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1. Aggressive fluid hydration plus non-steroidal anti-inflammatory drugs versus non-steroidal anti-inflammatory drugs alone for post-endoscopic retrograde cholangiopancreatography pancreatitis (FLUYT): a multicentre, open-label, randomised, controlled trial

Author

Sperna Weiland, Christina J, Smeets, Xavier J N M, Kievit, Wietske, Verdonk, Robert C, Poen, Alexander C, Bhalla, Abha, Venneman, Niels G, Witteman, Ben J M, da Costa, David W, van Eijck, Brechje C, Schwartz, Matthijs P, Römkens, Tessa E H, Vrolijk, Jan Maarten, Hadithi, Muhammed, Voorburg, Annet M C J, Baak, Lubbertus C, Thijs, Willem J, van Wanrooij, Roy L, Tan, Adriaan C I T L, Seerden, Tom C J, Keulemans, Yolande C A, de Wijkerslooth, Thomas R, van de Vrie, Wim, van der Schaar, Peter, van Dijk, Sven M, Hallensleben, Nora D L, Sperna Weiland, Ruud L, Timmerhuis, Hester C, Umans, Devica S, van Hooft, Jeanin E, van Goor, Harry, van Santvoort, Hjalmar C, Besselink, Marc G, Bruno, Marco J, Fockens, Paul, Drenth, Joost P H, and van Geenen, Erwin J M

Published
2021
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2. Short-term and Long-term Outcomes of a Disruption and Disconnection of the Pancreatic Duct in Necrotizing Pancreatitis: A Multicenter Cohort Study in 896 Patients

Author

Timmerhuis, Hester C, van Dijk, Sven M, Hollemans, Robbert A, Sperna Weiland, Christina J, Umans, Devica S, Boxhoorn, Lotte, Hallensleben, Nora H, van der Sluijs, Rogier, Brouwer, Lieke, van Duijvendijk, Peter, Kager, Liesbeth, Kuiken, Sjoerd, Poley, Jan-Werner, de Ridder, Rogier, Römkens, Tessa, Quispel, Rutger, Schwartz, Matthijs P, Tan, Adriaan C I T L, Venneman, Niels G, Vleggaar, Frank P, van Wanrooij, Roy L J, Witteman, Ben J, van Geenen, Erwin, Molenaar, I Quintus, Bruno, Marco J, van Hooft, Jeanin E, Besselink, Marc G, Voermans, Rogier P, Bollen, Thomas L, Verdonk, Robert C, van Santvoort, Hjalmar C, Dutch Pancreatitis Study Group, Timmerhuis, Hester C, van Dijk, Sven M, Hollemans, Robbert A, Sperna Weiland, Christina J, Umans, Devica S, Boxhoorn, Lotte, Hallensleben, Nora H, van der Sluijs, Rogier, Brouwer, Lieke, van Duijvendijk, Peter, Kager, Liesbeth, Kuiken, Sjoerd, Poley, Jan-Werner, de Ridder, Rogier, Römkens, Tessa, Quispel, Rutger, Schwartz, Matthijs P, Tan, Adriaan C I T L, Venneman, Niels G, Vleggaar, Frank P, van Wanrooij, Roy L J, Witteman, Ben J, van Geenen, Erwin, Molenaar, I Quintus, Bruno, Marco J, van Hooft, Jeanin E, Besselink, Marc G, Voermans, Rogier P, Bollen, Thomas L, Verdonk, Robert C, van Santvoort, Hjalmar C, and Dutch Pancreatitis Study Group

Abstract

INTRODUCTION:Necrotizing pancreatitis may result in a disrupted or disconnected pancreatic duct (DPD) with the potential for long-lasting negative impact on a patient's clinical outcome. There is a lack of detailed data on the full clinical spectrum of DPD, which is critical for the development of better diagnostic and treatment strategies.METHODS:We performed a long-term post hoc analysis of a prospectively collected nationwide cohort of 896 patients with necrotizing pancreatitis (2005-2015). The median follow-up after hospital admission was 75 months (P25-P75: 41-151). Clinical outcomes of patients with and without DPD were compared using regression analyses, adjusted for potential confounders. Predictive features for DPD were explored.RESULTS:DPD was confirmed in 243 (27%) of the 896 patients and resulted in worse clinical outcomes during both the patient's initial admission and follow-up. During hospital admission, DPD was associated with an increased rate of new-onset intensive care unit admission (adjusted odds ratio [aOR] 2.52; 95% confidence interval [CI] 1.62-3.93), new-onset organ failure (aOR 2.26; 95% CI 1.45-3.55), infected necrosis (aOR 4.63; 95% CI 2.87-7.64), and pancreatic interventions (aOR 7.55; 95% CI 4.23-13.96). During long-term follow-up, DPD increased the risk of pancreatic intervention (aOR 9.71; 95% CI 5.37-18.30), recurrent pancreatitis (aOR 2.08; 95% CI 1.32-3.29), chronic pancreatitis (aOR 2.73; 95% CI 1.47-5.15), and endocrine pancreatic insufficiency (aOR 1.63; 95% CI 1.05-2.53). Central or subtotal pancreatic necrosis on computed tomography (OR 9.49; 95% CI 6.31-14.29) and a high level of serum C-reactive protein in the first 48 hours after admission (per 10-point increase, OR 1.02; 95% CI 1.00-1.03) were identified as independent predictors for developing DPD.DISCUSSION:At least 1 of every 4 patients with necrotizing pancreatitis experience DPD, which is associated with detrimental, short-term and long-term interventions, and comp

Published
2023

3. Short- and long-term outcomes of a disruption and disconnection of the pancreatic duct in necrotizing pancreatitis: a multicenter cohort study in 896 patients : Disrupted pancreatic duct in acute pancreatitis

Author

Timmerhuis, Hester C, van Dijk, Sven M, Hollemans, Robbert A, Sperna Weiland, Christina J, Umans, Devica S, Boxhoorn, Lotte, Hallensleben, Nora H, van der Sluijs, Rogier, Brouwer, Lieke, van Duijvendijk, Peter, Kager, Liesbeth, Kuiken, Sjoerd, Poley, Jan-Werner, de Ridder, Rogier, Römkens, Tessa, Quispel, Rutger, Schwartz, Matthijs P, Tan, Adriaan C I T L, Venneman, Niels G, Vleggaar, Frank P, van Wanrooij, Roy L J, Witteman, Ben J, van Geenen, Erwin, Molenaar, I Quintus, Bruno, Marco J, van Hooft, Jeanin E, Besselink, Marc G, Voermans, Rogier P, Bollen, Thomas L, Verdonk, Robert C, van Santvoort, Hjalmar C, RS: FHML non-thematic output, MUMC+: MA Maag Darm Lever (9), and Interne Geneeskunde

Abstract

INTRODUCTION:Necrotizing pancreatitis may result in a disrupted or disconnected pancreatic duct (DPD) with the potential for long-lasting negative impact on a patient's clinical outcome. There is a lack of detailed data on the full clinical spectrum of DPD, which is critical for the development of better diagnostic and treatment strategies.METHODS:We performed a long-term post hoc analysis of a prospectively collected nationwide cohort of 896 patients with necrotizing pancreatitis (2005-2015). The median follow-up after hospital admission was 75 months (P25-P75: 41-151). Clinical outcomes of patients with and without DPD were compared using regression analyses, adjusted for potential confounders. Predictive features for DPD were explored.RESULTS:DPD was confirmed in 243 (27%) of the 896 patients and resulted in worse clinical outcomes during both the patient's initial admission and follow-up. During hospital admission, DPD was associated with an increased rate of new-onset intensive care unit admission (adjusted odds ratio [aOR] 2.52; 95% confidence interval [CI] 1.62-3.93), new-onset organ failure (aOR 2.26; 95% CI 1.45-3.55), infected necrosis (aOR 4.63; 95% CI 2.87-7.64), and pancreatic interventions (aOR 7.55; 95% CI 4.23-13.96). During long-term follow-up, DPD increased the risk of pancreatic intervention (aOR 9.71; 95% CI 5.37-18.30), recurrent pancreatitis (aOR 2.08; 95% CI 1.32-3.29), chronic pancreatitis (aOR 2.73; 95% CI 1.47-5.15), and endocrine pancreatic insufficiency (aOR 1.63; 95% CI 1.05-2.53). Central or subtotal pancreatic necrosis on computed tomography (OR 9.49; 95% CI 6.31-14.29) and a high level of serum C-reactive protein in the first 48 hours after admission (per 10-point increase, OR 1.02; 95% CI 1.00-1.03) were identified as independent predictors for developing DPD.DISCUSSION:At least 1 of every 4 patients with necrotizing pancreatitis experience DPD, which is associated with detrimental, short-term and long-term interventions, and complications. Central and subtotal pancreatic necrosis and high levels of serum C-reactive protein in the first 48 hours are independent predictors for DPD.

