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2. Precision radiotherapy using MR-linac for pancreatic neuroendocrine tumors in MEN1 patients (PRIME): a protocol for a phase I-II trial, and systematic review on available evidence for radiotherapy of pNETs.

Author

Vliembergen, E.N.M. van, Eijkelenkamp, H., Valk, G.D., Vriens, M.R., Meijer, G.J, Intven, M.P.W., Laat, J.M. de, Vliembergen, E.N.M. van, Eijkelenkamp, H., Valk, G.D., Vriens, M.R., Meijer, G.J, Intven, M.P.W., and Laat, J.M. de

Abstract

Contains fulltext : 293797.pdf (Publisher’s version ) (Open Access), BACKGROUND: Surgical resection is the standard of care for the treatment of pancreatic neuro-endocrine tumors (pNETs) in patients with Multiple Endocrine Neoplasia Type 1 (MEN1). However, surgery can cause significant short- and long-term morbidity. Magnetic resonance-guided radiotherapy (MRgRT) is a potential effective treatment with little side effects. With traditional radiotherapy techniques, irradiation of pancreatic tumors to high dose levels was hampered by poor visibility of the tumor during treatment. MRgRT uses onboard MRI to guide the treatment, thereby enabling delivery of ablative irradiation doses to the tumor, while sparing surrounding tissues. In this study, we describe results from a systematic review assessing efficacy of radiotherapy in pNET and present the protocol of the PRIME study. METHODS: PubMed, Embase and Cochrane Library were searched for articles assessing efficacy and side effects of radiotherapy for the treatment of pNETs. Risk of bias was assessed using the ROBINS-I Risk of Bias Tool for observational studies. Descriptive statistics were used to describe results of included trials. RESULTS: Four studies comprising of 33 patients treated by conventional radiotherapy were included. Despite the heterogeneity of studies, radiotherapy appeared to be effective for the treatment of pNETs with most patients responding (45.5%) or stabilizing (42.4%) in tumor size. CONCLUSION AND TRIAL DESIGN: Due to the limited literature available and concerns about damage to surrounding tissue, conventional radiotherapy is currently little used for pNETs. The PRIME study is a phase I-II trial with a single arm prospective cohort study design, investigating the efficacy of MRgRT in MEN1 patients with pNET. MEN1 patients with growing pNETs with a size between 1.0 and 3.0 cm without malignant features are eligible for inclusion. Patients are treated with 40 Gy in 5 fractions on the pNET, using online adaptive MRgRT on a 1.5T MR-linac. The primary endpoint is th

Published
2023

3. Reducing failures in daily medical practice: Healthcare failure mode and effect analysis combined with computer simulation

Author

Leeftink, A.G., Visser, J, Laat, J.M. de, Meij, N.T.M. van der, Vos, J.B., Valk, G.D., Leeftink, A.G., Visser, J, Laat, J.M. de, Meij, N.T.M. van der, Vos, J.B., and Valk, G.D.

Abstract

Item does not contain fulltext, This study proposes a risk analysis approach for complex healthcare processes that combines qualitative and quantitative methods to improve patient safety. We combine Healthcare Failure Mode and Effect Analysis with Computer Simulation (HFMEA-CS), to overcome widely recognised HFMEA drawbacks regarding the reproducibility and validity of the outcomes due to human interpretation, and show the application of this methodology in a complex healthcare setting. HFMEA-CS is applied to analyse drug adherence performance in the surgical admission to discharge process of pheochromocytoma patients. The multidisciplinary team identified and scored the failure modes, and the simulation model supported in prioritisation of failure modes, uncovered dependencies between failure modes, and predicted the impact of measures on system behaviour. The results show that drug adherence, defined as the percentage of required drugs received at the right time, can be significantly improved with 12%, to reach a drug adherence of 99%. We conclude that HFMEA-CS is both a viable and effective risk analysis approach, combining strengths of expert opinion and quantitative analysis, for analysing human-system interactions in socio-technical systems. Practitioner summary: We propose combining Healthcare Failure Mode and Effects Analysis with Computer Simulation (HFMEA-CS) for prospective risk analysis of complex and potentially harmful processes, to prevent critical incidents from occurring. HFMEA-CS combines expert opinions with quantitative analyses, such that the results are more reliable, reproducible, and fitting for complex healthcare settings.

Published
2021

4. Reducing failures in daily medical practice: Healthcare failure mode and effect analysis combined with computer simulation

Author

Leeftink, A.G., Visser, J, Laat, J.M. de, Meij, N.T.M. van der, Vos, J.B., Valk, G.D., Leeftink, A.G., Visser, J, Laat, J.M. de, Meij, N.T.M. van der, Vos, J.B., and Valk, G.D.

Abstract

Contains fulltext : 245827.pdf (Publisher’s version ) (Open Access), This study proposes a risk analysis approach for complex healthcare processes that combines qualitative and quantitative methods to improve patient safety. We combine Healthcare Failure Mode and Effect Analysis with Computer Simulation (HFMEA-CS), to overcome widely recognised HFMEA drawbacks regarding the reproducibility and validity of the outcomes due to human interpretation, and show the application of this methodology in a complex healthcare setting. HFMEA-CS is applied to analyse drug adherence performance in the surgical admission to discharge process of pheochromocytoma patients. The multidisciplinary team identified and scored the failure modes, and the simulation model supported in prioritisation of failure modes, uncovered dependencies between failure modes, and predicted the impact of measures on system behaviour. The results show that drug adherence, defined as the percentage of required drugs received at the right time, can be significantly improved with 12%, to reach a drug adherence of 99%. We conclude that HFMEA-CS is both a viable and effective risk analysis approach, combining strengths of expert opinion and quantitative analysis, for analysing human-system interactions in socio-technical systems. Practitioner summary: We propose combining Healthcare Failure Mode and Effects Analysis with Computer Simulation (HFMEA-CS) for prospective risk analysis of complex and potentially harmful processes, to prevent critical incidents from occurring. HFMEA-CS combines expert opinions with quantitative analyses, such that the results are more reliable, reproducible, and fitting for complex healthcare settings.

