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3. Incidence and prevalence of primary biliary cholangitis in the Netherlands – A nationwide cohort study

Author

Abraham, Sunje, Adang, Rob P.R., Aktas, Huseyin, Alderlieste, Yasser A., Aparicio-Pages, Maria N., Baak, L. (Bert) C., Baven-Pronk, Martine A.M.C., van der Beek, A. (Sander), Bekkering, Frank C., van Bergeijk, Jeroen D., Beuers, Ulrich, Beukema, Menno, de Boer, Wink, Boersma, Femke, Boonstra, Kirsten, ter Borg, Frank, ter Borg, Martijn J., ter Borg, Pieter C.J., de Bruin, Gijs J., Bus, Paul J., Cahen, Djuna L., Cazemier, Marcel, Cuperus, Frans J.C., van Dam, Lisette J.H., Denters, Maaike J., Drenth, Joost P.H., Epping, Ludger S.M., Erler, Nicole S., Flink, Hajo J., Friederich, Philip W., van Gerven, Nicole F.M., Gevers, Tom J.G., Hansen, Bettina E., van den Hazel, Sven J., van Hoek, Bart, van Hooff, Maria C., Hotho, Daphne M., Janssen, Harry L.A., de Jonge, Hendrik J.M., Jurgens, Matthias C., Kemenade, J.(Netty) van, Kerbert-Dreteler, Marjo J., Klemt-Kropp, Michael, Konings, Ingrid C.A.W., de Kort, Sander, Kuiper, Edith M.M., Kuyvenhoven, Johan P.H., van der Meer, Adriaan J., van Meer, Suzanne, Onderwater, Susanne L., Oterdoom, Leendert H., Ponsioen, Cyriel Y., van Putten, Paul G., van Rooij, Janne E., Roomer, Robert, Schmidt-Böhmer, Johannes, Schmittgens, Stephan, Schreuder, Tim C.M.A., Nicolaas, Jerome Sint, van Soest, Hanneke, Soufidi, Khalida, van Stiphout, Stephan H.C., Thio, Hans H.K., Tielemans, Merel M., Vandebosch, Sigrid, de Veer, Rozanne C., Veldt, Bart J., Verdonk, Robert C., Marleen de Vree, J., de Vries, Elsemieke, Vrieze, Anne, Vrolijk, Jan Maarten, van der Waaij, Laurens A., Werner, Ellen, de Wit, Ulrike, Wolfhagen, Frank H.J., van Hooff, Maria C.B., Baak, L.C., and Borg, Frank ter

Published
2024
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4. Type 1 Autoimmune Pancreatitis in Europe: Clinical Profile and Response to Treatment

Author

Drewes, A. Mohr, Haas, S.L., Hoyer, B.F., Hampe, J., Hinrichs, C. Noreen, Lerch, M.M., Aghdassi, A.A., Grote, T., Heuser, D.J., Ignatavicius, P., Malecka-Panas, E., Domínguez-Muñoz, J.E., López-Serrano, A., Auriemma, F., Oracz, G., Duman, D., Gubergrits, N., Overbeek, Kasper A., Poulsen, Jakob L., Lanzillotta, Marco, Vinge-Holmquist, Olof, Macinga, Peter, Demirci, A. Fatih, Sindhunata, Daniko P., Backhus, Johanna, Algül, Hana, Buijs, Jorie, Levy, Philippe, Kiriukova, Mariia, Goni, Elisabetta, Hollenbach, Marcus, Miksch, Rainer C., Kunovsky, Lumir, Vujasinovic, Miroslav, Nikolic, Sara, Dickerson, Luke, Hirth, Michael, Neurath, Markus F., Zumblick, Malte, Vila, Josephine, Jalal, Mustafa, Beyer, Georg, Frost, Fabian, Carrara, Silvia, Kala, Zdenek, Jabandziev, Petr, Sisman, Gurhan, Akyuz, Filiz, Capurso, Gabriele, Falconi, Massimo, Arlt, Alexander, Vleggaar, Frank P., Barresi, Luca, Greenhalf, Bill, Czakó, László, Hegyi, Peter, Hopper, Andrew, Nayar, Manu K., Gress, Thomas M., Vitali, Francesco, Schneider, Alexander, Halloran, Chris M., Trna, Jan, Okhlobystin, Alexey V., Dagna, Lorenzo, Cahen, Djuna L., Bordin, Dmitry, Rebours, Vinciane, Mayerle, Julia, Kahraman, Alisan, Rasch, Sebastian, Culver, Emma, Kleger, Alexander, Martínez-Moneo, Emma, Røkke, Ola, Hucl, Tomas, Olesen, Søren S., Bruno, Marco J., Della-Torre, Emanuel, Beuers, Ulrich, Löhr, J.-Matthias, and Rosendahl, Jonas

Published
2024
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5. Intrapancreatic fat deposition is unrelated to liver steatosis in metabolic dysfunction-associated steatotic liver disease

Author

Mak, Anne Linde, Wassenaar, Nienke, van Dijk, Anne-Marieke, Troelstra, Marian, Houttu, Veera, van Son, Koen, Driessen, Stan, Zwirs, Diona, van den Berg-Faay, Sandra, Shumbayawonda, Elizabeth, Runge, Jurgen, Doukas, Michail, Verheij, Joanne, Beuers, Ulrich, Nieuwdorp, Max, Cahen, Djuna L., Nederveen, Aart, Gurney-Champion, Oliver, and Holleboom, Adriaan

Published
2024
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7. Intraductal Papillary Mucinous Neoplasms in High-Risk Individuals: Incidence, Growth Rate, and Malignancy Risk

Author

Overbeek, Kasper A., Koopmann, Brechtje D.M., Levink, Iris J.M., Tacelli, Matteo, Erler, Nicole S., Arcidiacono, Paolo Giorgio, Ausems, Margreet G.E., Wagner, Anja, van Eijck, Casper H., Groot Koerkamp, Bas, Busch, Olivier R., Besselink, Marc G., van der Vlugt, Manon, van Driel, Lydi M.J.W., Fockens, Paul, Vleggaar, Frank P., Poley, Jan-Werner, Capurso, Gabriele, Cahen, Djuna L., and Bruno, Marco J.

Published
2024
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11. Timeline of Development of Pancreatic Cancer and Implications for Successful Early Detection in High-Risk Individuals

Author

Overbeek, Kasper A., Goggins, Michael G., Dbouk, Mohamad, Levink, Iris J.M., Koopmann, Brechtje D.M., Chuidian, Miguel, Konings, Ingrid C.A.W., Paiella, Salvatore, Earl, Julie, Fockens, Paul, Gress, Thomas M., Ausems, Margreet G.E.M., Poley, Jan-Werner, Thosani, Nirav C., Half, Elizabeth, Lachter, Jesse, Stoffel, Elena M., Kwon, Richard S., Stoita, Alina, Kastrinos, Fay, Lucas, Aimee L., Syngal, Sapna, Brand, Randall E., Chak, Amitabh, Carrato, Alfredo, Vleggaar, Frank P., Bartsch, Detlef K., van Hooft, Jeanin E., Cahen, Djuna L., Canto, Marcia Irene, and Bruno, Marco J.