Published
2023

4. Overuse and Misuse of Antibiotics and the Clinical Consequence in Necrotizing Pancreatitis.

Author

Timmerhuis, Hester C., den Berg, Fons F. van, Noorda, Paula C., van Dijk, Sven M., van Grinsven, Janneke, Weiland, Christina J. Sperna, Umans, Devica S., Mohamed, Yasmin A., Curvers, Wouter L., Bouwense, Stefan A. W., Hadithi, Muhammed, Inderson, Akin, Issa, Yama, Jansen, Jeroen M., de Jonge, Pieter Jan F., Quispel, Rutger, Schwartz, Matthijs P., Stommel, Martijn W. J., Tan, Adriaan C. I. T. L., and Venneman, Niels G.

Abstract

Objective: The use and impact of antibiotics and the impact of causative pathogens on clinical outcomes in a large real-world cohort covering the entire clinical spectrum of necrotizing pancreatitis remain unknown. Summary Background Data: International guidelines recommend broadspectrum antibiotics in patients with suspected infected necrotizing pancreatitis. This recommendation is not based on high-level evidence and clinical effects are unknown. Materials and Methods: This study is a post-hoc analysis of a nationwide prospective cohort of 401 patients with necrotizing pancreatitis in 15 Dutch centers (2010-2019). Across the patient population from the time of admission to 6 months postadmission, multivariable regression analyses were used to analyze (1) microbiological cultures and (2) antibiotic use. Results: Antibiotics were started in 321/401 patients (80%) administered at a median of 5 days (P25-P75: 1-13) after admission. The median duration of antibiotics was 27 days (P25-P75: 15-48). In 221/321 patients (69%) infection was not proven by cultures at the time of initiation of antibiotics. Empirical antibiotics for infected necrosis provided insuffi- cient coverage in 64/128 patients (50%) with a pancreatic culture. Prolonged antibiotic therapy was associated with Enterococcus infection (OR 1.08 [95% CI 1.03-1.16], P=0.01). Enterococcus infection was associated with new/persistent organ failure (OR 3.08 [95% CI 1.35-7.29], P< 0.01) and mortality (OR 5.78 [95% CI 1.46-38.73], P=0.03). Yeast was found in 30/147 cultures (20%). Discussion: In this nationwide study of patients with necrotizing pancreatitis, the vast majority received antibiotics, typically administered early in the disease course and without a proven infection. Empirical antibiotics were inappropriate based on pancreatic cultures in half the patients. Future clinical research and practice must consider antibiotic selective pressure due to prolonged therapy and coverage of Enterococcus and yeast. Improved guidelines on antimicrobial diagnostics and therapy could reduce inappropriate antibiotic use and improve clinical outcomes. [ABSTRACT FROM AUTHOR]

Published
2023
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5. Patient selection for urgent endoscopic retrograde cholangio-pancreatography by endoscopic ultrasound in predicted severe acute biliary pancreatitis (APEC-2): a multicentre prospective study

Author

Hallensleben, Nora D, primary, Stassen, Pauline M C, additional, Schepers, Nicolien J, additional, Besselink, Marc G, additional, Anten, Marie-Paule G F, additional, Bakker, Olaf J, additional, Bollen, Thomas L, additional, da Costa, David W, additional, van Dijk, Sven M, additional, van Dullemen, Hendrik M, additional, Dijkgraaf, Marcel G W, additional, van Eijck, Brechje, additional, van Eijck, Casper H J, additional, Erkelens, Willemien, additional, Erler, Nicole S, additional, Fockens, Paul, additional, van Geenen, Erwin-Jan M, additional, van Grinsven, Janneke, additional, Hazen, Wouter L, additional, Hollemans, Robbert A, additional, van Hooft, Jeanin E, additional, Jansen, Jeroen M, additional, Kubben, Frank J G M, additional, Kuiken, Sjoerd D, additional, Poen, Alexander C, additional, Quispel, Rutger, additional, de Ridder, Rogier J, additional, Römkens, Tessa E H, additional, Schoon, Erik J, additional, Schwartz, Matthijs P, additional, Seerden, Tom C J, additional, Smeets, Xavier J N M, additional, Spanier, B W Marcel, additional, Tan, Adriaan C I T L, additional, Thijs, Willem J, additional, Timmer, Robin, additional, Umans, Devica S, additional, Venneman, Niels G, additional, Verdonk, Robert C, additional, Vleggaar, Frank P, additional, van de Vrie, Wim, additional, van Wanrooij, Roy L J, additional, Witteman, Ben J, additional, van Santvoort, Hjalmar C, additional, Bouwense, Stefan A W, additional, and Bruno, Marco J, additional

Published
2023
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6. Fluid hydration to prevent post-ERCP pancreatitis in average- to high-risk patients receiving prophylactic rectal NSAIDs (FLUYT trial): study protocol for a randomized controlled trial

Author

Smeets, Xavier J. N. M., da Costa, David W., Fockens, Paul, Mulder, Chris J. J., Timmer, Robin, Kievit, Wietske, Zegers, Marieke, Bruno, Marco J., Besselink, Marc G. H., Vleggaar, Frank P., van der Hulst, Rene W. M., Poen, Alexander C., Heine, Gerbrand D. N., Venneman, Niels G., Kolkman, Jeroen J., Baak, Lubbertus C., Römkens, Tessa E. H., van Dijk, Sven M., Hallensleben, Nora D. L., van de Vrie, Wim, Seerden, Tom C. J., Tan, Adriaan C. I. T. L., Voorburg, Annet M. C. J., Poley, Jan-Werner, Witteman, Ben J., Bhalla, Abha, Hadithi, Muhammed, Thijs, Willem J., Schwartz, Matthijs P., Vrolijk, Jan Maarten, Verdonk, Robert C., van Delft, Foke, Keulemans, Yolande, van Goor, Harry, Drenth, Joost P. H., van Geenen, Erwin J. M., and for the Dutch Pancreatitis Study Group

Published
2018
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7. The additive value of CA19.9 monitoring in a pancreatic cyst surveillance program

Author

Levink, Iris J. M., Jaarsma, Sanne C., Koopmann, Brechtje D. M., Riet, Priscilla A., Overbeek, Kasper A., Meziani, Jihane, Sprij, Marloes L. J. A., Casadei, Riccardo, Ingaldi, Carlo, Polkowski, Marcin, Engels, Megan M. L., Waaij, Laurens A., Carrara, Silvia, Pando, Elizabeth, Vornhülz, Marlies, Honkoop, Pieter, Schoon, Erik J., Laukkarinen, Johanna, Bergmann, Jilling F., Rossi, Gemma, Vilsteren, Frederike G. I., Berkel, Anne‐Marie, Tabone, Trevor, Schwartz, Matthijs P., Tan, Adriaan C. I. T. L., Hooft, Jeanin E., Quispel, Rutger, Soest, Ellert, Czacko, Laszlo, Bruno, Marco J., and Cahen, Djuna L.

Abstract

Surveillance of pancreatic cysts focuses on the detection of (mostly morphologic) features warranting surgery. European guidelines consider elevated CA19.9 as a relative indication for surgery. We aimed to evaluate the role of CA19.9 monitoring for early detection and management in a cyst surveillance population. The PACYFIC‐registry is a prospective collaboration that investigates the yield of pancreatic cyst surveillance performed at the discretion of the treating physician. We included participants for whom at least one serum CA19.9 value was determined by a minimum follow‐up of 12 months. Of 1865 PACYFIC participants, 685 met the inclusion criteria for this study (mean age 67 years, SD 10; 61% female). During a median follow‐up of 25 months (IQR 24, 1966 visits), 29 participants developed high‐grade dysplasia (HGD) or pancreatic cancer. At baseline, CA19.9 ranged from 1 to 591 kU/L (median 10 kU/L [IQR 14]), and was elevated (≥37 kU/L) in 64 participants (9%). During 191 of 1966 visits (10%), an elevated CA19.9 was detected, and these visits more often led to an intensified follow‐up (42%) than those without an elevated CA19.9 (27%; p< 0.001). An elevated CA19.9 was the sole reason for surgery in five participants with benign disease (10%). The baseline CA19.9 value was (as continuous or dichotomous variable at the 37 kU/L threshold) not independently associated with HGD or pancreatic cancer development, whilst a CA19.9 of ≥ 133 kU/L was (HR 3.8, 95% CI 1.1–13, p= 0.03). In this pancreatic cyst surveillance cohort, CA19.9 monitoring caused substantial harm by shortening surveillance intervals (and performance of unnecessary surgery). The current CA19.9 cutoff was not predictive of HGD and pancreatic cancer, whereas a higher cutoff may decrease false‐positive values. The role of CA19.9 monitoring should be critically appraised prior to implementation in surveillance programs and guidelines.

Published
2023
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8. Short-term and Long-term Outcomes of a Disruption and Disconnection of the Pancreatic Duct in Necrotizing Pancreatitis: A Multicenter Cohort Study in 896 Patients.

Author

Timmerhuis, Hester C., van Dijk, Sven M., Hollemans, Robbert A., Weiland, Christina J. Sperna, Umans, Devica S., Boxhoorn, Lotte, Hallensleben, Nora H., van der Sluijs, Rogier, Brouwer, Lieke, van Duijvendijk, Peter, Kager, Liesbeth, Kuiken, Sjoerd, Poley, Jan-Werner, de Ridder, Rogier, Römkens, Tessa E. H., Quispel, Rutger, Schwartz, Matthijs P., Tan, Adriaan C. I. T. L., Venneman, Niels G., and Vleggaar, Frank P.