Published
2021

5. Long-Term Natural Course of Small Nonfunctional Pancreatic Neuroendocrine Tumors in MEN1-Results From the Dutch MEN1 Study Group

Author

Pieterman, C.R.C., Laat, J.M. de, Twisk, J.W.R., Leeuwaarde, R.S. van, Herder, W.W. de, Dreijerink, K.M.A., Hermus, A.R., Dekkers, O.M., Horst-Schrivers, A.N.A. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H.M. Borel, Vriens, M.R., Valk, G.D., Pieterman, C.R.C., Laat, J.M. de, Twisk, J.W.R., Leeuwaarde, R.S. van, Herder, W.W. de, Dreijerink, K.M.A., Hermus, A.R., Dekkers, O.M., Horst-Schrivers, A.N.A. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H.M. Borel, Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, Background: Pancreatic neuroendocrine tumors (pNETs) are highly prevalent in patients with multiple endocrine neoplasia type 1 (MEN1), and metastatic disease is an important cause of MEN1-related mortality. Especially small nonfunctional (NF) pNETs pose a challenge to the treating physician and more information is needed regarding their natural course. We assessed long-term natural history of small NF-pNETs and its modifiers in the Dutch MEN1 population. Patients and Methods: Retrospective longitudinal observational cohort study of patients with small (<2 cm) NF-pNETs from the Dutch national MEN1 database, which includes >90% of the Dutch MEN1 population. Modifiers of long-term natural course were analyzed using linear mixed-models analysis. Results: Growth rate of the 115 included small NF-pNETs from 99 patients was slow (0.4 mm/y; 95% confidence interval, 0.15 to 0.59). Seventy percent of the tumors was stable and a subgroup of 30% of the tumors was growing (1.6 mm/y; 95% confidence interval, 1.1 to 2.0). No differences in clinical characteristics were identified between growing and stable tumors. Within the subgroup of growing tumors, germline missense mutations were significantly associated with accelerated growth compared with nonsense and frameshift mutations. Conclusion: The majority of small NF-pNETs are stable at long-term follow-up, irrespective of the underlying MEN1 genotype. A subgroup of tumors is slowly growing but cannot be identified on clinical grounds. In this subgroup, tumors with missense mutations exhibited faster growth. Additional events appear necessary for pNETs to progress. Future studies should be aimed at identifying these molecular driving events, which could be used as potential biomarkers.

Published
2017

6. Long-Term Natural Course of Small Nonfunctional Pancreatic Neuroendocrine Tumors in MEN1-Results From the Dutch MEN1 Study Group

Author

Pieterman, C.R.C., Laat, J.M. de, Twisk, J.W.R., Leeuwaarde, R.S. van, Herder, W.W. de, Dreijerink, K.M.A., Hermus, A.R., Dekkers, O.M., Horst-Schrivers, A.N.A. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H.M. Borel, Vriens, M.R., Valk, G.D., Pieterman, C.R.C., Laat, J.M. de, Twisk, J.W.R., Leeuwaarde, R.S. van, Herder, W.W. de, Dreijerink, K.M.A., Hermus, A.R., Dekkers, O.M., Horst-Schrivers, A.N.A. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H.M. Borel, Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, Background: Pancreatic neuroendocrine tumors (pNETs) are highly prevalent in patients with multiple endocrine neoplasia type 1 (MEN1), and metastatic disease is an important cause of MEN1-related mortality. Especially small nonfunctional (NF) pNETs pose a challenge to the treating physician and more information is needed regarding their natural course. We assessed long-term natural history of small NF-pNETs and its modifiers in the Dutch MEN1 population. Patients and Methods: Retrospective longitudinal observational cohort study of patients with small (<2 cm) NF-pNETs from the Dutch national MEN1 database, which includes >90% of the Dutch MEN1 population. Modifiers of long-term natural course were analyzed using linear mixed-models analysis. Results: Growth rate of the 115 included small NF-pNETs from 99 patients was slow (0.4 mm/y; 95% confidence interval, 0.15 to 0.59). Seventy percent of the tumors was stable and a subgroup of 30% of the tumors was growing (1.6 mm/y; 95% confidence interval, 1.1 to 2.0). No differences in clinical characteristics were identified between growing and stable tumors. Within the subgroup of growing tumors, germline missense mutations were significantly associated with accelerated growth compared with nonsense and frameshift mutations. Conclusion: The majority of small NF-pNETs are stable at long-term follow-up, irrespective of the underlying MEN1 genotype. A subgroup of tumors is slowly growing but cannot be identified on clinical grounds. In this subgroup, tumors with missense mutations exhibited faster growth. Additional events appear necessary for pNETs to progress. Future studies should be aimed at identifying these molecular driving events, which could be used as potential biomarkers.

Published
2017

7. Long-Term Natural Course of Small Nonfunctional Pancreatic Neuroendocrine Tumors in MEN1-Results From the Dutch MEN1 Study Group

Author

Pieterman, C.R.C., Laat, J.M. de, Twisk, J.W.R., Leeuwaarde, R.S. van, Herder, W.W. de, Dreijerink, K.M.A., Hermus, A.R., Dekkers, O.M., Horst-Schrivers, A.N.A. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H.M. Borel, Vriens, M.R., Valk, G.D., Pieterman, C.R.C., Laat, J.M. de, Twisk, J.W.R., Leeuwaarde, R.S. van, Herder, W.W. de, Dreijerink, K.M.A., Hermus, A.R., Dekkers, O.M., Horst-Schrivers, A.N.A. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H.M. Borel, Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, Background: Pancreatic neuroendocrine tumors (pNETs) are highly prevalent in patients with multiple endocrine neoplasia type 1 (MEN1), and metastatic disease is an important cause of MEN1-related mortality. Especially small nonfunctional (NF) pNETs pose a challenge to the treating physician and more information is needed regarding their natural course. We assessed long-term natural history of small NF-pNETs and its modifiers in the Dutch MEN1 population. Patients and Methods: Retrospective longitudinal observational cohort study of patients with small (<2 cm) NF-pNETs from the Dutch national MEN1 database, which includes >90% of the Dutch MEN1 population. Modifiers of long-term natural course were analyzed using linear mixed-models analysis. Results: Growth rate of the 115 included small NF-pNETs from 99 patients was slow (0.4 mm/y; 95% confidence interval, 0.15 to 0.59). Seventy percent of the tumors was stable and a subgroup of 30% of the tumors was growing (1.6 mm/y; 95% confidence interval, 1.1 to 2.0). No differences in clinical characteristics were identified between growing and stable tumors. Within the subgroup of growing tumors, germline missense mutations were significantly associated with accelerated growth compared with nonsense and frameshift mutations. Conclusion: The majority of small NF-pNETs are stable at long-term follow-up, irrespective of the underlying MEN1 genotype. A subgroup of tumors is slowly growing but cannot be identified on clinical grounds. In this subgroup, tumors with missense mutations exhibited faster growth. Additional events appear necessary for pNETs to progress. Future studies should be aimed at identifying these molecular driving events, which could be used as potential biomarkers.

Published
2017

8. Impact of Delay in Diagnosis in Outcomes in MEN1: Results From the Dutch MEN1 Study Group

Author

Leeuwaarde, R.S. van, Nesselrooij, B.P. van, Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Laat, J.M. de, Pieterman, C.R., Valk, G.D., Leeuwaarde, R.S. van, Nesselrooij, B.P. van, Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Laat, J.M. de, Pieterman, C.R., and Valk, G.D.