Published
2022
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12. Incidence and prevalence of primary biliary cholangitis in the Netherlands – a nationwide cohort study

Author

de Veer, Rozanne C., primary, van Hooff, Maria C.B., additional, Werner, Ellen, additional, Beuers, Ulrich, additional, Drenth, Joost P.H., additional, Cuperus, Frans J.C., additional, van Hoek, Bart, additional, Veldt, Bart J., additional, Klemt-Kropp, Michael, additional, van Meer, Suzanne, additional, Verdonk, Robert C., additional, Flink, Hajo J., additional, Vrolijk, Jan Maarten, additional, Gevers, Tom J.G., additional, Ponsioen, Cyriel Y., additional, ter Borg, Martijn J., additional, Soufidi, Khalida, additional, Boersma, Femke, additional, de Jonge, Hendrik J.M., additional, Wolfhagen, Frank H.J., additional, Baak, L.C., additional, Onderwater, Susanne L., additional, van Bergeijk, Jeroen D., additional, van Putten, Paul G., additional, de Bruin, Gijs J., additional, Adang, Rob P.R., additional, Aparicio-Pages, Maria N., additional, de Boer, Wink, additional, Borg, Frank ter, additional, van Soest, Hanneke, additional, Janssen, Harry L.A., additional, Hansen, Bettina E., additional, Erler, Nicole S., additional, van der Meer, Adriaan J., additional, Abraham, Sunje, additional, Aktas, Huseyin, additional, Alderlieste, Yasser A., additional, Baak, L. (Bert) C., additional, Baven-Pronk, Martine A.M.C., additional, van der Beek, A.Sander, additional, Bekkering, Frank C., additional, Beukema, Menno, additional, Boonstra, Kirsten, additional, ter Borg, Frank, additional, ter Borg, Pieter C.J., additional, Bus, Paul J., additional, Cahen, Djuna L., additional, Cazemier, Marcel, additional, van Dam, Lisette J.H., additional, Denters, Maaike J., additional, Epping, Ludger S.M., additional, Friederich, Philip W., additional, van Gerven, Nicole F.M., additional, van den Hazel, Sven J., additional, van Hooff, Maria C., additional, Hotho, Daphne M., additional, Jurgens, Matthias C., additional, van Kemenade, J.Netty, additional, Kerbert-Dreteler, Marjo J., additional, Konings, Ingrid C.A.W., additional, de Kort, Sander, additional, Kuiper, Edith M.M., additional, Kuyvenhoven, Johan P.H., additional, Oterdoom, Leendert H., additional, van Rooij, Janne E., additional, Roomer, Robert, additional, Schmidt-Böhmer, Johannes, additional, Schmittgens, Stephan, additional, Schreuder, Tim C.M.A., additional, Nicolaas, Jerome Sint, additional, van Stiphout, Stephan H.C., additional, Thio, Hans H.K., additional, Tielemans, Merel M., additional, Vandebosch, Sigrid, additional, de Veer, Rozanne C., additional, Vree, J. Marleen de, additional, de Vries, Elsemieke, additional, Vrieze, Anne, additional, van der Waaij, Laurens A., additional, and de Wit, Ulrike, additional

Published
2024
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13. THU-120-YI The impact of ursodeoxycholic acid on biochemistry of patients with primary biliary cholangitis in a nationwide cohort

Author

Werner, Ellen, primary, van Hooff, Maria C., additional, van der Maas, Gerjan J., additional, de Veer, Rozanne C., additional, Beuers, Ulrich, additional, Drenth, Joost P.H., additional, Cuperus, Frans J.C., additional, van Hoek, Bart, additional, Veldt, Bart J., additional, Klemt-Kropp, Michael, additional, van Meer, Suzanne, additional, Verdonk, Robert C., additional, Flink, Hajo J., additional, Vrolijk, Jan Maarten, additional, Gevers, Tom J.G., additional, Ponsioen, Cyriel Y., additional, de Kort, Sander, additional, van Putten, Paul G., additional, Cahen, Djuna L., additional, van der Waaij, Lauren A., additional, Thio, Hans H.K., additional, Schreuder, Tim C.M.A., additional, van Dam, Lisette J.H., additional, Epping, Ludger S.M., additional, Jurgens, Matthias C., additional, Cazemier, Marcel, additional, van Kemenade, J., additional, Kuiper, Edith M.M., additional, Beukema, Menno, additional, Borg, Martijn J. ter, additional, Soufidi, Khalida, additional, Janssen, Harry L.A., additional, Hansen, Bettina E., additional, Erler, Nicole S., additional, and van der Meer, Adriaan J., additional

Published
2024
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14. Type 1 Autoimmune Pancreatitis in Europe: Clinical Profile and Response to Treatment

Author

Overbeek, Kasper A., primary, Poulsen, Jakob L., additional, Lanzillotta, Marco, additional, Vinge-Holmquist, Olof, additional, Macinga, Peter, additional, Demirci, A. Fatih, additional, Sindhunata, Daniko P., additional, Backhus, Johanna, additional, Algül, Hana, additional, Buijs, Jorie, additional, Levy, Philippe, additional, Kiriukova, Mariia, additional, Goni, Elisabetta, additional, Hollenbach, Marcus, additional, Miksch, Rainer C., additional, Kunovsky, Lumir, additional, Vujasinovic, Miroslav, additional, Nikolic, Sara, additional, Dickerson, Luke, additional, Hirth, Michael, additional, Neurath, Markus F., additional, Zumblick, Malte, additional, Vila, Josephine, additional, Jalal, Mustafa, additional, Beyer, Georg, additional, Frost, Fabian, additional, Carrara, Silvia, additional, Kala, Zdenek, additional, Jabandziev, Petr, additional, Sisman, Gurhan, additional, Akyuz, Filiz, additional, Capurso, Gabriele, additional, Falconi, Massimo, additional, Arlt, Alexander, additional, Vleggaar, Frank P., additional, Barresi, Luca, additional, Greenhalf, Bill, additional, Czakó, László, additional, Hegyi, Peter, additional, Hopper, Andrew, additional, Nayar, Manu K., additional, Gress, Thomas M., additional, Vitali, Francesco, additional, Schneider, Alexander, additional, Halloran, Chris M., additional, Trna, Jan, additional, Okhlobystin, Alexey V., additional, Dagna, Lorenzo, additional, Cahen, Djuna L., additional, Bordin, Dmitry, additional, Rebours, Vinciane, additional, Mayerle, Julia, additional, Kahraman, Alisan, additional, Rasch, Sebastian, additional, Culver, Emma, additional, Kleger, Alexander, additional, Martínez-Moneo, Emma, additional, Røkke, Ola, additional, Hucl, Tomas, additional, Olesen, Søren S., additional, Bruno, Marco J., additional, Della-Torre, Emanuel, additional, Beuers, Ulrich, additional, Löhr, J.-Matthias, additional, Rosendahl, Jonas, additional, Drewes, A. Mohr, additional, Haas, S.L., additional, Hoyer, B.F., additional, Hampe, J., additional, Hinrichs, C. Noreen, additional, Lerch, M.M., additional, Aghdassi, A.A., additional, Grote, T., additional, Heuser, D.J., additional, Ignatavicius, P., additional, Malecka-Panas, E., additional, Domínguez-Muñoz, J.E., additional, López-Serrano, A., additional, Auriemma, F., additional, Oracz, G., additional, Duman, D., additional, and Gubergrits, N., additional