Published
2023
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9. Web-Based Educational Intervention for Patients With Uninvestigated Dyspepsia Referred for Upper Gastrointestinal Tract Endoscopy

Author

de Jong, Judith J., primary, Lantinga, Marten A., additional, Tan, Adriaan C. I. T. L., additional, Aquarius, Michel, additional, Scheffer, Robert C. H., additional, Uil, Jan J., additional, de Reuver, Philip R., additional, Keszthelyi, Daniel, additional, Westert, Gert P., additional, Masclee, Ad A. M., additional, and Drenth, Joost P. H., additional

Published
2021
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10. Additional file 2 of Clip placement to prevent delayed bleeding after colonic endoscopic mucosal resection (CLIPPER): study protocol for a randomized controlled trial

Author

Turan, Ayla S., Moons, Leon M. G., Ramon-Michel Schreuder, Schoon, Erik J., Jochim S. Terhaar Sive Droste, Schrauwen, Ruud W. M., Straathof, Jan Willem, Bastiaansen, Barbara A. J., Schwartz, Matthijs P., Hazen, Wouter L., Alkhalaf, Alaa, Allajar, Daud, Hadithi, Muhammed, Spek, Bas W. Van Der, Heine, Dimitri G. D. N., Tan, Adriaan C. I. T. L., Graaf, Wilmar De, Boonstra, Jurjen J., Voogd, Fia J., Roomer, Robert, Ridder, Rogier J. J. De, Kievit, Wietske, Siersema, Peter D., Didden, Paul, and Geenen, Erwin J. M. Van

Abstract

Additional file 2. List of parameters collected in the Case Record Form.

Published
2021
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11. Additional file 1 of Clip placement to prevent delayed bleeding after colonic endoscopic mucosal resection (CLIPPER): study protocol for a randomized controlled trial

Author

Turan, Ayla S., Moons, Leon M. G., Ramon-Michel Schreuder, Schoon, Erik J., Jochim S. Terhaar Sive Droste, Schrauwen, Ruud W. M., Straathof, Jan Willem, Bastiaansen, Barbara A. J., Schwartz, Matthijs P., Hazen, Wouter L., Alkhalaf, Alaa, Allajar, Daud, Hadithi, Muhammed, Spek, Bas W. Van Der, Heine, Dimitri G. D. N., Tan, Adriaan C. I. T. L., Graaf, Wilmar De, Boonstra, Jurjen J., Voogd, Fia J., Roomer, Robert, Ridder, Rogier J. J. De, Kievit, Wietske, Siersema, Peter D., Didden, Paul, and Geenen, Erwin J. M. Van

Abstract

Additional file 1. Definitions of Secondary Endpoints. *Severity of DB was defined according to the ASGE working party document for adverse events in colonoscopy [20].

Published
2021
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12. Additional file 3 of Clip placement to prevent delayed bleeding after colonic endoscopic mucosal resection (CLIPPER): study protocol for a randomized controlled trial

Author

Turan, Ayla S., Moons, Leon M. G., Ramon-Michel Schreuder, Schoon, Erik J., Jochim S. Terhaar Sive Droste, Schrauwen, Ruud W. M., Straathof, Jan Willem, Bastiaansen, Barbara A. J., Schwartz, Matthijs P., Hazen, Wouter L., Alkhalaf, Alaa, Allajar, Daud, Hadithi, Muhammed, Spek, Bas W. Van Der, Heine, Dimitri G. D. N., Tan, Adriaan C. I. T. L., Graaf, Wilmar De, Boonstra, Jurjen J., Voogd, Fia J., Roomer, Robert, Ridder, Rogier J. J. De, Kievit, Wietske, Siersema, Peter D., Didden, Paul, and Geenen, Erwin J. M. Van

Abstract

Additional file 3. SPIRIT Checklist.

Published
2021
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13. Clip placement to prevent delayed bleeding after colonic endoscopic mucosal resection (CLIPPER): study protocol for a randomized controlled trial

Author

MS MDL 1, Cancer, Turan, Ayla S, Moons, Leon M G, Schreuder, Ramon-Michel, Schoon, Erik J, Terhaar Sive Droste, Jochim S, Schrauwen, Ruud W M, Straathof, Jan Willem, Bastiaansen, Barbara A J, Schwartz, Matthijs P, Hazen, Wouter L, Alkhalaf, Alaa, Allajar, Daud, Hadithi, Muhammed, van der Spek, Bas W, Heine, Dimitri G D N, Tan, Adriaan C I T L, de Graaf, Wilmar, Boonstra, Jurjen J, Voogd, Fia J, Roomer, Robert, de Ridder, Rogier J J, Kievit, Wietske, Siersema, Peter D, Didden, Paul, van Geenen, Erwin J M, Dutch EMR Study Group, MS MDL 1, Cancer, Turan, Ayla S, Moons, Leon M G, Schreuder, Ramon-Michel, Schoon, Erik J, Terhaar Sive Droste, Jochim S, Schrauwen, Ruud W M, Straathof, Jan Willem, Bastiaansen, Barbara A J, Schwartz, Matthijs P, Hazen, Wouter L, Alkhalaf, Alaa, Allajar, Daud, Hadithi, Muhammed, van der Spek, Bas W, Heine, Dimitri G D N, Tan, Adriaan C I T L, de Graaf, Wilmar, Boonstra, Jurjen J, Voogd, Fia J, Roomer, Robert, de Ridder, Rogier J J, Kievit, Wietske, Siersema, Peter D, Didden, Paul, van Geenen, Erwin J M, and Dutch EMR Study Group

Published
2021

14. Outcome of Reverse Switching From CT-P13 to Originator Infliximab in Patients With Inflammatory Bowel Disease

Author

Arts-assistenten Kinderen, MS MDL 1, Infection & Immunity, Cancer, Mahmmod, Shaden, Schultheiss, Johannes P D, van Bodegraven, Ad A, Dijkstra, Gerard, Gilissen, Lennard P L, Hoentjen, Frank, Lutgens, Maurice W M D, Mahmmod, Nofel, van der Meulen-de Jong, Andrea E, Smits, Lisa J T, Tan, Adriaan C I T L, Oldenburg, Bas, Fidder, Herma H, Arts-assistenten Kinderen, MS MDL 1, Infection & Immunity, Cancer, Mahmmod, Shaden, Schultheiss, Johannes P D, van Bodegraven, Ad A, Dijkstra, Gerard, Gilissen, Lennard P L, Hoentjen, Frank, Lutgens, Maurice W M D, Mahmmod, Nofel, van der Meulen-de Jong, Andrea E, Smits, Lisa J T, Tan, Adriaan C I T L, Oldenburg, Bas, and Fidder, Herma H

Published
2021

16. Outcome of Reverse Switching From CT-P13 to Originator Infliximab in Patients With Inflammatory Bowel Disease

Author

Mahmmod, Shaden, primary, Schultheiss, Johannes P D, additional, van Bodegraven, Ad A, additional, Dijkstra, Gerard, additional, Gilissen, Lennard P L, additional, Hoentjen, Frank, additional, Lutgens, Maurice W M D, additional, Mahmmod, Nofel, additional, van der Meulen–de Jong, Andrea E, additional, Smits, Lisa J T, additional, Tan, Adriaan C I T L, additional, Oldenburg, Bas, additional, and Fidder, Herma H, additional

Published
2021
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18. Clinical Outcomes of Covid-19 in Patients With Inflammatory Bowel Disease: A Nationwide Cohort Study

Author

Derikx, Lauranne A A P, primary, Lantinga, Marten A, additional, de Jong, Dirk J, additional, van Dop, Willemijn A, additional, Creemers, Rob H, additional, Römkens, Tessa E H, additional, Jansen, Jeroen M, additional, Mahmmod, Nofel, additional, West, Rachel L, additional, Tan, Adriaan C I T L, additional, Bodelier, Alexander G L, additional, Gorter, Moniek H P, additional, Boekema, Paul J, additional, Halet, Eric R C, additional, Horjus, Carmen S, additional, van Dijk, Maarten A, additional, Hirdes, Meike M C, additional, Epping Stippel, Ludger S M, additional, Jharap, Bindia, additional, Lutgens, Maurice W M D, additional, Russel, Maurice G, additional, Gilissen, Lennard P L, additional, Nauta, Sjoukje, additional, van Bodegraven, Adriaan A, additional, and Hoentjen, Frank, additional

Published
2020
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19. Urgent endoscopic retrograde cholangiopancreatography with sphincterotomy versus conservative treatment in predicted severe acute gallstone pancreatitis (APEC): a multicentre randomised controlled trial