Abstract

Item does not contain fulltext, OBJECTIVE: Identifying a germline mutation in the multiple endocrine neoplasia type 1 (MEN1) gene in an index case has consequences for a whole family. Eligible family members should be offered genetic counseling and MEN1 mutation testing. Subsequently, clinical screening of mutation carriers according to the guidelines should be initiated. We assessed whether there is a lag time from MEN1 diagnosis of the index case to MEN1 diagnosis of family members. In addition, we determined whether this lag time was associated with an increased morbidity and mortality risk. DESIGN: A cohort study was performed using the Dutch MEN1 database, including >90% of the Dutch MEN1 population >16 years of age (n = 393). RESULTS: Fifty-eight MEN1 families were identified, of whom 57 were index cases and 247 were non-index cases (n = 304). The median lag time in MEN1 diagnosis of family members was 3.5 (range, 0-30) years. At the time of MEN1 diagnosis, 30 (12.1%) non-index cases had a duodenopancreatic neuroendocrine tumor, of whom 20% had metastases with a mean lag time of 10.9 years, in comparison with 7.1 years without metastases. Twenty-five (10.1%) non-index cases had a pituitary tumor, of whom 80% had a microadenoma and 20% had a macroadenoma, with mean lag times of 7.2 and 10.6 years, respectively. Ninety-five (38.4%) non-index cases had a primary hyperparathyroidism with a mean lag time of 9.5 years in comparison with seven patients without a primary hyperparathyroidism with a mean lag time of 3 years (P = .005). Ten non-index cases died because of a MEN1-related cause that developed during or before the lag time. CONCLUSION: There is a clinically relevant delay in MEN1 diagnosis in families because of a lag time between the diagnosis of an index case and the rest of the family. More emphasis should be placed on the conduct of proper counseling and genetic testing in all eligible family members.

Published
2016

9. MEN1 redefined, a clinical comparison of mutation-positive and mutation-negative patients

Author

Laat, J.M. de, Luijt, R.B. van der, Pieterman, C.R., Oostveen, M.P., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Valk, G.D., Laat, J.M. de, Luijt, R.B. van der, Pieterman, C.R., Oostveen, M.P., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., and Valk, G.D.

Abstract

Contains fulltext : 170909.pdf (publisher's version ) (Open Access), BACKGROUND: Multiple Endocrine Neoplasia type 1 (MEN1) is diagnosed when two out of the three primary MEN1-associated endocrine tumors occur in a patient. Up to 10-30 % of those patients have no mutation in the MEN1 gene. It is unclear if the phenotype and course of the disease of mutation-negative patients is comparable with mutation-positive patients and if these patients have true MEN1. The present study aims to describe and compare the clinical course of MEN1 mutation-negative patients with two out of the three main MEN1 manifestations and mutation-positive patients during long-term follow-up. METHODS: This is a cohort study performed using the Dutch MEN1 database, including > 90 % of the Dutch MEN1 population. RESULTS: A total of 293 (90.7 %) mutation-positive and 30 (9.3 %) mutation-negative MEN1 patients were included. Median age of developing the first main MEN1 manifestation was higher in mutation-negative patients (46 vs. 33 years) (P = 0.007). Mutation-negative patients did not develop a third main MEN1 manifestation in the course of follow-up compared to 48.3 % of mutation-positive patients (P < 0.001). Median survival in mutation-positive patients was estimated at 73.0 years (95 % CI, 69.5-76.5) compared to 87.0 years (95 % CI not available) in mutation-negative patients (P = 0.001). CONCLUSIONS: Mutation-positive and mutation-negative MEN1 patients have a different phenotype and clinical course. Mutation-negative patients develop MEN1 manifestations at higher age and have a life expectancy comparable with the general population. The apparent differences in clinical course suggest that MEN1 mutation-negative patients do not have true MEN1, but another MEN1-like syndrome or sporadic co-incidence of two neuro-endocrine tumors.

Published
2016

10. Impact of Delay in Diagnosis in Outcomes in MEN1: Results From the Dutch MEN1 Study Group

Author

Leeuwaarde, R.S. van, Nesselrooij, B.P. van, Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Laat, J.M. de, Pieterman, C.R., Valk, G.D., Leeuwaarde, R.S. van, Nesselrooij, B.P. van, Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Laat, J.M. de, Pieterman, C.R., and Valk, G.D.

Abstract

Item does not contain fulltext, OBJECTIVE: Identifying a germline mutation in the multiple endocrine neoplasia type 1 (MEN1) gene in an index case has consequences for a whole family. Eligible family members should be offered genetic counseling and MEN1 mutation testing. Subsequently, clinical screening of mutation carriers according to the guidelines should be initiated. We assessed whether there is a lag time from MEN1 diagnosis of the index case to MEN1 diagnosis of family members. In addition, we determined whether this lag time was associated with an increased morbidity and mortality risk. DESIGN: A cohort study was performed using the Dutch MEN1 database, including >90% of the Dutch MEN1 population >16 years of age (n = 393). RESULTS: Fifty-eight MEN1 families were identified, of whom 57 were index cases and 247 were non-index cases (n = 304). The median lag time in MEN1 diagnosis of family members was 3.5 (range, 0-30) years. At the time of MEN1 diagnosis, 30 (12.1%) non-index cases had a duodenopancreatic neuroendocrine tumor, of whom 20% had metastases with a mean lag time of 10.9 years, in comparison with 7.1 years without metastases. Twenty-five (10.1%) non-index cases had a pituitary tumor, of whom 80% had a microadenoma and 20% had a macroadenoma, with mean lag times of 7.2 and 10.6 years, respectively. Ninety-five (38.4%) non-index cases had a primary hyperparathyroidism with a mean lag time of 9.5 years in comparison with seven patients without a primary hyperparathyroidism with a mean lag time of 3 years (P = .005). Ten non-index cases died because of a MEN1-related cause that developed during or before the lag time. CONCLUSION: There is a clinically relevant delay in MEN1 diagnosis in families because of a lag time between the diagnosis of an index case and the rest of the family. More emphasis should be placed on the conduct of proper counseling and genetic testing in all eligible family members.

Published
2016

11. MEN1 redefined, a clinical comparison of mutation-positive and mutation-negative patients

Author

Laat, J.M. de, Luijt, R.B. van der, Pieterman, C.R., Oostveen, M.P., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Valk, G.D., Laat, J.M. de, Luijt, R.B. van der, Pieterman, C.R., Oostveen, M.P., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., and Valk, G.D.

Abstract

Contains fulltext : 170909.pdf (publisher's version ) (Open Access), BACKGROUND: Multiple Endocrine Neoplasia type 1 (MEN1) is diagnosed when two out of the three primary MEN1-associated endocrine tumors occur in a patient. Up to 10-30 % of those patients have no mutation in the MEN1 gene. It is unclear if the phenotype and course of the disease of mutation-negative patients is comparable with mutation-positive patients and if these patients have true MEN1. The present study aims to describe and compare the clinical course of MEN1 mutation-negative patients with two out of the three main MEN1 manifestations and mutation-positive patients during long-term follow-up. METHODS: This is a cohort study performed using the Dutch MEN1 database, including > 90 % of the Dutch MEN1 population. RESULTS: A total of 293 (90.7 %) mutation-positive and 30 (9.3 %) mutation-negative MEN1 patients were included. Median age of developing the first main MEN1 manifestation was higher in mutation-negative patients (46 vs. 33 years) (P = 0.007). Mutation-negative patients did not develop a third main MEN1 manifestation in the course of follow-up compared to 48.3 % of mutation-positive patients (P < 0.001). Median survival in mutation-positive patients was estimated at 73.0 years (95 % CI, 69.5-76.5) compared to 87.0 years (95 % CI not available) in mutation-negative patients (P = 0.001). CONCLUSIONS: Mutation-positive and mutation-negative MEN1 patients have a different phenotype and clinical course. Mutation-negative patients develop MEN1 manifestations at higher age and have a life expectancy comparable with the general population. The apparent differences in clinical course suggest that MEN1 mutation-negative patients do not have true MEN1, but another MEN1-like syndrome or sporadic co-incidence of two neuro-endocrine tumors.