Published
2024
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15. Pancreatic cancer surveillance: Risk stratification of individuals with a germline CDKN2Apathogenic variant

Author

Klatte, Derk C. F., Meziani, Jihane, Cahen, Djuna L., Diepen, Merel, Bruno, Marco J., Leerdam, Monique E., Dekker, Friedo W., Hooft, Jeanin E., Onnekink, Anke M., Potjer, Thomas P., Levink, Iris J. M., Overbeek, Kasper A., Vleggaar, Frank P., and Voermans, Rogier P.

Abstract

Individuals carrying a germline CDKN2Apathogenic variant (PV) are at a high risk of developing pancreatic ductal adenocarcinoma. Risk stratification could allow tailored surveillance. To develop a Fine‐Gray prediction model for the risk of PDAC in carriers of a CDKN2APV. Data from two large Dutch pancreatic cancer surveillance programs were used. A limited set of predictor variables were selected bsased on previous literature and the clinical expertise of the study group. A total of 506 CDKN2APV carriers were included, among whom we showed a substantial lifetime risk of PDAC (23%). The model identifies having a first‐degree relative with PDAC (B= 0.7256) and a history of smoking (B= 0.4776) as significant risk factors. However, the model shows limited discrimination (c‐statistic 0.64) and calibration. Our study highlights the high lifetime risk of PDAC in carriers of a CDKN2APV. While identifying significant risk factors such as family history of PDAC and smoking, our prediction model shows limited precision, highlighting the need for additional factors such as biomarkers to improve its clinical utility for tailored surveillance of high‐risk individuals.

Published
2024
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16. Pancreatic Cysts.

Author

Gonda, Tamas A., Cahen, Djuna L., and Farrell, James J.

Subjects
*PANCREATIC cysts, *DISEASE risk factors, *NEEDLE biopsy
Abstract

The article provides an overview of pancreatic cysts, focusing on their increasing detection, varied risk of malignancy, and management strategies. Topics discussed include the types of pancreatic cysts and their malignancy risks, diagnostic approaches such as imaging and endoscopic ultrasonography, and guidelines for evaluating and managing cysts based on their potential for cancer.

Published
2024
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18. Intraductal papillary mucinous neoplasms in high-risk individuals:incidence, growth rate, and malignancy risk

Author

Overbeek, Kasper A, Koopmann, Brechtje D M, Levink, Iris J M, Tacelli, Matteo, Erler, Nicole S, Arcidiacono, Paolo Giorgio, Ausems, Margreet G E, Wagner, Anja, van Eijck, Casper H, Koerkamp, Bas Groot, Busch, Olivier R, Besselink, Marc G, van der Vlugt, Manon, van Driel, Lydi M J W, Fockens, Paul, Vleggaar, Frank P, Poley, Jan-Werner, Capurso, Gabriele, Cahen, Djuna L, Bruno, Marco J, Overbeek, Kasper A, Koopmann, Brechtje D M, Levink, Iris J M, Tacelli, Matteo, Erler, Nicole S, Arcidiacono, Paolo Giorgio, Ausems, Margreet G E, Wagner, Anja, van Eijck, Casper H, Koerkamp, Bas Groot, Busch, Olivier R, Besselink, Marc G, van der Vlugt, Manon, van Driel, Lydi M J W, Fockens, Paul, Vleggaar, Frank P, Poley, Jan-Werner, Capurso, Gabriele, Cahen, Djuna L, and Bruno, Marco J

Abstract

BACKGROUND AND AIMS: In high-risk individuals (HRIs), we aimed to assess the cumulative incidence of intraductal papillary mucinous neoplasms (IPMNs) and compare IPMN growth, neoplastic progression rate, and the value of growth as predictor for neoplastic progression to these in sporadic IPMNs.METHODS: We performed annual surveillance of Dutch HRIs, involving carriers of germline pathogenic variants (PV) and PV-negative familial pancreatic cancer (FPC) kindreds. HRIs with IPMNs were compared to Italian individuals without familial risk under surveillance for sporadic IPMNs.RESULTS: 457 HRIs were followed for 48 months (range 2-172); the estimated cumulative IPMN incidence was 46% (95%CI 28-64). In comparison to 442 controls, IPMNs in HRIs were more likely to grow ≥ 2.5 mm/year (31% versus 7%, P<0.001) and to develop worrisome features (32% versus 19%, P=0.010). PV carriers with IPMNs more often displayed neoplastic progression (n=3, 11%; versus n=6, 1%; P=0.011), while FPC kindreds did not (n=0, 0%; P=1.000). The malignancy risk in a PV carrier with an IPMN was 23% for growth rates ≥2.5 mm/year (n=13), 30% for ≥5 mm/year (n=10), and 60% for ≥10 mm/year (n=5).CONCLUSIONS: The cumulative incidence of IPMNs in HRIs is higher than previously reported in the general population. Compared to sporadic IPMNs, they have an increased growth rate. PV carriers with IPMNs are suggested to be at a higher malignancy risk. Intensive follow-up should be considered for PV carriers with an IPMN growing ≥2.5 mm/year, and surgical resection for those growing ≥5 mm/year.