Author

Schepers, Nicolien J, primary, Hallensleben, Nora D L, additional, Besselink, Marc G, additional, Anten, Marie-Paule G F, additional, Bollen, Thomas L, additional, da Costa, David W, additional, van Delft, Foke, additional, van Dijk, Sven M, additional, van Dullemen, Hendrik M, additional, Dijkgraaf, Marcel G W, additional, van Eijck, Casper H J, additional, Erkelens, G Willemien, additional, Erler, Nicole S, additional, Fockens, Paul, additional, van Geenen, Erwin J M, additional, van Grinsven, Janneke, additional, Hollemans, Robbert A, additional, van Hooft, Jeanin E, additional, van der Hulst, Rene W M, additional, Jansen, Jeroen M, additional, Kubben, Frank J G M, additional, Kuiken, Sjoerd D, additional, Laheij, Robert J F, additional, Quispel, Rutger, additional, de Ridder, Rogier J J, additional, Rijk, Marno C M, additional, Römkens, Tessa E H, additional, Ruigrok, Carola H M, additional, Schoon, Erik J, additional, Schwartz, Matthijs P, additional, Smeets, Xavier J N M, additional, Spanier, B W Marcel, additional, Tan, Adriaan C I T L, additional, Thijs, Willem J, additional, Timmer, Robin, additional, Venneman, Niels G, additional, Verdonk, Robert C, additional, Vleggaar, Frank P, additional, van de Vrie, Wim, additional, Witteman, Ben J, additional, van Santvoort, Hjalmar C, additional, Bakker, Olaf J, additional, and Bruno, Marco J, additional

Published
2020
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20. Impact of multidisciplinary tumor board discussion on palliation of patients with esophageal or gastro-esophageal junction cancer: a population-based study

Author

Vermeulen, Bram D., primary, Bruggeman, Lukas, additional, Bac, Dirk J., additional, Schrauwen, Ruud W. M., additional, Epping, Ludger S. M., additional, Scheffer, Robert C. H., additional, Tan, Adriaan C. I. T. L., additional, Groenen, Marcel J. M., additional, Verhoeven, Rob H. A., additional, and Siersema, Peter D., additional

Published
2020
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23. Clinical Outcomes of Covid-19 in Patients With Inflammatory Bowel Disease: A Nationwide Cohort Study.

Author

Derikx, Lauranne A A P, Lantinga, Marten A, Jong, Dirk J de, Dop, Willemijn A van, Creemers, Rob H, Römkens, Tessa E H, Jansen, Jeroen M, Mahmmod, Nofel, West, Rachel L, Tan, Adriaan C I T L, Bodelier, Alexander G L, Gorter, Moniek H P, Boekema, Paul J, Halet, Eric R C, Horjus, Carmen S, Dijk, Maarten A van, Hirdes, Meike M C, Stippel, Ludger S M Epping, Jharap, Bindia, and Lutgens, Maurice W M D

Abstract

Background and Aims The COVID-19 risk and disease course in inflammatory bowel disease [IBD] patients remains uncertain. Therefore, we aimed to assess the clinical presentation, disease course, and outcomes of COVID-19 in IBD patients. Second, we determined COVID-19 incidences in IBD patients and compared this with the general population. Methods We conducted a multicentre, nationwide IBD cohort study in The Netherlands and identified patients with COVID-19. First, we assessed the COVID-19 disease course and outcomes. Second, we compared COVID-19 incidences between our IBD study cohort and the general Dutch population. Results We established an IBD cohort of 34 763 patients. COVID-19 was diagnosed in 100/34 763 patients [0.29%]; 20/100 of these patients [20%] had severe COVID-19 defined as admission to the intensive care unit, mechanical ventilation, and/or death. Hospitalisation occurred in 59/100 [59.0%] patients and 13/100 [13.0%] died. All patients who died had comorbidities and all but one were ≥65 years old. In line, we identified ≥1 comorbidity as an independent risk factor for hospitalisation (odds ratio [OR] 4.20, 95% confidence interval [CI] 1.58–11.17,; p = 0.004). Incidences of COVID-19 between the IBD study cohort and the general population were comparable (287.6 [95% CI 236.6–349.7] versus 333.0 [95% CI 329.3–336.7] per 100000 patients, respectively; p = 0.15). Conclusions Of 100 cases with IBD and COVID-19, 20% developed severe COVID-19, 59% were hospitalised and 13% died. A comparable COVID-19 risk was found between the IBD cohort [100/34 763 = 0.29%] and the general Dutch population. The presence of ≥1 comorbidities was an independent risk factor for hospitalisation due to COVID-19. [ABSTRACT FROM AUTHOR]

Published
2021
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24. Fluid hydration to prevent post-ERCP pancreatitis in average- to high-risk patients receiving prophylactic rectal NSAIDs (FLUYT trial) : study protocol for a randomized controlled trial

Author

Smeets, Xavier J N M, da Costa, David W, Fockens, Paul, Mulder, Chris J J, Timmer, Robin, Kievit, Wietske, Zegers, Marieke, Bruno, Marco J, Besselink, Marc G H, Vleggaar, Frank P, van der Hulst, Rene W M, Poen, Alexander C, Heine, Gerbrand D N, Venneman, Niels G, Kolkman, Jeroen J, Baak, Lubbertus C, Römkens, Tessa E H, van Dijk, Sven M, Hallensleben, Nora D L, van de Vrie, Wim, Seerden, Tom C J, Tan, Adriaan C I T L, Voorburg, Annet M C J, Poley, Jan-Werner, Witteman, Ben J, Bhalla, Abha, Hadithi, Muhammed, Thijs, Willem J, Schwartz, Matthijs P, Vrolijk, Jan Maarten, Verdonk, Robert C, van Delft, Foke, Keulemans, Yolande, van Goor, Harry, Drenth, Joost P H, van Geenen, Erwin J M, Dutch Pancreatitis Study Group, Smeets, Xavier J N M, da Costa, David W, Fockens, Paul, Mulder, Chris J J, Timmer, Robin, Kievit, Wietske, Zegers, Marieke, Bruno, Marco J, Besselink, Marc G H, Vleggaar, Frank P, van der Hulst, Rene W M, Poen, Alexander C, Heine, Gerbrand D N, Venneman, Niels G, Kolkman, Jeroen J, Baak, Lubbertus C, Römkens, Tessa E H, van Dijk, Sven M, Hallensleben, Nora D L, van de Vrie, Wim, Seerden, Tom C J, Tan, Adriaan C I T L, Voorburg, Annet M C J, Poley, Jan-Werner, Witteman, Ben J, Bhalla, Abha, Hadithi, Muhammed, Thijs, Willem J, Schwartz, Matthijs P, Vrolijk, Jan Maarten, Verdonk, Robert C, van Delft, Foke, Keulemans, Yolande, van Goor, Harry, Drenth, Joost P H, van Geenen, Erwin J M, and Dutch Pancreatitis Study Group

Published
2018

25. Fluid hydration to prevent post-ERCP pancreatitis in average- to high-risk patients receiving prophylactic rectal NSAIDs (FLUYT trial): study protocol for a randomized controlled trial

Author

Arts-assistenten Radiologie, MS CGO, Cancer, Smeets, Xavier J N M, da Costa, David W, Fockens, Paul, Mulder, Chris J J, Timmer, Robin, Kievit, Wietske, Zegers, Marieke, Bruno, Marco J, Besselink, Marc G H, Vleggaar, Frank P, van der Hulst, Rene W M, Poen, Alexander C, Heine, Gerbrand D N, Venneman, Niels G, Kolkman, Jeroen J, Baak, Lubbertus C, Römkens, Tessa E H, van Dijk, Sven M, Hallensleben, Nora D L, van de Vrie, Wim, Seerden, Tom C J, Tan, Adriaan C I T L, Voorburg, Annet M C J, Poley, Jan-Werner, Witteman, Ben J, Bhalla, Abha, Hadithi, Muhammed, Thijs, Willem J, Schwartz, Matthijs P, Vrolijk, Jan Maarten, Verdonk, Robert C, van Delft, Foke, Keulemans, Yolande, van Goor, Harry, Drenth, Joost P H, van Geenen, Erwin J M, Dutch Pancreatitis Study Group, Arts-assistenten Radiologie, MS CGO, Cancer, Smeets, Xavier J N M, da Costa, David W, Fockens, Paul, Mulder, Chris J J, Timmer, Robin, Kievit, Wietske, Zegers, Marieke, Bruno, Marco J, Besselink, Marc G H, Vleggaar, Frank P, van der Hulst, Rene W M, Poen, Alexander C, Heine, Gerbrand D N, Venneman, Niels G, Kolkman, Jeroen J, Baak, Lubbertus C, Römkens, Tessa E H, van Dijk, Sven M, Hallensleben, Nora D L, van de Vrie, Wim, Seerden, Tom C J, Tan, Adriaan C I T L, Voorburg, Annet M C J, Poley, Jan-Werner, Witteman, Ben J, Bhalla, Abha, Hadithi, Muhammed, Thijs, Willem J, Schwartz, Matthijs P, Vrolijk, Jan Maarten, Verdonk, Robert C, van Delft, Foke, Keulemans, Yolande, van Goor, Harry, Drenth, Joost P H, van Geenen, Erwin J M, and Dutch Pancreatitis Study Group