Published
2016

12. Impact of Delay in Diagnosis in Outcomes in MEN1: Results From the Dutch MEN1 Study Group

Author

Leeuwaarde, R.S. van, Nesselrooij, B.P. van, Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Laat, J.M. de, Pieterman, C.R., Valk, G.D., Leeuwaarde, R.S. van, Nesselrooij, B.P. van, Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Laat, J.M. de, Pieterman, C.R., and Valk, G.D.

Abstract

Item does not contain fulltext, OBJECTIVE: Identifying a germline mutation in the multiple endocrine neoplasia type 1 (MEN1) gene in an index case has consequences for a whole family. Eligible family members should be offered genetic counseling and MEN1 mutation testing. Subsequently, clinical screening of mutation carriers according to the guidelines should be initiated. We assessed whether there is a lag time from MEN1 diagnosis of the index case to MEN1 diagnosis of family members. In addition, we determined whether this lag time was associated with an increased morbidity and mortality risk. DESIGN: A cohort study was performed using the Dutch MEN1 database, including >90% of the Dutch MEN1 population >16 years of age (n = 393). RESULTS: Fifty-eight MEN1 families were identified, of whom 57 were index cases and 247 were non-index cases (n = 304). The median lag time in MEN1 diagnosis of family members was 3.5 (range, 0-30) years. At the time of MEN1 diagnosis, 30 (12.1%) non-index cases had a duodenopancreatic neuroendocrine tumor, of whom 20% had metastases with a mean lag time of 10.9 years, in comparison with 7.1 years without metastases. Twenty-five (10.1%) non-index cases had a pituitary tumor, of whom 80% had a microadenoma and 20% had a macroadenoma, with mean lag times of 7.2 and 10.6 years, respectively. Ninety-five (38.4%) non-index cases had a primary hyperparathyroidism with a mean lag time of 9.5 years in comparison with seven patients without a primary hyperparathyroidism with a mean lag time of 3 years (P = .005). Ten non-index cases died because of a MEN1-related cause that developed during or before the lag time. CONCLUSION: There is a clinically relevant delay in MEN1 diagnosis in families because of a lag time between the diagnosis of an index case and the rest of the family. More emphasis should be placed on the conduct of proper counseling and genetic testing in all eligible family members.

Published
2016

14. Long-Term Natural Course of Pituitary Tumors in Patients With MEN1: Results From the DutchMEN1 Study Group (DMSG)

Author

Laat, J.M. de, Dekkers, O.M., Pieterman, C.R., Kluijfhout, W.P., Hermus, A.R.M.M., Pereira, A.M., Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Herder, W.W. de, Valk, G.D., Laat, J.M. de, Dekkers, O.M., Pieterman, C.R., Kluijfhout, W.P., Hermus, A.R.M.M., Pereira, A.M., Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Herder, W.W. de, and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: Guidelines advise lifelong radiological followup for asymptomatic pituitary adenomas (PITs) because of the risk for growth and subsequent visual field defects. In the context of multiple endocrine neoplasia type 1 (MEN1) an even more comprehensive screening is advised because PITs are presumed to manifest more aggressive behavior. We studied the long-term course of MEN1-related PITs, which may be used as a model for sporadically occurring PITs. OBJECTIVE: The aim of our study is to assess the results of systematic pre-symptomatic PIT screening and subsequent long-term followup of PITs with emphasis on nonfunctioning microadenomas diagnosed by screening. PATIENTS AND METHODS: A cohort study was performed using the Dutch national MEN1 database, including greater than 90% of the Dutch MEN1 population older than 16 years (n = 323). MAIN OUTCOME MEASURES: Screening results, natural course, and effects of treatment of PIT were assessed. RESULTS: PIT was diagnosed in 123 patients with MEN1 (38.1 %), of whom 66 were diagnosed by MEN1-related screening. Ninety-one percent of the nonfunctioning PIT detected during screening (n = 35), did not require intervention during followup (median, 6.0 y). Three microadenomas showed limited growth but did not progress toward macroadenomas. Both screening-detected and prevalent prolactinomas (n = 52) responded well to treatment with dopamine agonists. CONCLUSION: Systematic presymptomatic screening for PIT in patients with MEN1 predominantly results in detection of nonfunctioning microadenomas. Prolactinoma in patients with MEN1 responded well to medical treatment. Microadenomas grew only occasionally and after many years without clinical consequences. Frequent magnetic resonance imaging followup of nonfunctioning microadenomas in the context of MEN1 and sporadically occurring PITs therefore seems debatable.

Published
2015

15. No Association of Blood Type O With Neuroendocrine Tumors in Multiple Endocrine Neoplasia Type 1

Author

Nell, S., Leeuwaarde, R.S. van, Pieterman, C.R., Laat, J.M. de, Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., Valk, G.D., Nell, S., Leeuwaarde, R.S. van, Pieterman, C.R., Laat, J.M. de, Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: An association between ABO blood type and the development of cancer, in particular, pancreatic cancer, has been reported in the literature. An association between blood type O and neuroendocrine tumors in multiple endocrine neoplasia type 1 (MEN1) patients was recently suggested. Therefore, blood type O was proposed as an additional factor to personalize screening criteria for neuroendocrine tumors in MEN1 patients. OBJECTIVE: The aim of this study was to assess the association between blood type O and the occurrence of neuroendocrine tumors in the national Dutch MEN1 cohort. DESIGN: This is a cohort study using the Dutch National MEN1 database, which includes more than 90% of the Dutch MEN1 population. Demographic and clinical data were analyzed by blood type. Chi-square tests and Fisher exact tests were used to determine the association between blood type O and occurrence of neuroendocrine tumors. A cumulative incidence analysis (Gray's test) was performed to assess the equality of cumulative incidence of neuroendocrine tumors in blood type groups, taking death into account as a competing risk. RESULTS: The ABO blood type of 200 of 322 MEN1 patients was known. Demographic and clinical characteristics were similar among blood type O and non-O type cohorts. The occurrence of neuroendocrine tumors of the lung, thymus, pancreas, and gastrointestinal tract was equally distributed across the blood type O and non-O type cohorts (Grays's test for equality; P = 0.72). Furthermore, we found no association between blood type O and the occurrence of metastatic disease or survival. CONCLUSIONS: An association between blood type O and the occurrence of neuroendocrine tumors in MEN1 patients was not confirmed. For this reason, the addition of the blood type to screening and surveillance practice seems not to be of additional value for identifying MEN1 patients at risk for the development of neuroendocrine tumors, metastatic disease, or a shortened survival.

