Rancati T., Ahlgren H., Mascaros J., Lofgren A., Lin C.H., Hirama H., Lee K.S., Moore C.M., and Jenster G.

Abstract

Two active surveillance risk calculators to predict disease reclassification on prostate biopsy are externally validated by the Movember Foundation's Global Action Plan (GAP3) consortium. They proved to be clinically useful and could reduce unnecessary biopsies, but need recalibration to local settings. Background: Men with prostate cancer (PCa) on active surveillance (AS) are followed through regular prostate biopsies, a burdensome and often unnecessary intervention, not without risks. Identifying men with at a low risk of disease reclassification may help reduce the number of biopsies. Objective(s): To assess the external validity of two Canary Prostate Active Surveillance Study Risk Calculators (PASS-RCs), which estimate the probability of reclassification (Gleason grade >=7 with or without >34% of biopsy cores positive for PCa) on a surveillance biopsy, using a mix of months since last biopsy, age, body mass index, prostate-specific antigen, prostate volume, number of prior negative biopsies, and percentage (or ratio) of positive cores on last biopsy. Design, setting, and participants: We used data up to November 2017 from the Movember Foundation's Global Action Plan (GAP3) consortium, a global collaboration between AS studies. Outcome measurements and statistical analysis: External validity of the PASS-RCs for estimating reclassification on biopsy was assessed by calibration, discrimination, and decision curve analyses. Results and limitations: Five validation cohorts (Prostate Cancer Research International: Active Surveillance, Johns Hopkins, Toronto, Memorial Sloan Kettering Cancer Center, and University of California San Francisco), comprising 5105 men on AS, were eligible for analysis. The individual cohorts comprised 429-2416 men, with a median follow-up between 36 and 84 mo, in both community and academic practices mainly from western countries. Abilities of the PASS-RCs to discriminate between men with and without reclassification on biopsy were reasonab

Published
2019

34. Concordance of cribriform architecture in matched prostate cancer biopsy and radical prostatectomy specimens

Author

Hollemans, E. (Eva), Verhoef, E.I. (Esther), Bangma, C.H. (Chris), Schoots, I.G. (Ivo), Rietbergen, J.B. (John), Helleman, J. (Jozien), Roobol-Bouts, M.J. (Monique), Leenders, G.J.H.L. (Geert), Hollemans, E. (Eva), Verhoef, E.I. (Esther), Bangma, C.H. (Chris), Schoots, I.G. (Ivo), Rietbergen, J.B. (John), Helleman, J. (Jozien), Roobol-Bouts, M.J. (Monique), and Leenders, G.J.H.L. (Geert)

Abstract

Aims: Invasive cribriform and/or intraductal carcinoma have been identified as independent adverse parameters for prostate cancer outcome. Little is known on biopsy undersampling of cribriform architecture. Our aim was to determine the extent of cribriform architecture undersampling and to find predictive factors for identifying false cribriform-negative cases. Methods and results: We reviewed 186 matched prostate biopsies and radical prostatectomy specimens. Of 97 biopsy grade group 2 (Gleason score 3 + 4 = 7) patients, 22 (23%) had true cribriform-negative (TN), 39 (40%) false-negative (FN) and 36 (37%) true-positive (TP) biopsies. Patients with FN biopsies had higher, although not statistically significant (P = 0.06), median PSA levels than patients with TP biopsies (12 versus 8 ng/ml). A PI-RADS 5 lesion was present in nine of 16 (54%) FN and three of 11 (27%) TN biopsies (P = 0.05). Positive biopsy rate (P = 0.47), percentage Gleason pattern 4 (P = 0.55) and glomeruloid architecture (P = 1.0) were not different. Logistic regression identified PSA as an independent pre

Published
2019
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45. Molecular profiling of platinum resistant ovarian cancer

Author

Helleman, J., Jansen, M.P.H.M., Span, P.N., Staveren, I.L. van, Massuger, L.F.A.G., Meijer-van Gelder, M.E., Sweep, C.G.J., Ewing, P.C., Burg, M.E.L. van der, Stoter, G., Nooter, K., and Berns, E.M.J.J.