Published
2018

26. Biochemical efficacy of tioguanine in autoimmune hepatitis: a retrospective review of practice in the Netherlands

Author

van den Brand, Floris F., primary, van Nieuwkerk, Carin M. J., additional, Verwer, Bart J., additional, de Boer, Ynto S., additional, de Boer, Nanne K. H., additional, Mulder, Chris J. J., additional, Bloemena, Elisabeth, additional, Bakker, Christine M., additional, Vrolijk, Jan M., additional, Drenth, Joost P. H., additional, Tan, Adriaan C. I. T. L., additional, ter Borg, Frank, additional, ter Borg, Martijn J., additional, van den Hazel, Sven J., additional, Inderson, Akin, additional, Tushuizen, Maarten E., additional, and Bouma, Gerd, additional

Published
2018
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27. Early biliary decompression versus conservative treatment in acute biliary pancreatitis (APEC trial) : Study protocol for a randomized controlled trial

Author

Schepers, Nicolien J., Bakker, Olaf J., Besselink, Marc G H, Bollen, Thomas L., Dijkgraaf, Marcel G W, van Eijck, Casper H J, Fockens, Paul, van Geenen, Erwin J M, van Grinsven, Janneke, Hallensleben, Nora D L, Hansen, Bettina E., van Santvoort, Hjalmar C., Timmer, Robin, Anten, Marie Paule G F, Bolwerk, Clemens J M, van Delft, Foke, van Dullemen, Hendrik M., Erkelens, G. Willemien, van Hooft, Jeanin E., Laheij, Robert, van der Hulst, René W M, Jansen, Jeroen M., Kubben, Frank J G M, Kuiken, Sjoerd D., Perk, Lars E., de Ridder, Rogier J J, Rijk, Marno C M, Römkens, Tessa E H, Schoon, Erik J., Schwartz, Matthijs P., Spanier, B. W Marcel, Tan, Adriaan C I T L, Thijs, Willem J., Venneman, Niels G., Vleggaar, Frank P., van de Vrie, Wim, Witteman, Ben J., Gooszen, Hein G., Bruno, Marco J., Schepers, Nicolien J., Bakker, Olaf J., Besselink, Marc G H, Bollen, Thomas L., Dijkgraaf, Marcel G W, van Eijck, Casper H J, Fockens, Paul, van Geenen, Erwin J M, van Grinsven, Janneke, Hallensleben, Nora D L, Hansen, Bettina E., van Santvoort, Hjalmar C., Timmer, Robin, Anten, Marie Paule G F, Bolwerk, Clemens J M, van Delft, Foke, van Dullemen, Hendrik M., Erkelens, G. Willemien, van Hooft, Jeanin E., Laheij, Robert, van der Hulst, René W M, Jansen, Jeroen M., Kubben, Frank J G M, Kuiken, Sjoerd D., Perk, Lars E., de Ridder, Rogier J J, Rijk, Marno C M, Römkens, Tessa E H, Schoon, Erik J., Schwartz, Matthijs P., Spanier, B. W Marcel, Tan, Adriaan C I T L, Thijs, Willem J., Venneman, Niels G., Vleggaar, Frank P., van de Vrie, Wim, Witteman, Ben J., Gooszen, Hein G., and Bruno, Marco J.

Published
2016

33. No role for glutathione S-transferase genotypes in Caucasian esophageal squamous cell or adenocarcinoma etiology: an European case-control study.

Author

Dura, Polat, Salomon, Jody, Te Morsche, Rene H. M., Roelofs, Hennie M. J., Kristinsson, Jon O., Wobbes, Theo, Witteman, Ben J. M., Tan, Adriaan C. I. T. L, Drenth, Joost P. H., and Peters, Wilbert H. M.

Subjects
GLUTATHIONE, OLIGOPEPTIDES, TRANSFERASES, ENZYMES, GENETIC polymorphisms
Abstract

Background: Identifying and monitoring high-risk patients can aid the prevention of esophageal cancer (EC). The interaction of environmental risk factor exposure and genetic susceptibility may contribute to the etiology of EC. Biotransformation enzymes such as Glutathione S-Transferases (GSTs ) detoxify mutagenic and genotoxic compounds and therefore control the rate of detoxification of carcinogens. Functional polymorphisms in the genes coding for GSTs alter their enzyme activity in vitro, and were reported to modify EC risk in Asians. We hypothesized that altered enzyme activity GST genotypes influence the susceptibility for esophageal adeno- (EAC) and squamous cell carcinoma (ESCC) in Caucasians.Methods: We performed a case-control study including 440 Caucasian patients with EC and 592 healthy Caucasian controls matched for age and sex. Functional polymorphisms were selected and genotypes were determined in GST classes Alpha, Mu, Theta and Pi by means of polymerase chain reaction. Genotypes were classified into predicted high, intermediate and low enzyme activity categories based on in vitro activity data. The distribution of the activity genotypes were compared between patients with EAC or ESCC, and controls. Odds ratios (OR) with 95% confidence intervals (CI) were calculated by logistic regression analyses. Gene-gene interactions were tested and for comparison purposes, the predicted low and intermediate activity genotypes were combined. Genotypes with similar risks for EAC or ESCC were combined and analyzed for multiplicative effects.Results: Our analyses includes 327 patients with EAC and 106 patients with ESCC. Low or intermediate activity enzyme genotypes for GSTM1, GSTA1, GSTP1 I105V and A114V as well as for GSTT1, did not significantly modify the risk for ESCC or EAC in our Dutch population.Conclusion: Functional genotypes in GST genes are not involved in EAC or ESCC susceptibility in Caucasians, in contrast to results on ESCC from Asia or Africa. [ABSTRACT FROM AUTHOR]

Published
2013
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34. Open-Access Upper Gastrointestinal Endoscopy a Decade after the Introduction of Proton Pump Inhibitors and Helicobacter pylori Eradication: A Shift in Endoscopic Findings.

Author

van Kerkhoven, Lieke A. S., van Rijswijck, Sally J., van Rossum, Leo G. M., Laheij, Robert J. F., Witteman, Ellen M., Tan, Adriaan C. I. T. L., and Jansen, Jan B. M. J.

Subjects
ENDOSCOPY, PEPTIC ulcer, ESOPHAGUS diseases, PROTON pump inhibitors, EPIDEMIOLOGY, GASTROINTESTINAL diseases, HELICOBACTER pylori
Abstract

Background/Aim: Over the past 15 years, there were considerable changes in factors associated with the development and treatment of upper gastrointestinal symptoms, of which the introduction of proton pump inhibitors and Helicobacter pylori eradication in guidelines for treatment of patients with dyspepsia are the most prominent: findings at open-access upper gastrointestinal endoscopy have not been evaluated properly ever since. This study aims to compare the current prevalence of upper gastrointestinal endoscopic findings to the prevalence 15 years ago. Methods: Data about endoscopic findings of consecutive patients for the first time referred for open-access upper gastrointestinal endoscopy between January 2002 and December 2004 was collected from medical files. The prevalence of each specific finding was compared with data described in three historical populations about 15 years ago. Results: The current and historical study population consisted of 1,286 and 3,062 subjects, respectively. The prevalence of peptic ulcer disease and duodenitis significantly decreased by 12.6% (95% CI: 14.5–10.7) and 2.9% (95% CI: 4.5–1.3), respectively. On the other hand, the prevalence of reflux esophagitis and Barrett’s esophagus both significantly increased by 6.9% (95% CI: 4.2–9.6) and 2.1% (95% CI: 0.8–4.4), respectively. Conclusions: Compared to 15 years ago, the prevalence of specific findings at open-access upper gastrointestinal endoscopy has changed considerably. Copyright © 2007 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published
2007
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36. Alexithymia is Associated With Gastrointestinal Symptoms, but Does Not Predict Endoscopy Outcome in Patients With Gastrointestinal Symptoms

Author

Kerkhoven, Lieke A. S. van, Rossum, Leo G. M. van, Oijen, Martijn G. H. van, Tan, Adriaan C. I. T. L., Witteman, Ellen M., Laheij, Robert J. F., and Jansen, Jan B. M. J.

Abstract

Alexithymia, where a person has difficulty in distinguishing between emotions and bodily sensations, is considered to be a character trait and a vulnerability factor for various psychosomatic disorders. Assessing alexithymia in patients with gastrointestinal (GI) symptoms before endoscopy might therefore be useful in selecting patients who are more prone to functional GI disorders.

Published
2006

37. Clip placement to prevent delayed bleeding after colonic endoscopic mucosal resection (CLIPPER): study protocol for a randomized controlled trial.