Published
2015

16. Thyroid incidentalomas in patients with multiple endocrine neoplasia type 1

Author

Lodewijk, L., Bongers, P.J., Kist, J.W., Conemans, E.B., Laat, J.M. de, Pieterman, C.R., Horst-Schrivers, A.N. van der, Jorna, C., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., Valk, G.D., Lodewijk, L., Bongers, P.J., Kist, J.W., Conemans, E.B., Laat, J.M. de, Pieterman, C.R., Horst-Schrivers, A.N. van der, Jorna, C., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, OBJECTIVE: Currently, little is known about the prevalence of thyroid tumors in multiple endocrine neoplasia type 1 (MEN1) patients and it is unclear whether tumorigenesis of these thyroid tumors is MEN1-related. The aim of the study was to assess the prevalence of thyroid incidentalomas in MEN1 patients compared with nonMEN1 patients and to verify whether thyroid tumorigenesis is MEN1-related. DESIGN: A cross-sectional study. METHODS: The study included two groups: patients with MEN1 and a matched non-MEN1 control group without known thyroid disease, who underwent an ultrasound of the neck for the localization of parathyroid adenoma. Ninety-five MEN1 patients underwent ultrasound of the neck and were matched on gender and age with non-MEN1 patients. The prevalence of thyroid incidentalomas described in the ultrasound report was scored. Multinodular goiters, solitary nodes, and cysts were scored as incidentalomas. Presence of nuclear menin expression was evaluated by menin immunostaining of the thyroid tumors. RESULTS: In the MEN1 group, 43 (45%) patients had a thyroid incidentaloma compared with 48 (51%) in the non-MEN1 group, of which 14 (15%) and 16 (17%), respectively, were solitary nodes. Menin was expressed in the nuclei of all evaluated thyroid tumors. CONCLUSIONS: MEN1 patients do not have a higher prevalence of thyroid incidentalomas compared with primary hyperparathyroidism patients without the diagnosis of MEN1. Menin was expressed in the thyroid tumors of MEN1 patients.

Published
2015

19. Long-Term Natural Course of Pituitary Tumors in Patients With MEN1: Results From the DutchMEN1 Study Group (DMSG)

Author

Laat, J.M. de, Dekkers, O.M., Pieterman, C.R., Kluijfhout, W.P., Hermus, A.R.M.M., Pereira, A.M., Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Herder, W.W. de, Valk, G.D., Laat, J.M. de, Dekkers, O.M., Pieterman, C.R., Kluijfhout, W.P., Hermus, A.R.M.M., Pereira, A.M., Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Herder, W.W. de, and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: Guidelines advise lifelong radiological followup for asymptomatic pituitary adenomas (PITs) because of the risk for growth and subsequent visual field defects. In the context of multiple endocrine neoplasia type 1 (MEN1) an even more comprehensive screening is advised because PITs are presumed to manifest more aggressive behavior. We studied the long-term course of MEN1-related PITs, which may be used as a model for sporadically occurring PITs. OBJECTIVE: The aim of our study is to assess the results of systematic pre-symptomatic PIT screening and subsequent long-term followup of PITs with emphasis on nonfunctioning microadenomas diagnosed by screening. PATIENTS AND METHODS: A cohort study was performed using the Dutch national MEN1 database, including greater than 90% of the Dutch MEN1 population older than 16 years (n = 323). MAIN OUTCOME MEASURES: Screening results, natural course, and effects of treatment of PIT were assessed. RESULTS: PIT was diagnosed in 123 patients with MEN1 (38.1 %), of whom 66 were diagnosed by MEN1-related screening. Ninety-one percent of the nonfunctioning PIT detected during screening (n = 35), did not require intervention during followup (median, 6.0 y). Three microadenomas showed limited growth but did not progress toward macroadenomas. Both screening-detected and prevalent prolactinomas (n = 52) responded well to treatment with dopamine agonists. CONCLUSION: Systematic presymptomatic screening for PIT in patients with MEN1 predominantly results in detection of nonfunctioning microadenomas. Prolactinoma in patients with MEN1 responded well to medical treatment. Microadenomas grew only occasionally and after many years without clinical consequences. Frequent magnetic resonance imaging followup of nonfunctioning microadenomas in the context of MEN1 and sporadically occurring PITs therefore seems debatable.

Published
2015

20. No Association of Blood Type O With Neuroendocrine Tumors in Multiple Endocrine Neoplasia Type 1

Author

Nell, S., Leeuwaarde, R.S. van, Pieterman, C.R., Laat, J.M. de, Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., Valk, G.D., Nell, S., Leeuwaarde, R.S. van, Pieterman, C.R., Laat, J.M. de, Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: An association between ABO blood type and the development of cancer, in particular, pancreatic cancer, has been reported in the literature. An association between blood type O and neuroendocrine tumors in multiple endocrine neoplasia type 1 (MEN1) patients was recently suggested. Therefore, blood type O was proposed as an additional factor to personalize screening criteria for neuroendocrine tumors in MEN1 patients. OBJECTIVE: The aim of this study was to assess the association between blood type O and the occurrence of neuroendocrine tumors in the national Dutch MEN1 cohort. DESIGN: This is a cohort study using the Dutch National MEN1 database, which includes more than 90% of the Dutch MEN1 population. Demographic and clinical data were analyzed by blood type. Chi-square tests and Fisher exact tests were used to determine the association between blood type O and occurrence of neuroendocrine tumors. A cumulative incidence analysis (Gray's test) was performed to assess the equality of cumulative incidence of neuroendocrine tumors in blood type groups, taking death into account as a competing risk. RESULTS: The ABO blood type of 200 of 322 MEN1 patients was known. Demographic and clinical characteristics were similar among blood type O and non-O type cohorts. The occurrence of neuroendocrine tumors of the lung, thymus, pancreas, and gastrointestinal tract was equally distributed across the blood type O and non-O type cohorts (Grays's test for equality; P = 0.72). Furthermore, we found no association between blood type O and the occurrence of metastatic disease or survival. CONCLUSIONS: An association between blood type O and the occurrence of neuroendocrine tumors in MEN1 patients was not confirmed. For this reason, the addition of the blood type to screening and surveillance practice seems not to be of additional value for identifying MEN1 patients at risk for the development of neuroendocrine tumors, metastatic disease, or a shortened survival.