Published
2024

19. Intraductal papillary mucinous neoplasms in high-risk individuals: incidence, growth rate, and malignancy risk

Author

Cancer, Genetica Klinische Genetica, MS MDL 1, Overbeek, Kasper A, Koopmann, Brechtje D M, Levink, Iris J M, Tacelli, Matteo, Erler, Nicole S, Arcidiacono, Paolo Giorgio, Ausems, Margreet G E, Wagner, Anja, van Eijck, Casper H, Koerkamp, Bas Groot, Busch, Olivier R, Besselink, Marc G, van der Vlugt, Manon, van Driel, Lydi M J W, Fockens, Paul, Vleggaar, Frank P, Poley, Jan-Werner, Capurso, Gabriele, Cahen, Djuna L, Bruno, Marco J, Dutch Familial Pancreatic Cancer Surveillance Study work group, Cancer, Genetica Klinische Genetica, MS MDL 1, Overbeek, Kasper A, Koopmann, Brechtje D M, Levink, Iris J M, Tacelli, Matteo, Erler, Nicole S, Arcidiacono, Paolo Giorgio, Ausems, Margreet G E, Wagner, Anja, van Eijck, Casper H, Koerkamp, Bas Groot, Busch, Olivier R, Besselink, Marc G, van der Vlugt, Manon, van Driel, Lydi M J W, Fockens, Paul, Vleggaar, Frank P, Poley, Jan-Werner, Capurso, Gabriele, Cahen, Djuna L, Bruno, Marco J, and Dutch Familial Pancreatic Cancer Surveillance Study work group

Published
2024

20. Type 1 Autoimmune Pancreatitis in Europe:Clinical Profile and Response to Treatment

Author

Overbeek, Kasper A., Poulsen, Jakob L., Lanzillotta, Marco, Vinge-Holmquist, Olof, Macinga, Peter, Demirci, A. Fatih, Sindhunata, Daniko P., Backhus, Johanna, Algül, Hana, Buijs, Jorie, Levy, Philippe, Kiriukova, Mariia, Goni, Elisabetta, Hollenbach, Marcus, Miksch, Rainer C., Kunovsky, Lumir, Vujasinovic, Miroslav, Nikolic, Sara, Dickerson, Luke, Hirth, Michael, Neurath, Markus F., Zumblick, Malte, Vila, Josephine, Jalal, Mustafa, Beyer, Georg, Frost, Fabian, Carrara, Silvia, Kala, Zdenek, Jabandziev, Petr, Sisman, Gurhan, Akyuz, Filiz, Capurso, Gabriele, Falconi, Massimo, Arlt, Alexander, Vleggaar, Frank P., Barresi, Luca, Greenhalf, Bill, Czakó, László, Hegyi, Peter, Hopper, Andrew, Nayar, Manu K., Gress, Thomas M., Vitali, Francesco, Schneider, Alexander, Halloran, Chris M., Trna, Jan, Okhlobystin, Alexey V., Cahen, Djuna L., Bruno, Marco J., Haas, S. L., Overbeek, Kasper A., Poulsen, Jakob L., Lanzillotta, Marco, Vinge-Holmquist, Olof, Macinga, Peter, Demirci, A. Fatih, Sindhunata, Daniko P., Backhus, Johanna, Algül, Hana, Buijs, Jorie, Levy, Philippe, Kiriukova, Mariia, Goni, Elisabetta, Hollenbach, Marcus, Miksch, Rainer C., Kunovsky, Lumir, Vujasinovic, Miroslav, Nikolic, Sara, Dickerson, Luke, Hirth, Michael, Neurath, Markus F., Zumblick, Malte, Vila, Josephine, Jalal, Mustafa, Beyer, Georg, Frost, Fabian, Carrara, Silvia, Kala, Zdenek, Jabandziev, Petr, Sisman, Gurhan, Akyuz, Filiz, Capurso, Gabriele, Falconi, Massimo, Arlt, Alexander, Vleggaar, Frank P., Barresi, Luca, Greenhalf, Bill, Czakó, László, Hegyi, Peter, Hopper, Andrew, Nayar, Manu K., Gress, Thomas M., Vitali, Francesco, Schneider, Alexander, Halloran, Chris M., Trna, Jan, Okhlobystin, Alexey V., Cahen, Djuna L., Bruno, Marco J., and Haas, S. L.

Abstract

Background & Aims: Autoimmune pancreatitis (AIP) is an immune-mediated disease of the pancreas with distinct pathophysiology and manifestations. Our aims were to characterize type 1 AIP in a large pan-European cohort and study the effectiveness of current treatment regimens. Methods: We retrospectively analyzed adults diagnosed since 2005 with type 1 or not-otherwise-specified AIP in 42 European university hospitals. Type 1 AIP was uniformly diagnosed using specific diagnostic criteria. Patients with type 2 AIP and those who had undergone pancreatic surgery were excluded. The primary end point was complete remission, defined as the absence of clinical symptoms and resolution of the index radiologic pancreatic abnormalities attributed to AIP. Results: We included 735 individuals with AIP (69% male; median age, 57 years; 85% White). Steroid treatment was started in 634 patients, of whom 9 (1%) were lost to follow-up. The remaining 625 had a 79% (496/625) complete, 18% (111/625) partial, and 97% (607/625) cumulative remission rate, whereas 3% (18/625) did not achieve remission. No treatment was given in 95 patients, who had a 61% complete (58/95), 19% partial (18/95), and 80% cumulative (76/95) spontaneous remission rate. Higher (≥0.4 mg/kg/day) corticosteroid doses were no more effective than lower (<0.4 mg/kg/day) doses (odds ratio, 0.428; 95% confidence interval, 0.054–3.387) and neither was a starting dose duration >2 weeks (odds ratio, 0.908; 95% confidence interval, 0.818–1.009). Elevated IgG4 levels were independently associated with a decreased chance of complete remission (odds ratio, 0.639; 95% confidence interval, 0.427–0.955). Relapse occurred in 30% of patients. Relapses within 6 months of remission induction were independent of the steroid-tapering duration, induction treatment duration, and total cumulative dose. Conclusions: Patients with type 1 AIP and elevated IgG4 level may need closer monitoring. For remission induction, a starting dose

Published
2024

22. The Natural Disease Course of Pancreatic Cyst–Associated Neoplasia, Dysplasia, and Ductal Adenocarcinoma:Results of a Microsimulation Model

Author

Koopmann, Brechtje D.M., Dunnewind, Niels, van Duuren, Luuk A., Lansdorp-Vogelaar, Iris, Naber, Steffie K., Cahen, Djuna L., Bruno, Marco J., de Kok, Inge M.C.M., Koopmann, Brechtje D.M., Dunnewind, Niels, van Duuren, Luuk A., Lansdorp-Vogelaar, Iris, Naber, Steffie K., Cahen, Djuna L., Bruno, Marco J., and de Kok, Inge M.C.M.

Abstract

Background & Aims: Estimates on the progression of precursor lesions to pancreatic cancer (PC) are scarce. We used microsimulation modeling to gain insight into the natural disease course of PC and its precursors. This information is pivotal to explore the efficacy of PC screening. Methods: A Microsimulation Screening Analysis model was developed in which pancreatic intraepithelial neoplasms and cysts can evolve from low-grade dysplasia (LGD) to high-grade dysplasia (HGD) to PC. The model was calibrated to Dutch PC incidence data and Japanese precursor prevalence data (autopsy cases without PC) and provides estimates of PC progression (precursor lesion onset and stage duration).Results: Mean LGD state durations of cysts and pancreatic intraepithelial neoplasms were 15.8 years and 17.1 years, respectively. Mean HGD state duration was 5.8 years. For lesions that progress to PC, the mean duration was 4.8–4.9 years for LGD lesions and 4.0–4.1 years for HGD lesions. In 13.7% of individuals who developed PC, the HGD state lasted less than 1 year. The probability that an individual at age 50 years developed PC in the next 20 years was estimated to be 1.8% in the presence of any cyst and 6.1% in case of an LGD mucinous cyst. This 20-year PC risk was estimated to be 5.1% for individuals with an LGD pancreatic intraepithelial neoplasm. Conclusions: Mean duration of HGD lesions before development of PC was estimated to be 4.0 years. This implies a window of opportunity for screening, presuming the availability of a reliable diagnostic test. The probability that an LGD cyst will progress to cancer was predicted to be low.

