Search

Your search keyword '"Brons, P.P."' showing total 23 results
Start Over Author "Brons, P.P."
23 results on '"Brons, P.P."'

2. Little discrepancy between one-stage and chromogenic factor VIII (FVIII)/IX assays in a large international cohort of persons with nonsevere hemophilia A and B.

Author

Zwagemaker, A.F., Kloosterman, F.R., Gouw, S.C., Boyce, S., Brons, P.P., Cnossen, M.H., Collins, P.W., Eikenboom, J., Hay, C., Hengeveld, R.C.C., Jackson, S., Klopper-Tol, C.A.M., Kruip, M.J.H.A., Laros-van Gorkom, B.A.P., Male, C., Nieuwenhuizen, L., Shapiro, S., Fijnvandraat, K., Coppens, M., Zwagemaker, A.F., Kloosterman, F.R., Gouw, S.C., Boyce, S., Brons, P.P., Cnossen, M.H., Collins, P.W., Eikenboom, J., Hay, C., Hengeveld, R.C.C., Jackson, S., Klopper-Tol, C.A.M., Kruip, M.J.H.A., Laros-van Gorkom, B.A.P., Male, C., Nieuwenhuizen, L., Shapiro, S., Fijnvandraat, K., and Coppens, M.

Abstract

01 april 2023, Item does not contain fulltext, BACKGROUND: Accurate measurements of coagulation factor activity form an essential part of hemophilia management and are performed by the one-stage or chromogenic assay. Current literature suggests that approximately one-third of persons with nonsevere hemophilia A exhibit assay discrepancy, albeit with a high variability between studies. Such data are scarce in nonsevere hemophilia B. OBJECTIVES: To investigate the extent of factor VIII/IX one-stage and chromogenic assay discrepancy in moderate and mild hemophilia A and B. METHODS: Persons with previously diagnosed nonsevere hemophilia A and B with a factor level of 2 to 35 IU/dL were included from the international DYNAMO cohort study. Central measurements of the factor VIII and IX activity levels were performed by the one-stage and chromogenic assay. Relative and absolute discrepancy definitions were used, with the International Society on Thrombosis and Haemostasis-Scientific and Standardization Committee proposed ratio of >2.0 or <0.5 being the primary outcome. Discrepancy was also evaluated in a subgroup of 13 persons with mutations previously associated with discrepancy (≥3 cases reported in literature). RESULTS: A total of 220 persons were included, of whom 3 (1%) showed assay discrepancy: 2/175 hemophilia A and 1/45 hemophilia B. Six persons (3%) exhibited an absolute difference >10 IU/dL between the assay results. In addition, with more lenient definitions, over 90% of participants (n = 197) had no discrepant results. Only 1 out of 13 persons with a mutation previously associated with discrepancy had significant assay discrepancy. CONCLUSION: Little assay discrepancy was observed despite the presence of mutations previously associated with discrepancy, suggesting that the presence and magnitude of assay discrepancy are largely determined by laboratory variables.

Published
2023

3. Inhibitor development and mortality in non‐severe hemophilia A

Author

Eckhardt, C.L., Loomans, J.I., van Velzen, A.S., Peters, M., Mauser‐Bunschoten, E.P., Schwaab, R., Mazzucconi, M.G., Tagliaferri, A., Siegmund, B., Reitter‐Pfoertner, S.E., van der Bom, J.G., Fijnvandraat, K., Kamphuisen, P.W., Peerlinck, K., Oldenburg, J., Santagostino, E., Astermark, J., Eckhardt, C.L, van Velzen, A.S, Streefkerk, N., Loomans, J.L., van Eijkelenburg, A., Jansen, A.J., Kruijt, C.C., van Tienoven, B., van Baar, A.C.G., Corten, I.W., Meijer, K., Nijziel, M.R., Dors, N., Hamulyak, K., Beckers, E., Brons, P.P., Laros‐van Gorkom, B.A.P., van Heerde, W.L., Leebeek, F., Kruip, M., Cnossen, M.H., Mauser‐Bunschoten, E., Fischer, K., Smiers, F.J., Hermans, C., Klamroth, R., Escuriola‐Ettingshausen, C., Königs, C., Petrini, P., Holmström, M., Mäkipernaa, A., Male, C., Pabinger, I., Keenan, R.D., Liesner, R., Khair, K., Yee, T.T., Hart, D.P., Rangarajan, S., Mitchell, M., Thompson, G., Haya, S., Moret, A., Cid, A.R., Jimenez‐Yuste, V., Mancuso, M.E., Mazzuconni, M.G., Santoro, C., Morfini, M., Castaman, G., Schinco, P., Rivolta, G.F., Platokouki, H., and McRae, S.