Published
2015

21. Thyroid incidentalomas in patients with multiple endocrine neoplasia type 1

Author

Lodewijk, L., Bongers, P.J., Kist, J.W., Conemans, E.B., Laat, J.M. de, Pieterman, C.R., Horst-Schrivers, A.N. van der, Jorna, C., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., Valk, G.D., Lodewijk, L., Bongers, P.J., Kist, J.W., Conemans, E.B., Laat, J.M. de, Pieterman, C.R., Horst-Schrivers, A.N. van der, Jorna, C., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, OBJECTIVE: Currently, little is known about the prevalence of thyroid tumors in multiple endocrine neoplasia type 1 (MEN1) patients and it is unclear whether tumorigenesis of these thyroid tumors is MEN1-related. The aim of the study was to assess the prevalence of thyroid incidentalomas in MEN1 patients compared with nonMEN1 patients and to verify whether thyroid tumorigenesis is MEN1-related. DESIGN: A cross-sectional study. METHODS: The study included two groups: patients with MEN1 and a matched non-MEN1 control group without known thyroid disease, who underwent an ultrasound of the neck for the localization of parathyroid adenoma. Ninety-five MEN1 patients underwent ultrasound of the neck and were matched on gender and age with non-MEN1 patients. The prevalence of thyroid incidentalomas described in the ultrasound report was scored. Multinodular goiters, solitary nodes, and cysts were scored as incidentalomas. Presence of nuclear menin expression was evaluated by menin immunostaining of the thyroid tumors. RESULTS: In the MEN1 group, 43 (45%) patients had a thyroid incidentaloma compared with 48 (51%) in the non-MEN1 group, of which 14 (15%) and 16 (17%), respectively, were solitary nodes. Menin was expressed in the nuclei of all evaluated thyroid tumors. CONCLUSIONS: MEN1 patients do not have a higher prevalence of thyroid incidentalomas compared with primary hyperparathyroidism patients without the diagnosis of MEN1. Menin was expressed in the thyroid tumors of MEN1 patients.

Published
2015

23. Thyroid incidentalomas in patients with multiple endocrine neoplasia type 1

Author

Lodewijk, L., Bongers, P.J., Kist, J.W., Conemans, E.B., Laat, J.M. de, Pieterman, C.R., Horst-Schrivers, A.N. van der, Jorna, C., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., Valk, G.D., Lodewijk, L., Bongers, P.J., Kist, J.W., Conemans, E.B., Laat, J.M. de, Pieterman, C.R., Horst-Schrivers, A.N. van der, Jorna, C., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, OBJECTIVE: Currently, little is known about the prevalence of thyroid tumors in multiple endocrine neoplasia type 1 (MEN1) patients and it is unclear whether tumorigenesis of these thyroid tumors is MEN1-related. The aim of the study was to assess the prevalence of thyroid incidentalomas in MEN1 patients compared with nonMEN1 patients and to verify whether thyroid tumorigenesis is MEN1-related. DESIGN: A cross-sectional study. METHODS: The study included two groups: patients with MEN1 and a matched non-MEN1 control group without known thyroid disease, who underwent an ultrasound of the neck for the localization of parathyroid adenoma. Ninety-five MEN1 patients underwent ultrasound of the neck and were matched on gender and age with non-MEN1 patients. The prevalence of thyroid incidentalomas described in the ultrasound report was scored. Multinodular goiters, solitary nodes, and cysts were scored as incidentalomas. Presence of nuclear menin expression was evaluated by menin immunostaining of the thyroid tumors. RESULTS: In the MEN1 group, 43 (45%) patients had a thyroid incidentaloma compared with 48 (51%) in the non-MEN1 group, of which 14 (15%) and 16 (17%), respectively, were solitary nodes. Menin was expressed in the nuclei of all evaluated thyroid tumors. CONCLUSIONS: MEN1 patients do not have a higher prevalence of thyroid incidentalomas compared with primary hyperparathyroidism patients without the diagnosis of MEN1. Menin was expressed in the thyroid tumors of MEN1 patients.

Published
2015

24. Long-Term Natural Course of Pituitary Tumors in Patients With MEN1: Results From the DutchMEN1 Study Group (DMSG)

Author

Laat, J.M. de, Dekkers, O.M., Pieterman, C.R., Kluijfhout, W.P., Hermus, A.R.M.M., Pereira, A.M., Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Herder, W.W. de, Valk, G.D., Laat, J.M. de, Dekkers, O.M., Pieterman, C.R., Kluijfhout, W.P., Hermus, A.R.M.M., Pereira, A.M., Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Herder, W.W. de, and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: Guidelines advise lifelong radiological followup for asymptomatic pituitary adenomas (PITs) because of the risk for growth and subsequent visual field defects. In the context of multiple endocrine neoplasia type 1 (MEN1) an even more comprehensive screening is advised because PITs are presumed to manifest more aggressive behavior. We studied the long-term course of MEN1-related PITs, which may be used as a model for sporadically occurring PITs. OBJECTIVE: The aim of our study is to assess the results of systematic pre-symptomatic PIT screening and subsequent long-term followup of PITs with emphasis on nonfunctioning microadenomas diagnosed by screening. PATIENTS AND METHODS: A cohort study was performed using the Dutch national MEN1 database, including greater than 90% of the Dutch MEN1 population older than 16 years (n = 323). MAIN OUTCOME MEASURES: Screening results, natural course, and effects of treatment of PIT were assessed. RESULTS: PIT was diagnosed in 123 patients with MEN1 (38.1 %), of whom 66 were diagnosed by MEN1-related screening. Ninety-one percent of the nonfunctioning PIT detected during screening (n = 35), did not require intervention during followup (median, 6.0 y). Three microadenomas showed limited growth but did not progress toward macroadenomas. Both screening-detected and prevalent prolactinomas (n = 52) responded well to treatment with dopamine agonists. CONCLUSION: Systematic presymptomatic screening for PIT in patients with MEN1 predominantly results in detection of nonfunctioning microadenomas. Prolactinoma in patients with MEN1 responded well to medical treatment. Microadenomas grew only occasionally and after many years without clinical consequences. Frequent magnetic resonance imaging followup of nonfunctioning microadenomas in the context of MEN1 and sporadically occurring PITs therefore seems debatable.