Published
2023

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

Abstract

Background: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. Methods: 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.Results: 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). Conclusions: 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 imp

Published
2023

24. An 8q24 Gain in Pancreatic Juice Is a Candidate Biomarker for the Detection of Pancreatic Cancer

Author

Levink, Iris J.M., Srebniak, Malgorzata I., De Valk, Walter G., van Veghel-Plandsoen, Monique M., Wagner, Anja, Cahen, Djuna L., Fuhler, Gwenny M., Bruno, Marco J., Levink, Iris J.M., Srebniak, Malgorzata I., De Valk, Walter G., van Veghel-Plandsoen, Monique M., Wagner, Anja, Cahen, Djuna L., Fuhler, Gwenny M., and Bruno, Marco J.

Abstract

Secretin-stimulated pancreatic juice (PJ), collected from the duodenum, presents a valuable biomarker source for the (earlier) detection of pancreatic cancer (PC). Here, we evaluate the feasibility and performance of shallow sequencing to detect copy number variations (CNVs) in cell-free DNA (cfDNA) from PJ for PC detection. First, we confirmed the feasibility of shallow sequencing in PJ (n = 4), matched plasma (n = 3) and tissue samples (n = 4, microarray). Subsequently, shallow sequencing was performed on cfDNA from PJ of 26 cases (25 sporadic PC, 1 high-grade dysplasia) and 19 controls with a hereditary or familial increased risk of PC. 40 of the 45 PJ samples met the quality criteria for cfDNA analysis. Nine individuals had an 8q24 gain (oncogene MYC; 23%; eight cases (33%) and one control (6%), p = 0.04); six had both a 2q gain (STAT1) and 5p loss (CDH10; 15%; four cases (7%) and two controls (13%), p = 0.72). The presence of an 8q24 gain differentiated the cases and controls, with a sensitivity of 33% (95% CI 16–55%) and specificity of 94% (95% CI 70–100%). The presence of either an 8q24 or 2q gain with a 5p loss was related to a sensitivity of 50% (95% CI 29–71%) and specificity of 81% (95% CI 54–96%). Shallow sequencing of PJ is feasible. The presence of an 8q24 gain in PJ shows promise as a biomarker for the detection of PC. Further research is required with a larger sample size and consecutively collected samples in high-risk individuals prior to implementation in a surveillance cohort.

Published
2023

25. The impact of pancreatic cancer screening on life expectancy:A systematic review of modeling studies

Author

Koopmann, Brechtje D.M., Omidvari, Amir Houshang, Lansdorp-Vogelaar, Iris, Cahen, Djuna L., Bruno, Marco J., de Kok, Inge M.C.M., Koopmann, Brechtje D.M., Omidvari, Amir Houshang, Lansdorp-Vogelaar, Iris, Cahen, Djuna L., Bruno, Marco J., and de Kok, Inge M.C.M.

Abstract

Evidence supporting the effectiveness of pancreatic cancer (PC) screening is scant. Most clinical studies concern small populations with short follow-up durations. Mathematical models are useful to estimate long-term effects of PC screening using short-term indicators. This systematic review aims to evaluate the impact of PC screening on life expectancy (LE) in model-based studies. Therefore, we searched four databases (Embase, Medline, Web-of-science, Cochrane) until 30 May 2022 to identify model-based studies evaluating the impact of PC screening on LE in different risk populations. Two authors independently screened identified papers, extracted data and assessed the methodological quality of studies. A descriptive analysis was performed and the impact of screening strategies on LE of different risk groups was reported. Our search resulted in 419 studies, of which eight met the eligibility criteria (mathematical model, PC screening, LE). Reported relative risks (RR) for PC varied from 1 to 70. In higher risk individuals (RR > 5), annual screening (by imaging with 56% sensitivity for HGD/early stage PC) predicted to increase LE of screened individuals by 20 to 260 days. In the general population, one-time PC screening was estimated to decrease LE (2-110 days), depending on the test characteristics and treatment mortality risk. In conclusion, although the models use different and sometimes outdated or unrealistic assumptions, it seems that PC screening in high-risk populations improves LE, and that this gain increases with a higher PC risk. Updated model studies, with data from large clinical trials are necessary to predict the long-term effect of PC screening more accurately.

Published
2023

26. Intraductal Papillary Mucinous Neoplasms in High-Risk Individuals: Incidence, Growth Rate, and Malignancy Risk

Author

Overbeek, Kasper A., primary, Koopmann, Brechtje D.M., additional, Levink, Iris J.M., additional, Tacelli, Matteo, additional, Erler, Nicole S., additional, Arcidiacono, Paolo Giorgio, additional, Ausems, Margreet G.E., additional, Wagner, Anja, additional, van Eijck, Casper H., additional, Groot Koerkamp, Bas, additional, Busch, Olivier R., additional, Besselink, Marc G., additional, van der Vlugt, Manon, additional, van Driel, Lydi M.J.W., additional, Fockens, Paul, additional, Vleggaar, Frank P., additional, Poley, Jan-Werner, additional, Capurso, Gabriele, additional, Cahen, Djuna L., additional, and Bruno, Marco J., additional

Published
2023
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29. Reply

Author

Overbeek, Kasper A., Cahen, Djuna L., and Bruno, Marco J.

Published
2024
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30. International external validation of a stratification tool to identify branch-duct intraductal papillary mucinous neoplasms at lowest risk of progression

Author

Overbeek, Kasper A., van Leeuwen, Nikki, Tacelli, Matteo, Anwar, Muhammad S., Yousaf, Muhammad N., Chhoda, Ankit, Arcidiacono, Paolo Giorgio, Gonda, Tamas A., Wallace, Michael B., Capurso, Gabriele, Farrell, James J., Cahen, Djuna L., Bruno, Marco J., Overbeek, Kasper A., van Leeuwen, Nikki, Tacelli, Matteo, Anwar, Muhammad S., Yousaf, Muhammad N., Chhoda, Ankit, Arcidiacono, Paolo Giorgio, Gonda, Tamas A., Wallace, Michael B., Capurso, Gabriele, Farrell, James J., Cahen, Djuna L., and Bruno, Marco J.