Author

Turan, Ayla S, Moons, Leon M G, Schreuder, Ramon-Michel, Schoon, Erik J, Terhaar Sive Droste, Jochim S, Schrauwen, Ruud W M, Straathof, Jan Willem, Bastiaansen, Barbara A J, Schwartz, Matthijs P, Hazen, Wouter L, Alkhalaf, Alaa, Allajar, Daud, Hadithi, Muhammed, van der Spek, Bas W, Heine, Dimitri G D N, Tan, Adriaan C I T L, de Graaf, Wilmar, Boonstra, Jurjen J, Voogd, Fia J, and Roomer, Robert

Subjects
HEMORRHAGE, ENDOSCOPIC surgery, RANDOMIZED controlled trials, HYPERTROPHIC scars, COLORECTAL cancer, COLON polyps
Abstract

Background: Endoscopic mucosal resection (EMR) for large colorectal polyps is in most cases the preferred treatment to prevent progression to colorectal carcinoma. The most common complication after EMR is delayed bleeding, occurring in 7% overall and in approximately 10% of polyps ≥ 2 cm in the proximal colon. Previous research has suggested that prophylactic clipping of the mucosal defect after EMR may reduce the incidence of delayed bleeding in polyps with a high bleeding risk.Methods: The CLIPPER trial is a multicenter, parallel-group, single blinded, randomized controlled superiority study. A total of 356 patients undergoing EMR for large (≥ 2 cm) non-pedunculated polyps in the proximal colon will be included and randomized to the clip group or the control group. Prophylactic clipping will be performed in the intervention group to close the resection defect after the EMR with a distance of < 1 cm between the clips. Primary outcome is delayed bleeding within 30 days after EMR. Secondary outcomes are recurrent or residual polyps and clip artifacts during surveillance colonoscopy after 6 months, as well as cost-effectiveness of prophylactic clipping and severity of delayed bleeding.Discussion: The CLIPPER trial is a pragmatic study performed in the Netherlands and is powered to determine the real-time efficacy and cost-effectiveness of prophylactic clipping after EMR of proximal colon polyps ≥ 2 cm in the Netherlands. This study will also generate new data on the achievability of complete closure and the effects of clip placement on scar surveillance after EMR, in order to further promote the debate on the role of prophylactic clipping in everyday clinical practice.Trial Registration: ClinicalTrials.gov NCT03309683 . Registered on 13 October 2017. Start recruitment: 05 March 2018. Planned completion of recruitment: 31 August 2021. [ABSTRACT FROM AUTHOR]

Published
2021
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38. Atrial Natriuretic Peptide

Author

Tan, Adriaan C. I. T. L., Russel, Frans G. M., Thien, Theo, and Benraad, Theo J.

Abstract

The atrial natriuretic peptide (ANP) is part of a new family of cardiac hormones regulating water and salt homeostasis. Besides acting as a blood pressure-lowering agent, it also exerts potent natriuretic and diuretic effects. ANP can be considered an endogenous antagonist of the renin-angiotensin-aldosterone system and the antidiuretic hormone. One of the roles of ANP is to protect the body against fluid overload: it decreases intravascular fluid volume, which in turn diminishes cardiac secretion of ANP. The pharmacokinetic parameters of ANP reported in the literature vary widely. In general, ANP rapidly disappears from plasma with a high total body clearance. This is in agreement with the short-lived effects of the hormone. The actions of ANP have led to efforts to use this peptide hormone in the treatment of various cardiovascular dis-orders such as hypertension and congestive heart failure. Intravenous ANP administration indeed resulted in beneficial effects in these disorders. However, the peptide nature of ANP and its rapid elimination from the circulation limit its suitability as a drug. More promising is the development of long-acting ANP analogues and inhibitors of ANP degradation. Proper understanding of ANP pharmacokinetics is essential for the clinical use of these pharmacological agents.

Published
1993
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39. Validation and update of a prediction model for risk of relapse after cessation of anti-TNF treatment in Crohn's disease.

Author

Ten Bokkel Huinink S, de Jong DC, Nieboer D, Thomassen D, Steyerberg EW, Dijkgraaf MGW, Bodelier AGL, West RL, Römkens TEH, Hoentjen F, Mallant RC, van Tuyl BAC, Mares WGN, Wolfhagen FHJ, Dijkstra G, Reijnders JGP, de Boer NK, Tan ACITL, van Boeckel PGA, Tack GJ, van Asseldonk DP, D'Haens GRAM, van der Woude CJ, Duijvestein M, and de Vries AC

Subjects
Humans, Models, Statistical, Recurrence, Reproducibility of Results, Retrospective Studies, Risk Assessment, Crohn Disease drug therapy, Tumor Necrosis Factor Inhibitors therapeutic use, Withholding Treatment
Abstract

Background: Anti-tumor necrosis factor (TNF) therapy is effective for the treatment of Crohn's disease. Cessation may be considered in patients with a low risk of relapse. We aimed to externally validate and update our previously developed prediction model to estimate the risk of relapse after cessation of anti-TNF therapy., Methods: We performed a retrospective cohort study in 17 Dutch hospitals. Crohn's disease patients in clinical, biochemical or endoscopic remission were included after anti-TNF cessation. Primary outcome was a relapse necessitating treatment. Discrimination and calibration of the previously developed model were assessed. After external validation, the model was updated. The performance of the updated prediction model was assessed in internal-external validation and by using decision curve analysis., Results: 486 patients were included with a median follow-up of 1.7 years. Relapse rates were 35 and 54% after 1 and 2 years. At external validation, the discriminative ability of the prediction model was equal to that found at the development of the model [c-statistic 0.58 (95% confidence interval (CI) 0.54-0.62)], though the model was not well-calibrated on our cohort [calibration slope: 0.52 (0.28-0.76)]. After an update, a c-statistic of 0.60 (0.58-0.63) and calibration slope of 0.89 (0.69-1.09) were reported in internal-external validation., Conclusion: Our previously developed and updated prediction model for the risk of relapse after cessation of anti-TNF in Crohn's disease shows reasonable performance. The use of the model may support clinical decision-making to optimize patient selection in whom anti-TNF can be withdrawn. Clinical validation is ongoing in a prospective randomized trial., (Copyright © 2022 Wolters Kluwer Health, Inc. All rights reserved.)

Published
2022
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40. Risk factors and clinical outcomes of endoscopic dilation in benign esophageal strictures: a long-term follow-up study.

Author

Vermeulen BD, de Zwart M, Sijben J, Soons E, van der Weerd L, Arese D, von den Hoff DW, Craviotto V, Tan ACITL, Groenen MJM, Bogte A, Repici A, Spaander MCW, and Siersema PD

Subjects
Dilatation, Follow-Up Studies, Humans, Netherlands, Retrospective Studies, Risk Factors, Treatment Outcome, Esophageal Stenosis etiology, Esophageal Stenosis therapy
Abstract

Background and Aims: Endoscopic dilation (ED) is still the mainstay of therapeutic management of benign esophageal strictures (BESs). This study aimed to establish risk factors for refractory BESs and assess long-term clinical outcomes of ED., Methods: We performed a retrospective study in 891 patients who underwent ED from 2003 to 2018 for BESs. We searched electronic medical records in 6 tertiary care centers in the Netherlands for data on clinical outcome of ED. Median follow-up was 39 months. The primary endpoint was risk factors for refractory BESs, defined as factors associated with an increased number of ED sessions during follow-up. Secondary endpoints were time from first to last ED session and adverse events., Results: Dilation up to 13 to 15 mm was associated with a higher number of ED sessions than dilation up to 16 to 18 mm (5.0 vs 4.1; hazard ratio [HR], 1.4; P = .001). Compared with peptic strictures, anastomotic (4.9 vs 3.6; HR, 2.1; P < .001), radiation (5.0 vs 3.6; HR, 3.0; P < .001), caustic (7.2 vs 3.6; HR, 2.7; P < .001), and postendotherapy (3.9 vs 3.6; HR, 1.8; P = .005) strictures were associated with a higher number of ED sessions. After 1 year of follow-up, the proportions of patients who remained free of ED was 75% in anastomotic, 71% in radiation, 70% in peptic, 83% in postendotherapy, and 62% in caustic strictures. Esophageal perforation occurred in 23 ED sessions (.4%) in 22 patients (2.4%)., Conclusions: More than 60% of patients with BESs remain free of ED after 1 year of follow-up. Because dilation up to 16 to 18 mm diameter was associated with fewer ED sessions during follow-up, we suggest that clinicians should consider dilation up to at least 16 mm to reduce the number of ED sessions in these patients., (Copyright © 2020 American Society for Gastrointestinal Endoscopy. Published by Elsevier Inc. All rights reserved.)

Published
2020
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41. Unexpected amebic colitis presenting with rectal bleeding and perforation after biopsy.

Author

de Leijer JH, Tan ACITL, Mulder B, and Zomer SF

Subjects
Aged, Biopsy adverse effects, Cecal Diseases complications, Cecal Diseases diagnosis, Cecal Diseases drug therapy, Cecal Diseases surgery, Colectomy, Colonic Diseases complications, Colonic Diseases diagnosis, Colonic Diseases drug therapy, Colonic Diseases surgery, Colonoscopy, Dysentery, Amebic drug therapy, Dysentery, Amebic pathology, Gastrointestinal Hemorrhage etiology, Humans, Intestinal Diseases complications, Intestinal Diseases drug therapy, Intestinal Diseases surgery, Intestinal Perforation etiology, Intestinal Perforation surgery, Male, Rectal Diseases complications, Rectal Diseases diagnosis, Rectal Diseases drug therapy, Rectum pathology, Dysentery, Amebic diagnosis, Intestinal Diseases diagnosis
Published
2018
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43. Early biliary decompression versus conservative treatment in acute biliary pancreatitis (APEC trial): study protocol for a randomized controlled trial.