Published
2015

25. No Association of Blood Type O With Neuroendocrine Tumors in Multiple Endocrine Neoplasia Type 1

Author

Nell, S., Leeuwaarde, R.S. van, Pieterman, C.R., Laat, J.M. de, Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., Valk, G.D., Nell, S., Leeuwaarde, R.S. van, Pieterman, C.R., Laat, J.M. de, Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Rinkes, I.H., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: An association between ABO blood type and the development of cancer, in particular, pancreatic cancer, has been reported in the literature. An association between blood type O and neuroendocrine tumors in multiple endocrine neoplasia type 1 (MEN1) patients was recently suggested. Therefore, blood type O was proposed as an additional factor to personalize screening criteria for neuroendocrine tumors in MEN1 patients. OBJECTIVE: The aim of this study was to assess the association between blood type O and the occurrence of neuroendocrine tumors in the national Dutch MEN1 cohort. DESIGN: This is a cohort study using the Dutch National MEN1 database, which includes more than 90% of the Dutch MEN1 population. Demographic and clinical data were analyzed by blood type. Chi-square tests and Fisher exact tests were used to determine the association between blood type O and occurrence of neuroendocrine tumors. A cumulative incidence analysis (Gray's test) was performed to assess the equality of cumulative incidence of neuroendocrine tumors in blood type groups, taking death into account as a competing risk. RESULTS: The ABO blood type of 200 of 322 MEN1 patients was known. Demographic and clinical characteristics were similar among blood type O and non-O type cohorts. The occurrence of neuroendocrine tumors of the lung, thymus, pancreas, and gastrointestinal tract was equally distributed across the blood type O and non-O type cohorts (Grays's test for equality; P = 0.72). Furthermore, we found no association between blood type O and the occurrence of metastatic disease or survival. CONCLUSIONS: An association between blood type O and the occurrence of neuroendocrine tumors in MEN1 patients was not confirmed. For this reason, the addition of the blood type to screening and surveillance practice seems not to be of additional value for identifying MEN1 patients at risk for the development of neuroendocrine tumors, metastatic disease, or a shortened survival.

Published
2015

28. Natural Course and Survival of Neuroendocrine Tumors of Thymus and Lung in MEN1 Patients

Author

Laat, J.M. de, Pieterman, C.R., Broek, M. van den, Twisk, J.W.R., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Valk, G.D., Laat, J.M. de, Pieterman, C.R., Broek, M. van den, Twisk, J.W.R., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: The natural course and survival of neuroendocrine tumors (NETs) of thymus (Th) and lung in multiple endocrine neoplasia type 1 (MEN1) patients are still unknown. OBJECTIVE: Our objective was to assess prevalence, tumor growth, and survival of Th and lung NETs in an unselected MEN1 population with long-term follow-up. DESIGN: This was an observational study. PATIENTS AND METHODS: A longitudinal study was performed using the Dutch national MEN1 database, including >90% of the Dutch MEN1 population >16 years of age. Patients under care of the Dutch University Medical Centers (1990-2011) (n = 323) were included. MAIN OUTCOME MEASURES: The prevalence and survival of Th and lung NETs were assessed. Linear mixed-models analysis was applied to assess tumor growth with age as a possible confounder and gender, genotype and baseline tumor size as possible effect modifiers. RESULTS: Th NETs occurred in 3.4% of patients, almost exclusively in males with a 10-year survival of 25% (95% confidence interval = 8%-80%). A thoracic computed tomography scan was available in 188 patients (58.2%). A lung NET was identified in 42 patients (13.0%) with a 10-year survival of 71.1% (95% confidence interval = 51%-100%). Tumor volume of lung NETs increased 17% per year (P < .001) (tumor doubling time 4.5 years). Tumor doubling time in males was 2.5 vs 5.5 years in females (P = .05). Lung NET growth was not associated with genotype or with baseline tumor size (<1 vs >/=1 cm). CONCLUSION: In MEN1 patients, Th NETs almost exclusively occurred in males and had a very low prevalence and a high mortality. Lung NETs occurred more often than previously thought, had an indolent course, and occurred equally in both sexes. Tumor growth in males was double compared with female patients.

Published
2014

29. Natural Course and Survival of Neuroendocrine Tumors of Thymus and Lung in MEN1 Patients

Author

Laat, J.M. de, Pieterman, C.R., Broek, M. van den, Twisk, J.W.R., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Valk, G.D., Laat, J.M. de, Pieterman, C.R., Broek, M. van den, Twisk, J.W.R., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: The natural course and survival of neuroendocrine tumors (NETs) of thymus (Th) and lung in multiple endocrine neoplasia type 1 (MEN1) patients are still unknown. OBJECTIVE: Our objective was to assess prevalence, tumor growth, and survival of Th and lung NETs in an unselected MEN1 population with long-term follow-up. DESIGN: This was an observational study. PATIENTS AND METHODS: A longitudinal study was performed using the Dutch national MEN1 database, including >90% of the Dutch MEN1 population >16 years of age. Patients under care of the Dutch University Medical Centers (1990-2011) (n = 323) were included. MAIN OUTCOME MEASURES: The prevalence and survival of Th and lung NETs were assessed. Linear mixed-models analysis was applied to assess tumor growth with age as a possible confounder and gender, genotype and baseline tumor size as possible effect modifiers. RESULTS: Th NETs occurred in 3.4% of patients, almost exclusively in males with a 10-year survival of 25% (95% confidence interval = 8%-80%). A thoracic computed tomography scan was available in 188 patients (58.2%). A lung NET was identified in 42 patients (13.0%) with a 10-year survival of 71.1% (95% confidence interval = 51%-100%). Tumor volume of lung NETs increased 17% per year (P < .001) (tumor doubling time 4.5 years). Tumor doubling time in males was 2.5 vs 5.5 years in females (P = .05). Lung NET growth was not associated with genotype or with baseline tumor size (<1 vs >/=1 cm). CONCLUSION: In MEN1 patients, Th NETs almost exclusively occurred in males and had a very low prevalence and a high mortality. Lung NETs occurred more often than previously thought, had an indolent course, and occurred equally in both sexes. Tumor growth in males was double compared with female patients.

Published
2014

30. Natural Course and Survival of Neuroendocrine Tumors of Thymus and Lung in MEN1 Patients

Author

Laat, J.M. de, Pieterman, C.R., Broek, M. van den, Twisk, J.W.R., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Valk, G.D., Laat, J.M. de, Pieterman, C.R., Broek, M. van den, Twisk, J.W.R., Hermus, A.R., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: The natural course and survival of neuroendocrine tumors (NETs) of thymus (Th) and lung in multiple endocrine neoplasia type 1 (MEN1) patients are still unknown. OBJECTIVE: Our objective was to assess prevalence, tumor growth, and survival of Th and lung NETs in an unselected MEN1 population with long-term follow-up. DESIGN: This was an observational study. PATIENTS AND METHODS: A longitudinal study was performed using the Dutch national MEN1 database, including >90% of the Dutch MEN1 population >16 years of age. Patients under care of the Dutch University Medical Centers (1990-2011) (n = 323) were included. MAIN OUTCOME MEASURES: The prevalence and survival of Th and lung NETs were assessed. Linear mixed-models analysis was applied to assess tumor growth with age as a possible confounder and gender, genotype and baseline tumor size as possible effect modifiers. RESULTS: Th NETs occurred in 3.4% of patients, almost exclusively in males with a 10-year survival of 25% (95% confidence interval = 8%-80%). A thoracic computed tomography scan was available in 188 patients (58.2%). A lung NET was identified in 42 patients (13.0%) with a 10-year survival of 71.1% (95% confidence interval = 51%-100%). Tumor volume of lung NETs increased 17% per year (P < .001) (tumor doubling time 4.5 years). Tumor doubling time in males was 2.5 vs 5.5 years in females (P = .05). Lung NET growth was not associated with genotype or with baseline tumor size (<1 vs >/=1 cm). CONCLUSION: In MEN1 patients, Th NETs almost exclusively occurred in males and had a very low prevalence and a high mortality. Lung NETs occurred more often than previously thought, had an indolent course, and occurred equally in both sexes. Tumor growth in males was double compared with female patients.