Abstract

Background: Identifying branch-duct intraductal papillary mucinous neoplasms (BD-IPMNs) at lowest risk of progression may allow for a reduced intensity of surveillance. Objective: We aimed to externally validate the previously developed Dutch-American Risk stratification Tool (DART-1; https://rtools.mayo.edu/DART/), which identifies cysts at low risk of developing worrisome features (WFs) or high-risk stigmata (HRS). Methods: Three prospective cohorts of individuals under surveillance for BD-IPMNs were combined, independent from the original development cohort. We assessed the performance (discrimination and calibration) of DART-1, a multivariable Cox-proportional logistic regression model with five predictors for the development of WFs or HRS. Results: Of 832 individuals (mean age 77 years, SD 11.5) under surveillance for a median of 40 months (IQR 44), 163 (20%) developed WFs or HRS. DART-1's discriminative ability (C-statistic 0.68) was similar to that in the development cohort (0.64–0.72) and showed moderate calibration. DART-1 adequately estimated the risk for patients in the middle risk quintile, and slightly underestimated it in the lowest quintiles. Their range of predicted versus observed 3-year risk was 0%–0% versus 0%–3.7% for Q1; 0.3%–0.4% versus 3%–11% for Q2; and 2.6%–3% versus 2.4%–9.8% for Q3. The development of WFs or HRS was associated with pancreatic cancer (p < 0.001). Vice versa, in absence of WFs or HRS, the risk of malignancy was low (0.3%). Conclusions: The performance of DART-1 to predict the development of WFs or HRS in BD-IPMN was validated in an external international cohort, with a discriminative ability equal as in the development cohort. Risk estimations were most accurate for patients with BD-IPMNs in the middle risk quintile and slightly underestimated in the lowest quintiles.

Published
2022

31. Long-term yield of pancreatic cancer surveillance in high-risk individuals

Author

Overbeek, Kasper A., Levink, Iris J. M., Koopmann, Brechtje D. M., Harinck, Femme, Konings, Ingrid C. A. W., Ausems, Margreet G. E. M., Wagner, Anja, Fockens, Paul, van Eijck, Casper H., Koerkamp, Bas Groot, Busch, Olivier R. C., Besselink, Marc G., Bastiaansen, Barbara A. J., van Driel, Lydi M. J. W., Erler, Nicole S., Vleggaar, Frank P., Poley, Jan-Werner, Cahen, Djuna L., van Hooft, Jeanin E., Bruno, Marco J., Overbeek, Kasper A., Levink, Iris J. M., Koopmann, Brechtje D. M., Harinck, Femme, Konings, Ingrid C. A. W., Ausems, Margreet G. E. M., Wagner, Anja, Fockens, Paul, van Eijck, Casper H., Koerkamp, Bas Groot, Busch, Olivier R. C., Besselink, Marc G., Bastiaansen, Barbara A. J., van Driel, Lydi M. J. W., Erler, Nicole S., Vleggaar, Frank P., Poley, Jan-Werner, Cahen, Djuna L., van Hooft, Jeanin E., and Bruno, Marco J.

Abstract

Objective We aimed to determine the long-term yield of pancreatic cancer surveillance in hereditary predisposed high-risk individuals.Design From 2006 to 2019, we prospectively enrolled asymptomatic individuals with an estimated 10% or greater lifetime risk of pancreatic ductal adenocarcinoma (PDAC) after obligatory evaluation by a clinical geneticist and genetic testing, and subjected them to annual surveillance with both endoscopic ultrasonography (EUS) and MRI/cholangiopancreatography (MRI/MRCP) at each visit.Results 366 individuals (201 mutation-negative familial pancreatic cancer (FPC) kindreds and 165 PDAC susceptibility gene mutation carriers; mean age 54 years, SD 9.9) were followed for 63 months on average (SD 43.2). Ten individuals developed PDAC, of which four presented with a symptomatic interval carcinoma and six underwent resection. The cumulative PDAC incidence was 9.3% in the mutation carriers and 0% in the FPC kindreds (p<0.001). Median PDAC survival was 18 months (range 1-32). Surgery was performed in 17 individuals (4.6%), whose pathology revealed 6 PDACs (3 T1N0M0), 7 low-grade precursor lesions, 2 neuroendocrine tumours <2 cm, 1 autoimmune pancreatitis and in 1 individual no abnormality. There was no surgery-related mortality. EUS detected more solid lesions than MRI/MRCP (100% vs 22%, p<0.001), but less cystic lesions (42% vs 83%, p<0.001).Conclusion The diagnostic yield of PDAC was substantial in established high-risk mutation carriers, but non-existent in the mutation-negative proven FPC kindreds. Nevertheless, timely identification of resectable lesions proved challenging despite the concurrent use of two imaging modalities, with EUS outperforming MRI/MRCP. Overall, surveillance by imaging yields suboptimal results with a clear need for more sensitive diagnostic markers, including biomarkers.

Published
2022

32. Neoantigen Quantity and Quality in Relation to Pancreatic Cancer Survival

Author

Levink, Iris J.M., Brosens, Lodewijk A.A., Rensen, Sander S., Aberle, Merel R., Olde Damink, Steven S.W., Cahen, Djuna L., Buschow, Sonja I., Fuhler, Gwenny M., Peppelenbosch, Maikel P., Bruno, Marco J., Levink, Iris J.M., Brosens, Lodewijk A.A., Rensen, Sander S., Aberle, Merel R., Olde Damink, Steven S.W., Cahen, Djuna L., Buschow, Sonja I., Fuhler, Gwenny M., Peppelenbosch, Maikel P., and Bruno, Marco J.

Abstract

Introduction: Factors underlying antitumor immunity in pancreatic cancer (PC) are poorly understood. We hypothesized that not neoantigen quantity, but quality, is related to immune cell infiltration and survival. Methodology: We performed genomic and transcriptomic profiling of paired normal, tumor tissue of 13 patients with PC with distinct survival times. Additionally, neoantigens prediction and immunological profiling were performed. Results: The proportion of neoantigens with a low similarity-to-self score was higher in short-term survivors (p < 0.0001), while mutational load and burden, similarity-to-known-pathogens, and immunogenicity of neoantigens were not associated with immune cell infiltration or survival. Discussion: No tumor mutational load or neoantigen quantity, but low similarity-to-self score, was associated with immune cell infiltration and survival.

Published
2022

33. Size and Concentration of Extracellular Vesicles in Pancreatic Juice from Patients with Pancreatic Ductal Adenocarcinoma

Author

Nesteruk, Kateryna, Levink, Iris J.M., Dits, Natasja F.J., Cahen, Djuna L., Peppelenbosch, Maikel P., Bruno, Marco J., Fuhler, Gwenny M., Nesteruk, Kateryna, Levink, Iris J.M., Dits, Natasja F.J., Cahen, Djuna L., Peppelenbosch, Maikel P., Bruno, Marco J., and Fuhler, Gwenny M.