Subjects
Hereditary cancer and cancer-related syndromes [ONCOL 1], Translational research [ONCOL 3], Endocrinology and reproduction [UMCN 5.2], Hormonal regulation [IGMD 6], Immunotherapy, gene therapy and transplantation [UMCN 1.4], Aetiology, screening and detection [ONCOL 5]
Abstract

Contains fulltext : 50492.pdf (Publisher’s version ) (Closed access) The aim of this study is to discover a gene set that can predict resistance to platinum-based chemotherapy in ovarian cancer. The study was performed on 96 primary ovarian adenocarcinoma specimens from 2 hospitals all treated with platinum-based chemotherapy. In our search for genes, 24 specimens of the discovery set (5 nonresponders and 19 responders) were profiled in duplicate with 18K cDNA microarrays. Confirmation was done using quantitative RT-PCR on 72 independent specimens (9 nonresponders and 63 responders). Sixty-nine genes were differentially expressed between the nonresponders (n=5) and the responders (n=19) in the discovery phase. An algorithm was constructed to identify predictive genes in this discovery set. This resulted in 9 genes (FN1, TOP2A, LBR, ASS, COL3A1, STK6, SGPP1, ITGAE, PCNA), which were confirmed with qRT-PCR. This gene set predicted platinum resistance in an independent validation set of 72 tumours with a sensitivity of 89% (95% CI: 0.68-1.09) and a specificity of 59% (95% CI: 0.47-0.71)(OR=0.09, p=0.026). Multivariable analysis including patient and tumour characteristics demonstrated that this set of 9 genes is independent for the prediction of resistance (p

Published
2006
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47. APOBEC3G expression correlates with T-cell infiltration and improved clinical outcomes in high-grade serous ovarian carcinoma

Author

Leonard, B. (Brandon), Starrett, G.J. (Gabriel J.), Maurer, M.J. (Matthew J.), Oberg, A.L. (Ann L.), Van Bockstal, M. (Mieke), Van Dorpe, J. (Jo), De Wever, O. (Olivier), Helleman, J. (Jozien), Sieuwerts, A.M. (Anieta), Berns, P.M.J.J. (Els), Martens, J.W.M. (John), Anderson, B.D. (Brett D.), Brown, W.L. (William L.), Kalli, K.R. (Kimberly R.), Kaufmann, S.H. (Scott H.), Harris, R.S. (Reuben), Leonard, B. (Brandon), Starrett, G.J. (Gabriel J.), Maurer, M.J. (Matthew J.), Oberg, A.L. (Ann L.), Van Bockstal, M. (Mieke), Van Dorpe, J. (Jo), De Wever, O. (Olivier), Helleman, J. (Jozien), Sieuwerts, A.M. (Anieta), Berns, P.M.J.J. (Els), Martens, J.W.M. (John), Anderson, B.D. (Brett D.), Brown, W.L. (William L.), Kalli, K.R. (Kimberly R.), Kaufmann, S.H. (Scott H.), and Harris, R.S. (Reuben)

Abstract

__Purpose:__ APOBEC3 DNA cytosine deaminase family members normally defend against viruses and transposons. However, deregulated APOBEC3 activity causes mutations in cancer. Because of broad expression profiles and varying mixtures of normal and cancer cells in tumors, including immune cell infiltration, it is difficult to determine where different APOBEC3s are expressed. Here, we ask whether correlations exist between APOBEC3 expression and T-cell infiltration in high-grade serous ovarian cancer (HGSOC), and assess whether these correlations have prognostic value. __Experimental Design:__ Transcripts for APOBEC3G, APOBEC3B, and the T-cell markers, CD3D, CD4, CD8A, GZMB, PRF1, and RNF128 were quantified by RT-qPCR for a cohort of 354 HGSOC patients. Expression values were correlated with each other and clinical parameters. Two additional cohorts were used to extend HGSOC clinical results. Immunoimaging was used to colocalize APOBEC3G and the T-cell marker CD3. TCGA data extended expression analyses to additional cancer types. __Results:__ A surprising positive correlation was found for expression of APOBEC3G and several T cell genes in HGSOC. Immunohistochemistry and immunofluorescent imaging showed protein colocalization in tumor-infiltrating T lymphocytes. High APOBEC3G expression correlated with improved outcomes in multiple HGSOC cohorts. TCGA data analyses revealed that expression of APOBEC3D and APOBEC3H also correlates with CD3D across multiple cancer types. __Conclusions:__ Our results identify APOBEC3G as a new candidate biomarker for tumor-infiltrating T lymphocytes and favorable prognoses for HGSOC. Our data also highlight the complexity of the tumor environment with respect to differential APOBEC family gene expression in both tumor and surrounding normal cell types. Clin Cancer Res; 22(18); 4746-55.

Published
2016
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