Published
2015
Full Text
View/download PDF

5. Perioperative pharmacokinetic-guided factor VIII concentrate dosing in haemophilia (OPTI-CLOT trial): an open-label, multicentre, randomised, controlled trial

Author

Moort, I. van, Preijers, T., Bukkems, L.H., Hazendonk, H., Bom, J.G. van der, Laros-van Gorkom, B.A.P., Beckers, E.A., Nieuwenhuizen, L., Meer, F.J. van der, Ypma, P., Coppens, M., Fijnvandraat, K., Schutgens, R.E., Meijer, K, Leebeek, F.W.G., Brons, P.P., Schols, S.E.M., Mathôt, R.A.A., Cnossen, M.H., Moort, I. van, Preijers, T., Bukkems, L.H., Hazendonk, H., Bom, J.G. van der, Laros-van Gorkom, B.A.P., Beckers, E.A., Nieuwenhuizen, L., Meer, F.J. van der, Ypma, P., Coppens, M., Fijnvandraat, K., Schutgens, R.E., Meijer, K, Leebeek, F.W.G., Brons, P.P., Schols, S.E.M., Mathôt, R.A.A., and Cnossen, M.H.

Abstract

Item does not contain fulltext, BACKGROUND: Dosing of replacement therapy with factor VIII concentrate in patients with haemophilia A in the perioperative setting is challenging. Underdosing and overdosing of factor VIII concentrate should be avoided to minimise risk of perioperative bleeding and treatment costs. We hypothesised that dosing of factor VIII concentrate on the basis of a patient's pharmacokinetic profile instead of bodyweight, which is standard treatment, would reduce factor VIII consumption and improve the accuracy of attained factor VIII levels. METHODS: In this open-label, multicentre, randomised, controlled trial (OPTI-CLOT), patients were recruited from nine centres in Rotterdam, Groningen, Utrecht, Nijmegen, The Hague, Leiden, Amsterdam, Eindhoven, and Maastricht in The Netherlands. Eligible patients were aged 12 years or older with severe or moderate haemophilia A (severe haemophilia was defined as factor VIII concentrations of <0·01 IU/mL, and moderate haemophilia as 0·01-0·05 IU/mL), without factor VIII inhibitors, and planned for elective low or medium risk surgery as defined by surgical risk score. Patients were randomly assigned (1:1) using a web-based randomisation system and treatment minimisation, stratified by method of administration of factor VIII concentrate (continuous infusion vs bolus administration) and risk level of surgery (low and medium risk surgery), to the pharmacokinetic-guided or standard treatment group. The primary endpoint was total amount of infused factor VIII concentrate (IU per kg bodyweight) during perioperative period (from day of surgery up to 14 days after surgery). Analysis was by intention to treat and the safety analysis population comprised all participants who underwent surgery with factor VIII concentrate. This study is registered with the Netherlands Trial Registry, NL3955, and is now closed to accrual. FINDINGS: Between May 1, 2014, and March 1, 2020, 98 patients were assessed for eligibility and 66 were enrolled in the trial and rand

Published
2021

6. Acrophyseal growth arrest in a long-term survivor of acute lymphoblastic leukemia

Author

Rooy, J.W.J. de, Buckens, C.F.M., Brons, P.P., Geest, I.C. van der, Vanhoenacker, F., Rooy, J.W.J. de, Buckens, C.F.M., Brons, P.P., Geest, I.C. van der, and Vanhoenacker, F.