Abstract

INTRODUCTION:Extracellular vesicles (EVs) and their cargo may provide promising biomarkers for the early detection of pancreatic ductal adenocarcinoma (PDAC). Although blood-borne EVs are most frequently studied as cancer biomarkers, pancreatic juice (PJ) may represent a better biomarker source because it is in close contact with the ductal cells from which PDAC arises. It is, as yet, unknown whether PDAC results in a distinct type or increased number of particles in PJ and whether this has diagnostic value.METHODS:Secretin-stimulated PJ was collected from the duodenum of 54 cases and 117 nonmalignant controls under surveillance for PDAC. Serum was available for a subset of these individuals. The vesicular composition of these biofluids was analyzed with nanoparticle tracking analysis.RESULTS:The concentration of EVs did not differ between controls and PDAC cases. However, a higher number of large vesicles were found in PJ (but not serum) for patients with PDAC compared with controls.DISCUSSION:The composition of isolated EVs from PJ, but not serum, is altered in patients with PDAC. This suggests that PJ may carry disease-specific markers not present in serum and provides a valuable biomarker source for PDAC diagnosis. The nature of the larger particles in EV isolates from PJ of PDAC cases requires further investigation.

Published
2022

34. Neoantigen Quantity and Quality in Relation to Pancreatic Cancer Survival

Author

Pathologie Pathologen staf, Cancer, Levink, Iris J M, Brosens, Lodewijk A A, Rensen, Sander S, Aberle, Merel R, Olde Damink, Steven S W, Cahen, Djuna L, Buschow, Sonja I, Fuhler, Gwenny M, Peppelenbosch, Maikel P, Bruno, Marco J, Pathologie Pathologen staf, Cancer, Levink, Iris J M, Brosens, Lodewijk A A, Rensen, Sander S, Aberle, Merel R, Olde Damink, Steven S W, Cahen, Djuna L, Buschow, Sonja I, Fuhler, Gwenny M, Peppelenbosch, Maikel P, and Bruno, Marco J

Published
2022

35. Timeline of development of pancreatic cancer and implications for successful early detection in high-risk individuals

Author

Cancer, Genetica Klinische Genetica, MS MDL 1, Overbeek, Kasper A, Goggins, Michael G, Dbouk, Mohamad, Levink, Iris J M, Koopmann, Brechtje D M, Chuidian, Miguel, Konings, Ingrid C A W, Paiella, Salvatore, Earl, Julie, Fockens, Paul, Gress, Thomas M, Ausems, Margreet G E M, Poley, Jan-Werner, Thosani, Nirav C, Half, Elizabeth, Lachter, Jesse, Stoffel, Elena M, Kwon, Richard S, Stoita, Alina, Kastrinos, Fay, Lucas, Aimee L, Syngal, Sapna, Brand, Randall E, Chak, Amitabh, Carrato, Alfredo, Vleggaar, Frank P, Bartsch, Detlef K, van Hooft, Jeanin E, Cahen, Djuna L, Canto, Marcia Irene, Bruno, Marco J, International Cancer of the Pancreas Screening Consortium, Cancer, Genetica Klinische Genetica, MS MDL 1, Overbeek, Kasper A, Goggins, Michael G, Dbouk, Mohamad, Levink, Iris J M, Koopmann, Brechtje D M, Chuidian, Miguel, Konings, Ingrid C A W, Paiella, Salvatore, Earl, Julie, Fockens, Paul, Gress, Thomas M, Ausems, Margreet G E M, Poley, Jan-Werner, Thosani, Nirav C, Half, Elizabeth, Lachter, Jesse, Stoffel, Elena M, Kwon, Richard S, Stoita, Alina, Kastrinos, Fay, Lucas, Aimee L, Syngal, Sapna, Brand, Randall E, Chak, Amitabh, Carrato, Alfredo, Vleggaar, Frank P, Bartsch, Detlef K, van Hooft, Jeanin E, Cahen, Djuna L, Canto, Marcia Irene, Bruno, Marco J, and International Cancer of the Pancreas Screening Consortium

Published
2022

36. 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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37. International external validation of a stratification tool to identify branch‐duct intraductal papillary mucinous neoplasms at lowest risk of progression

Author

Overbeek, Kasper A., primary, van Leeuwen, Nikki, additional, Tacelli, Matteo, additional, Anwar, Muhammad S., additional, Yousaf, Muhammad N., additional, Chhoda, Ankit, additional, Arcidiacono, Paolo Giorgio, additional, Gonda, Tamas A., additional, Wallace, Michael B., additional, Capurso, Gabriele, additional, Farrell, James J., additional, Cahen, Djuna L., additional, and Bruno, Marco J., additional

Published
2022
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39. Neoantigen Quantity and Quality in Relation to Pancreatic Cancer Survival

Author

Levink, Iris J. M., primary, Brosens, Lodewijk A. A., additional, Rensen, Sander S., additional, Aberle, Merel R., additional, Olde Damink, Steven S. W., additional, Cahen, Djuna L., additional, Buschow, Sonja I., additional, Fuhler, Gwenny M., additional, Peppelenbosch, Maikel P., additional, and Bruno, Marco J., additional

Published
2022
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40. The impact of pancreatic cancer screening on life expectancy: A systematic review of modeling studies.

Author

Koopmann, Brechtje D. M., Omidvari, Amir‐Houshang, Lansdorp‐Vogelaar, Iris, Cahen, Djuna L., Bruno, Marco J., and de Kok, Inge M. C. M.

Subjects
EARLY detection of cancer, PANCREATIC cancer, LIFE expectancy, MEDICAL screening, DATABASE searching
Abstract

Evidence supporting the effectiveness of pancreatic cancer (PC) screening is scant. Most clinical studies concern small populations with short follow‐up durations. Mathematical models are useful to estimate long‐term effects of PC screening using short‐term indicators. This systematic review aims to evaluate the impact of PC screening on life expectancy (LE) in model‐based studies. Therefore, we searched four databases (Embase, Medline, Web‐of‐science, Cochrane) until 30 May 2022 to identify model‐based studies evaluating the impact of PC screening on LE in different risk populations. Two authors independently screened identified papers, extracted data and assessed the methodological quality of studies. A descriptive analysis was performed and the impact of screening strategies on LE of different risk groups was reported. Our search resulted in 419 studies, of which eight met the eligibility criteria (mathematical model, PC screening, LE). Reported relative risks (RR) for PC varied from 1 to 70. In higher risk individuals (RR > 5), annual screening (by imaging with 56% sensitivity for HGD/early stage PC) predicted to increase LE of screened individuals by 20 to 260 days. In the general population, one‐time PC screening was estimated to decrease LE (2‐110 days), depending on the test characteristics and treatment mortality risk. In conclusion, although the models use different and sometimes outdated or unrealistic assumptions, it seems that PC screening in high‐risk populations improves LE, and that this gain increases with a higher PC risk. Updated model studies, with data from large clinical trials are necessary to predict the long‐term effect of PC screening more accurately. [ABSTRACT FROM AUTHOR]