Author

Schepers NJ, Bakker OJ, Besselink MG, Bollen TL, Dijkgraaf MG, van Eijck CH, Fockens P, van Geenen EJ, van Grinsven J, Hallensleben ND, Hansen BE, van Santvoort HC, Timmer R, Anten MP, Bolwerk CJ, van Delft F, van Dullemen HM, Erkelens GW, van Hooft JE, Laheij R, van der Hulst RW, Jansen JM, Kubben FJ, Kuiken SD, Perk LE, de Ridder RJ, Rijk MC, Römkens TE, Schoon EJ, Schwartz MP, Spanier BW, Tan AC, Thijs WJ, Venneman NG, Vleggaar FP, van de Vrie W, Witteman BJ, Gooszen HG, and Bruno MJ

Subjects
Acute Disease, Cholangiography, Humans, Sample Size, Sphincterotomy, Endoscopic, Biliary Tract Surgical Procedures methods, Clinical Protocols, Decompression, Surgical methods, Pancreatitis surgery
Abstract

Background: Acute pancreatitis is mostly caused by gallstones or sludge. Early decompression of the biliary tree by endoscopic retrograde cholangiography (ERC) with sphincterotomy may improve outcome in these patients. Whereas current guidelines recommend early ERC in patients with concomitant cholangitis, early ERC is not recommended in patients with mild biliary pancreatitis. Evidence on the role of routine early ERC with endoscopic sphincterotomy in patients without cholangitis but with biliary pancreatitis at high risk for complications is lacking. We hypothesize that early ERC with sphincterotomy improves outcome in these patients., Methods/design: The APEC trial is a randomized controlled, parallel group, superiority multicenter trial. Within 24 hours after presentation to the emergency department, patients with biliary pancreatitis without cholangitis and at high risk for complications, based on an Acute Physiology and Chronic Health Evaluation (APACHE-II) score of 8 or greater, Modified Glasgow score of 3 or greater, or serum C-reactive protein above 150 mg/L, will be randomized. In 27 hospitals of the Dutch Pancreatitis Study Group, 232 patients will be allocated to early ERC with sphincterotomy or to conservative treatment. The primary endpoint is a composite of major complications (that is, organ failure, pancreatic necrosis, pneumonia, bacteremia, cholangitis, pancreatic endocrine, or exocrine insufficiency) or death within 180 days after randomization. Secondary endpoints include ERC-related complications, infected necrotizing pancreatitis, length of hospital stay and an economical evaluation., Discussion: The APEC trial investigates whether an early ERC with sphincterotomy reduces the composite endpoint of major complications or death compared with conservative treatment in patients with biliary pancreatitis at high risk of complications., Trial Registration: Current Controlled Trials ISRCTN97372133 (date registration: 17-12-2012).

Published
2016
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44. Polymorphisms in alcohol-metabolizing enzymes and esophageal carcinoma susceptibility: a Dutch Caucasian case-control study.

Author

Dura P, Berkers T, van Veen EM, Salomon J, te Morsche RH, Roelofs HM, Kristinsson JO, Wobbes T, Witteman BJ, Tan AC, Drenth JP, and Peters WH

Subjects
Adenocarcinoma enzymology, Adenocarcinoma ethnology, Aged, Alcohol Dehydrogenase metabolism, Carcinoma, Squamous Cell enzymology, Carcinoma, Squamous Cell ethnology, Case-Control Studies, Cytochrome P-450 CYP2E1 metabolism, Esophageal Neoplasms enzymology, Esophageal Neoplasms ethnology, Esophageal Squamous Cell Carcinoma, Female, Genetic Association Studies, Genetic Predisposition to Disease, Humans, Male, Middle Aged, Netherlands, Polymorphism, Genetic, Adenocarcinoma genetics, Alcohol Dehydrogenase genetics, Carcinoma, Squamous Cell genetics, Cytochrome P-450 CYP2E1 genetics, Esophageal Neoplasms genetics, Ethanol metabolism, White People
Abstract

Esophageal cancer (EC), mainly consisting of squamous cell carcinoma (ESCC) in the Eastern world and adenocarcinoma (EAC) in the Western world, is strongly associated with dietary factors such as alcohol use. We aimed to clarify the modifying role in EC etiology in Caucasians of functional genotypes in alcohol-metabolizing enzymes. In all, 351 Caucasian patients with EC and 430 matched controls were included and polymorphisms in CYP2E1, ADH and near ALDH2 genes were determined. In contrast to the results on ESCC in mainly Asian studies, we found that functional genotypes of alcohol-metabolizing enzymes were not significantly associated with EAC or ESCC in an European population.

Published
2013
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45. Barrett associated MHC and FOXF1 variants also increase esophageal carcinoma risk.

Author

Dura P, van Veen EM, Salomon J, te Morsche RH, Roelofs HM, Kristinsson JO, Wobbes T, Witteman BJ, Tan AC, Drenth JP, and Peters WH

Subjects
Adenocarcinoma etiology, Aged, Barrett Esophagus complications, Esophageal Neoplasms etiology, Female, Gastroesophageal Reflux complications, Genetic Predisposition to Disease, Genotype, Humans, Male, Middle Aged, Obesity complications, Polymorphism, Single Nucleotide, Smoking, Barrett Esophagus genetics, Esophageal Neoplasms genetics, Forkhead Transcription Factors genetics, Major Histocompatibility Complex genetics
Abstract

Barrett's esophagus, with gastroesophageal reflux disease and obesity as risk factors, predisposes to esophageal adenocarcinoma (EAC). Recently a British genome wide association study identified two Barrett's esophagus susceptibility loci mapping within the major histocompatibility complex (MHC; rs9257809) and closely to the Forkhead-F1 (FOXF1; rs9936833) coding gene. An interesting issue is whether polymorphisms associated with Barrett's esophagus, are also implicated in esophageal carcinoma (EC), and more specifically EAC genesis. Assessing the individual genetic susceptibility can help identify high risk patients more prone to benefit from surveillance programs. Our hypothesis: Barrett associated MHC and FOXF1 variants modify EC risk in Caucasians. In a Dutch case-control study, 431 patients with EC and 605 healthy controls were included. Polymorphisms at chromosomes 6p21 (MHC) and 16q24 (FOXF1) were determined by means of real-time polymerase chain reaction (RT-PCR). Logistic regression analysis was used to calculate odds ratios with 95% confidence intervals. The FOXF1 rs9936833 variant C allele was associated with an increased EAC susceptibility; OR, [95% CI]; 1.21, [0.99-1.47]. A sex-stratified analysis revealed a similar association in males; 1.24 [1.00-1.55]. The variant MHC rs9257809 G allele as well as the MHC heterozygous AG genotype significantly increased ESCC risk; 1.76 [1.16-2.66] and 1.74 [1.08-2.80], respectively. Sex-stratification showed that the variant G allele was especially present in female patients; 2.32 [1.04-5.20]. In conclusion, this study provides evidence that MHC rs9257809 and FOXF1 rs9936833 variants, associated with Barrett's esophagus, also increase ESCC and EAC susceptibility in Caucasians. FOX proteins are transcription factors involved in organogenesis of the GI tract, while MHC haplotypes are strongly associated with smoking behavior, a crucial risk factor for ESCC. Assessing the individual genetic susceptibility can help identify high risk patients more prone to benefit from (Barrett) surveillance programs., (© 2013 UICC.)

Published
2013
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46. GWAS-uncovered SNPs in PLCE1 and RFT2 genes are not implicated in Dutch esophageal adenocarcinoma and squamous cell carcinoma etiology.

Author

Dura P, Bregitha CV, te Morsche RH, Roelofs HM, Kristinsson JO, Wobbes T, Witteman BJ, Tan AC, Drenth JP, and Peters WH

Subjects
Adenocarcinoma epidemiology, Carcinoma, Squamous Cell epidemiology, Case-Control Studies, Esophageal Neoplasms epidemiology, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Male, Netherlands epidemiology, Risk Factors, White People statistics & numerical data, Adenocarcinoma genetics, Carcinoma, Squamous Cell genetics, Esophageal Neoplasms genetics, Membrane Transport Proteins genetics, Phosphoinositide Phospholipase C genetics, Polymorphism, Single Nucleotide physiology
Abstract

Susceptibility to esophageal carcinoma (EC) is influenced by the interaction between genetic and environmental factors. To clarify the etiology of EC, several genome-wide association studies have identified single nucleotide polymorphisms (SNPs) in PCLE1 and RFT2 genes as esophageal squamous cell carcinoma (ESCC) susceptibility loci in Asian populations. This study aimed to determine whether these SNPs also modify the risk of esophageal adenocarcinoma (EAC) and ESCC in western populations of Caucasian ethnicity. A European case-control study including 349 EC patients and 580 controls matched for age, sex, geographical location, and race was carried out. The SNPs rs2274223 in the PCLE1 gene at chromosome 10q23 and rs13042395 in the RFT2 gene at chromosome 20p13 were determined using PCR. Genotype distributions were compared between patients and controls, and odds ratios with 95% confidence intervals were calculated. The total EC group included 86 patients with ESCC and 258 patients with EAC. The distribution of PLCE1 and RFT2 genotypes did not differ between patients with EAC or ESSC, and the controls. In contrast to the modulation of the risk of ESCC in Asians, it is unlikely that the PLCE1 rs2274223 and RFT2 13042395 SNPs play a role in EAC or ESCC susceptibility in Dutch Caucasians.