Published
2014

32. Low accuracy of tumor markers for diagnosing pancreatic neuroendocrine tumors in multiple endocrine neoplasia type 1 patients

Author

Laat, J.M. de, Pieterman, C.R., Weijmans, M., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Valk, G.D., Laat, J.M. de, Pieterman, C.R., Weijmans, M., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: The assessment of tumor markers for diagnosing pancreatic neuroendocrine tumors (pNET) in multiple endocrine neoplasia type 1 (MEN1) patients is advised in the current guidelines but has never been validated for this purpose. OBJECTIVE: The objective of the study was to assess the diagnostic accuracy of chromogranin A (CgA), pancreatic polypeptide (PP), and glucagon for pNET in MEN1. DESIGN: This was a diagnostic study. SETTING: The study was conducted at Dutch university medical centers from 2008 to 2011, representing 90% of the total Dutch MEN1 population. PATIENTS AND METHODS: Patients for whom data on tumor markers in combination with the reference standard (ie, radiological imaging) were available between 2008 and 2011 were included. The reference standard for the presence of pNET was pathology or detection on magnetic resonance imaging, computed tomography, or endoscopic ultrasound confirmed on subsequent imaging, irrespective of modality at follow-up. MAIN OUTCOME MEASURES: The area under the receiver-operating characteristic curve (AUC), positive predictive value, negative predictive value, positive likelihood ratio, negative likelihood ratio, sensitivity, and specificity were calculated for each marker. RESULTS: For the analysis of PP, CgA, and glucagon, 73, 81, and 94 patients were available, respectively. The AUC for CgA was 0.48 [95% confidence interval (CI) 0.35-0.61] with a sensitivity 0.33 and a specificity 0.73; the AUC for glucagon was 0.58 (95% CI 0.46-0.70) with a sensitivity 0.43 and a specificity 0.73; and the AUC for PP was 0.64 (95% CI 0.50-0.77) with a sensitivity 0.36 and a specificity 0.74. Age, imaging modality, tumor size, and number did not influence the outcomes. CONCLUSION: The diagnostic accuracy of the tumor markers CgA, PP, and glucagon for pNET in MEN1 is low.

Published
2013

33. Low accuracy of tumor markers for diagnosing pancreatic neuroendocrine tumors in multiple endocrine neoplasia type 1 patients

Author

Laat, J.M. de, Pieterman, C.R., Weijmans, M., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Valk, G.D., Laat, J.M. de, Pieterman, C.R., Weijmans, M., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: The assessment of tumor markers for diagnosing pancreatic neuroendocrine tumors (pNET) in multiple endocrine neoplasia type 1 (MEN1) patients is advised in the current guidelines but has never been validated for this purpose. OBJECTIVE: The objective of the study was to assess the diagnostic accuracy of chromogranin A (CgA), pancreatic polypeptide (PP), and glucagon for pNET in MEN1. DESIGN: This was a diagnostic study. SETTING: The study was conducted at Dutch university medical centers from 2008 to 2011, representing 90% of the total Dutch MEN1 population. PATIENTS AND METHODS: Patients for whom data on tumor markers in combination with the reference standard (ie, radiological imaging) were available between 2008 and 2011 were included. The reference standard for the presence of pNET was pathology or detection on magnetic resonance imaging, computed tomography, or endoscopic ultrasound confirmed on subsequent imaging, irrespective of modality at follow-up. MAIN OUTCOME MEASURES: The area under the receiver-operating characteristic curve (AUC), positive predictive value, negative predictive value, positive likelihood ratio, negative likelihood ratio, sensitivity, and specificity were calculated for each marker. RESULTS: For the analysis of PP, CgA, and glucagon, 73, 81, and 94 patients were available, respectively. The AUC for CgA was 0.48 [95% confidence interval (CI) 0.35-0.61] with a sensitivity 0.33 and a specificity 0.73; the AUC for glucagon was 0.58 (95% CI 0.46-0.70) with a sensitivity 0.43 and a specificity 0.73; and the AUC for PP was 0.64 (95% CI 0.50-0.77) with a sensitivity 0.36 and a specificity 0.74. Age, imaging modality, tumor size, and number did not influence the outcomes. CONCLUSION: The diagnostic accuracy of the tumor markers CgA, PP, and glucagon for pNET in MEN1 is low.

Published
2013

34. Low accuracy of tumor markers for diagnosing pancreatic neuroendocrine tumors in multiple endocrine neoplasia type 1 patients

Author

Laat, J.M. de, Pieterman, C.R., Weijmans, M., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., Valk, G.D., Laat, J.M. de, Pieterman, C.R., Weijmans, M., Hermus, A.R.M.M., Dekkers, O.M., Herder, W.W. de, Horst-Schrivers, A.N. van der, Drent, M.L., Bisschop, P.H., Havekes, B., Vriens, M.R., and Valk, G.D.

Abstract

Item does not contain fulltext, CONTEXT: The assessment of tumor markers for diagnosing pancreatic neuroendocrine tumors (pNET) in multiple endocrine neoplasia type 1 (MEN1) patients is advised in the current guidelines but has never been validated for this purpose. OBJECTIVE: The objective of the study was to assess the diagnostic accuracy of chromogranin A (CgA), pancreatic polypeptide (PP), and glucagon for pNET in MEN1. DESIGN: This was a diagnostic study. SETTING: The study was conducted at Dutch university medical centers from 2008 to 2011, representing 90% of the total Dutch MEN1 population. PATIENTS AND METHODS: Patients for whom data on tumor markers in combination with the reference standard (ie, radiological imaging) were available between 2008 and 2011 were included. The reference standard for the presence of pNET was pathology or detection on magnetic resonance imaging, computed tomography, or endoscopic ultrasound confirmed on subsequent imaging, irrespective of modality at follow-up. MAIN OUTCOME MEASURES: The area under the receiver-operating characteristic curve (AUC), positive predictive value, negative predictive value, positive likelihood ratio, negative likelihood ratio, sensitivity, and specificity were calculated for each marker. RESULTS: For the analysis of PP, CgA, and glucagon, 73, 81, and 94 patients were available, respectively. The AUC for CgA was 0.48 [95% confidence interval (CI) 0.35-0.61] with a sensitivity 0.33 and a specificity 0.73; the AUC for glucagon was 0.58 (95% CI 0.46-0.70) with a sensitivity 0.43 and a specificity 0.73; and the AUC for PP was 0.64 (95% CI 0.50-0.77) with a sensitivity 0.36 and a specificity 0.74. Age, imaging modality, tumor size, and number did not influence the outcomes. CONCLUSION: The diagnostic accuracy of the tumor markers CgA, PP, and glucagon for pNET in MEN1 is low.

Published
2013

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