Published
2023
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42. Long-term yield of pancreatic cancer surveillance in high-risk individuals

Author

Overbeek, Kasper A, Levink, Iris J M, Koopmann, Brechtje D M, Harinck, Femme, Konings, Ingrid C A W, Ausems, Margreet G E M, Wagner, Anja, Fockens, Paul, van Eijck, Casper H, Groot Koerkamp, Bas, Busch, Olivier R C, Besselink, Marc G, Bastiaansen, Barbara A J, van Driel, Lydi M J W, Erler, Nicole S, Vleggaar, Frank P, Poley, Jan-Werner, Cahen, Djuna L, van Hooft, Jeanin E, and Bruno, Marco J

Abstract

ObjectiveWe aimed to determine the long-term yield of pancreatic cancer surveillance in hereditary predisposed high-risk individuals.DesignFrom 2006 to 2019, we prospectively enrolled asymptomatic individuals with an estimated 10% or greater lifetime risk of pancreatic ductal adenocarcinoma (PDAC) after obligatory evaluation by a clinical geneticist and genetic testing, and subjected them to annual surveillance with both endoscopic ultrasonography (EUS) and MRI/cholangiopancreatography (MRI/MRCP) at each visit.Results366 individuals (201 mutation-negative familial pancreatic cancer (FPC) kindreds and 165 PDAC susceptibility gene mutation carriers; mean age 54 years, SD 9.9) were followed for 63 months on average (SD 43.2). Ten individuals developed PDAC, of which four presented with a symptomatic interval carcinoma and six underwent resection. The cumulative PDAC incidence was 9.3% in the mutation carriers and 0% in the FPC kindreds (p<0.001). Median PDAC survival was 18 months (range 1–32). Surgery was performed in 17 individuals (4.6%), whose pathology revealed 6 PDACs (3 T1N0M0), 7 low-grade precursor lesions, 2 neuroendocrine tumours <2 cm, 1 autoimmune pancreatitis and in 1 individual no abnormality. There was no surgery-related mortality. EUS detected more solid lesions than MRI/MRCP (100% vs 22%, p<0.001), but less cystic lesions (42% vs 83%, p<0.001).ConclusionThe diagnostic yield of PDAC was substantial in established high-risk mutation carriers, but non-existent in the mutation-negative proven FPC kindreds. Nevertheless, timely identification of resectable lesions proved challenging despite the concurrent use of two imaging modalities, with EUS outperforming MRI/MRCP. Overall, surveillance by imaging yields suboptimal results with a clear need for more sensitive diagnostic markers, including biomarkers.

Published
2022
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43. Pancreatic cancer surveillance: Risk stratification of individuals with a germline CDKN2A pathogenic variant.

Author

Klatte DCF, Meziani J, Cahen DL, van Diepen M, Bruno MJ, and van Leerdam ME

Subjects
Humans, Male, Risk Assessment methods, Female, Middle Aged, Risk Factors, Aged, Netherlands epidemiology, Adult, Smoking adverse effects, Smoking epidemiology, Early Detection of Cancer methods, Pancreatic Neoplasms genetics, Pancreatic Neoplasms epidemiology, Germ-Line Mutation, Cyclin-Dependent Kinase Inhibitor p16 genetics, Carcinoma, Pancreatic Ductal genetics, Carcinoma, Pancreatic Ductal epidemiology, Genetic Predisposition to Disease
Abstract

Background: Individuals carrying a germline CDKN2A pathogenic variant (PV) are at a high risk of developing pancreatic ductal adenocarcinoma. Risk stratification could allow tailored surveillance., Objective: To develop a Fine-Gray prediction model for the risk of PDAC in carriers of a CDKN2A PV., Methods: Data from two large Dutch pancreatic cancer surveillance programs were used. A limited set of predictor variables were selected bsased on previous literature and the clinical expertise of the study group., Results: A total of 506 CDKN2A PV carriers were included, among whom we showed a substantial lifetime risk of PDAC (23%). The model identifies having a first-degree relative with PDAC (B = 0.7256) and a history of smoking (B = 0.4776) as significant risk factors. However, the model shows limited discrimination (c-statistic 0.64) and calibration., Conclusion: Our study highlights the high lifetime risk of PDAC in carriers of a CDKN2A PV. While identifying significant risk factors such as family history of PDAC and smoking, our prediction model shows limited precision, highlighting the need for additional factors such as biomarkers to improve its clinical utility for tailored surveillance of high-risk individuals., (© 2024 The Author(s). United European Gastroenterology Journal published by Wiley Periodicals LLC on behalf of United European Gastroenterology.)

Published
2024
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45. Small cyst size and lack of growth as negative predictors of malignant transformation in low-risk intraductal papillary mucinous neoplasms of the pancreas: A systematic review and meta-analysis.

Author

Meziani J, Sprij MLJA, Fuhler GM, Bruno MJ, Marchegiani G, and Cahen DL

Abstract

Background and Aim: For branch-duct intraductal papillary mucinous neoplasms (BD-IPMNs) without worrisome features (WFs) or high-risk stigmata (HRS), current guidelines recommend surveillance. However, these intraductal papillary mucinous neoplasm (IPMNs), especially the small and stable-sized ones, carry a low risk of malignant transformation. Our aim was to assess whether small cyst size and absence of rapid growth provide reassurance against the development of WFs/HRS and malignancy (high-grade dysplasia (HGD) or pancreatic cancer (PC))., Methods: PubMed/Medline, Embase, the Cochrane Library and the Web of Science Core Collection were systematically searched from inception to May 2023 to identify studies investigating surveillance outcomes of low-risk BD-IPMNs. Studies assessing baseline cyst size and/or growth in relation to WFs/HRS and/or HGD/PC were included. The Newcastle-Ottawa scale tool was used to assess study quality., Results: Of the 1937 identified manuscripts, 21 studies were eligible for inclusion. The quality of these studies was considered reasonable. A negative association between cyst size and WFs/HRS development was found in 11 out of 13 relevant studies, but only one out of nine studies reported a negative association between size and malignancy. Regarding cyst growth, four out of six studies described a negative association with the development of WFs/HRS, and all six reported a negative association with malignancy. The pooled relative risk (RR) of developing WFs/HRS or malignancy for cysts ≤15 mm was 0.37 (95% CI 0.25-0.57) and the RR of developing malignancy for cyst growth <2-2.5 mm/year was 0.04 (95% CI 0.02-0.09))., Conclusion: This systematic review and meta-analysis shows that small and stable-sized low-risk BD-IPMNs are associated with a markedly low progression rate, with stable cyst size being the most reassuring feature. Because of substantial heterogeneity in definitions and reported outcome measures, prospective studies are needed to confirm that surveillance of small and stable sized cyst can be de-intensified or even discontinued., (© 2024 The Author(s). United European Gastroenterology Journal published by Wiley Periodicals LLC on behalf of United European Gastroenterology.)

Published
2024
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