Published
2013
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47. Dietary supplement use is not associated with recurrence of colorectal adenomas: a prospective cohort study.

Author

Heine-Bröring RC, Winkels RM, Botma A, Wahab PJ, Tan AC, Nagengast FM, Witteman BJ, and Kampman E

Subjects
Adenoma etiology, Cohort Studies, Colonoscopy, Colorectal Neoplasms etiology, Diet, Early Detection of Cancer, Feeding Behavior, Female, Humans, Male, Middle Aged, Neoplasm Recurrence, Local etiology, Proportional Hazards Models, Prospective Studies, Adenoma epidemiology, Colorectal Neoplasms epidemiology, Dietary Supplements adverse effects, Neoplasm Recurrence, Local epidemiology
Abstract

Diet and lifestyle influence colorectal adenoma recurrence. The role of dietary supplement use in colorectal adenoma recurrence remains controversial. In this prospective cohort study, we examined the association between dietary supplement use, total colorectal adenoma recurrence and advanced adenoma recurrence. Colorectal adenoma cases (n = 565) from a former case-control study, recruited between 1995 and 2002, were prospectively followed until 2008. Adenomas with a diameter of ≥1 cm and/or (tubulo)villous histology and/or with high grade dysplasia and/or ≥3 adenomas detected at the same colonic examination were considered advanced adenomas. Hazard ratios (HRs) and 95% confidence intervals (CIs) for dietary supplement users (use of any supplement during the past year) compared to nonusers and colorectal adenoma recurrence were calculated using stratified Cox proportional hazard models for counting processes and were adjusted for age, sex, educational level and number of colonoscopies during follow-up. Robust sandwich covariance estimation was used to adjust for the within subject correlation. A number of 165 out of 565 adenoma patients had at least one colorectal adenoma recurrence during a median person-time of 5.4 years and of these, 37 patients had at least one advanced adenoma. One-third of the total study population (n = 203) used a dietary supplement. Compared to no use, dietary supplement use was neither statistically significantly associated with total colorectal adenoma recurrence (HR = 1.03; 95% CI 0.79-1.34) nor with recurrent advanced adenomas (HR = 1.59; 95% CI 0.88-2.87). This prospective cohort study did not suggest an association between dietary supplement use and colorectal adenoma recurrence., (Copyright © 2012 UICC.)

Published
2013
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48. High enzyme activity UGT1A1 or low activity UGT1A8 and UGT2B4 genotypes increase esophageal cancer risk.

Author

Dura P, Salomon J, Te Morsche RH, Roelofs HM, Kristinsson JO, Wobbes T, Witteman BJ, Tan AC, Drenth JP, and Peters WH

Subjects
Adenocarcinoma genetics, Aged, Carcinoma, Squamous Cell genetics, Case-Control Studies, Esophageal Neoplasms genetics, Female, Genetic Association Studies, Genetic Predisposition to Disease, Glucuronosyltransferase genetics, Haplotypes, Humans, Male, Middle Aged, Polymorphism, Genetic, Risk Factors, Adenocarcinoma enzymology, Carcinoma, Squamous Cell enzymology, Esophageal Neoplasms enzymology, Glucuronosyltransferase metabolism
Abstract

Esophageal cancer (EC) has a globally increasing incidence with poor curative treatment options and survival rates. Environmental and dietary factors have crucial roles in esophageal carcinogenesis. Polymorphisms in the UGT genes, a superfamily of enzymes essential for the detoxification of carcinogens, may alter enzyme activity and subsequently may play a role in EC etiology. Rather than solely establishing differences in genotype distribution, we investigated whether functional polymorphisms in UGT genes that can predict enzyme activity in vivo, may influence EC risk. A case-control study including 351 Caucasian EC patients and 592 Caucasian controls was conducted and polymorphisms in seven UGT genes were determined, using the polymerase chain reaction. On the basis of allelic in vitro enzyme activity measurements, genotypes were categorized according to their predicted in vivo enzyme activity into high, medium and low categories. Predicted enzyme activity groups were combined and compared between patients and controls. The UGT1A1 and UGT1A8 predicted high enzyme activity genotypes were significantly more (OR=1.62; 95% CI, 1.02-2.56) and less frequent (OR=0.36; 95% CI, 0.15-0.84) among patients with esophageal squamous cell carcinoma (ESCC), respectively. High (OR=0.42; 95% CI, 0.22-0.84) and medium (OR=0.25; 95% CI, 0.12-0.52) activity UGT2B4 genotypes were significantly less often present in ESCC patients. No association was detected between UGT genotypes and esophageal adenocarcinoma (EAC) risk. Polymorphisms in UGT genes, resulting in altered enzyme activity genotypes, do not seem modifiers of EAC risk. However, the predicted high activity UGT1A1 genotype, associated with low serum levels of the antioxidant bilirubin, was associated with an increased ESCC risk. The UGT1A8 and UGT2B4 genotypes associated with decreased predicted enzyme activities, were significantly associated with an increased risk of ESCC, probably by a decreased detoxification of carcinogens.

Published
2012
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49. EPHX1 polymorphisms do not modify esophageal carcinoma susceptibility in Dutch Caucasians.

Author

Dura P, Bregitha CV, Te Morsche RH, Roelofs HM, Kristinsson JO, Wobbes T, Witteman BJ, Tan AC, Drenth JP, and Peters WH

Subjects
Adenocarcinoma enzymology, Adenocarcinoma ethnology, Aged, Aged, 80 and over, Carcinoma, Squamous Cell enzymology, Carcinoma, Squamous Cell ethnology, Carcinoma, Squamous Cell genetics, Case-Control Studies, Esophageal Neoplasms enzymology, Esophageal Neoplasms ethnology, Female, Genetic Predisposition to Disease, Genotype, Heterozygote, Homozygote, Humans, Male, Middle Aged, Netherlands epidemiology, Polymorphism, Single Nucleotide, Risk Factors, White People genetics, Adenocarcinoma genetics, Epoxide Hydrolases genetics, Esophageal Neoplasms genetics
Abstract

Esophageal cancer (EC) has a globally increasing incidence with poor curative treatment options and survival rates. Crucial risk factors are exposure to toxins or carcinogens. Microsomal epoxide hydrolase (mEH) is a biotransformation enzyme essential for the detoxification of xenobiotics. Polymorphisms in exon 3 and exon 4 of the microsomal epoxide hydrolase gene (EPHX1) modify catalytic activity of this enzyme and subsequently may play a role in EC etiology. This case-control study investigated whether these polymorphisms in the EPHX1 gene influence esophageal cancer susceptibility in a Dutch Caucasian population. A case-control study including 349 Caucasian EC patients and 581 Caucasian healthy controls was conducted and the polymorphisms Tyr113His (exon 3) and His139Arg (exon 4) in the EPHX1 gene were determined, using polymerase chain reaction. The distribution of exon 3 and exon 4 genotypes were compared between cases and controls. Analyses included a stratification according to tumor histology; esophageal adenocarcinoma (EAC) or squamous cell carcinoma (ESCC). Furthermore, on the basis of allelic in vitro enzyme activity assays, exon 3 and 4 genotypes were combined and categorized according to their predicted high, medium or low enzyme activity. Homozygosity and heterozygosity for both exon 3 and 4 polymorphisms were correlated with a decreased esophageal squamous cell carcinoma risk. Heterozygosity and homozygosity for both polymorphisms correlated with an increased and a decreased esophageal adenocarcinoma risk, respectively. Predicted intermediate and high activity genotypes were risk and protective factors for esophageal squamous cell carcinoma and esophageal adenocarcinoma, respectively. However, none of these associations were statistically significant. In conclusion, the polymorphisms in exon 3 and exon 4 of the EPHX1 gene do not seem to be modifiers of esophageal squamous cell carcinoma or esophageal adenocarcinoma risk in Dutch Caucasians.

Published
2012
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50. [Submucosal presentation of Whipple's disease: a variant that is easily missed].

Author

Lynch MG, van den Berg-van Erp SH, Tan AC, and Pettersson AM

Subjects
Aged, Aged, 80 and over, Biopsy, Diagnosis, Differential, Humans, Male, Whipple Disease microbiology, Tropheryma isolation & purification, Whipple Disease pathology
Abstract

Whipple's disease is a multisystem, and often chronic, disease caused by infection with the bacterium Tropheryma whipplei, and mainly occurs in middle-aged Caucasian men. In most cases, histological detection of large numbers of bacteria-laden macrophages in the mucosa of the small intestine confirms the diagnosis. Less commonly, these macrophages may be sparse and predominantly located beneath the mucosa. In these submucosally presenting cases, endoscopic and classic histological clues are absent and, therefore, the diagnosis can be missed. As a result, further periodic acid-Schiff (PAS) staining and PCR analysis are of great importance in arriving at the correct diagnosis.

Published
2012

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