Abstract

Contains fulltext : 229552.pdf (Publisher’s version ) (Open Access), Growth arrest at the secondary growth plate, also known as the acrophysis, is a rare phenomenon with only very few known published case reports. We report on a case of formation of ghost secondary ossification centers at the acrophyses of the knee joint in a 14-year-old female, who survived early childhood acute lymphoblastic leukemia. The patient suffered from severe side effects from both disease and subsequent treatment strategies with a 10-month immobilization period as a consequence at the age of 3 years. The ghost secondary ossification centers were encountered on radiographs and MRI 10 years later, when she presented for evaluation of chronic pain in her left knee related to sports activities, due to a meniscal cyst. Awareness of this phenomenon is nevertheless important, because it seems that endochondral bone growth recovery at the acrophyses might be different from recovery in physes, because we found no concomitant sequelae of growth arrest in the metaphyses.

Published
2020

7. ADAMTS-13 and bleeding phenotype in von Willebrand disease

Author

Boender, J. (Johan), Nederlof, A. (Angelique), Meijer, K. (Karina), Mauser-Bunschoten, E.P. (Evelien P.), Cnossen, M.H. (Marjon), Fijnvandraat, K., Bom, J.G. (Anske) van der, Meris, J. (Joke) de, Laros-Van Gorkom, B.A.P. (Britta), Galen, K.P.M. van, Eikenboom, J.C.J. (Jeroen), Maat, M.P.M. (Moniek) de, Leebeek, F.W.G. (Frank), Coppens, M. (M.), Nieuwenhuizen, L. (Laurens), Tamminga, R.Y.J. (R. Y.J.), Ypma, P.F. (Paula), Smiers, F.J.W. (Frans), Beckers, E.A.M. (Erik), Brons, P.P., Atiq, F. (Ferdows), Boender, J. (Johan), Nederlof, A. (Angelique), Meijer, K. (Karina), Mauser-Bunschoten, E.P. (Evelien P.), Cnossen, M.H. (Marjon), Fijnvandraat, K., Bom, J.G. (Anske) van der, Meris, J. (Joke) de, Laros-Van Gorkom, B.A.P. (Britta), Galen, K.P.M. van, Eikenboom, J.C.J. (Jeroen), Maat, M.P.M. (Moniek) de, Leebeek, F.W.G. (Frank), Coppens, M. (M.), Nieuwenhuizen, L. (Laurens), Tamminga, R.Y.J. (R. Y.J.), Ypma, P.F. (Paula), Smiers, F.J.W. (Frans), Beckers, E.A.M. (Erik), Brons, P.P., and Atiq, F. (Ferdows)

Abstract

Background: The bleeding phenotype of von Willebrand disease (VWD) varies highly between patients and can only partly be explained by von Willebrand factor (VWF) parameters. By cleaving large VWF multimers into smaller, less active multimers, ADAMTS-13 is an important regulator of VWF activity. However, it is unknown what the role of ADAMTS-13 is in individuals with VWD. Objectives: We therefore studied how ADAMTS-13 activity is associated with the laboratory and bleeding phenotype in individuals with VWD. Methods: We measured ADAMTS-13 activity using the fluorescence resonance energy transfer substrate VWF 73 assay in 638 individuals with VWD in the nationwide cross-sectional Willebrand in the Netherlands study and in 36 healthy controls. The bleeding phenotype was assessed using the Tosetto bleeding score. Results: ADAMTS-13 activity was similar in individuals with VWD (109% ± 20.6%) and controls (110% ± 19.7%). ADAMTS-13 activity was higher in individuals with VWD with type 3 than those with type 1 (mean difference, 11.8%; 95% confidence interval [CI], 2.9%-20.8%) or type 2 (mean difference, 16.1%; 95% CI, 7.1%-25.1%). ADAMTS-13 activity was not associated with the Tosetto bleeding score (0.1 Tosetto bleeding score increase per 10% ADAMTS-13 increase, 95% CI, −0.2 to 0.3). Furthermore, ADAMTS-13 activity did not differ between individuals with and without a bleeding event during the year preceding blood sampling (mean difference, 1.4%; 95% CI, −2.1% to 4.9%). Conclusion: ADAMTS-13 activity was highest in individuals with type 3 VWD, but it had only minor associations with VWF parameters. ADAMTS-13 activity does not influence the bleeding phenotype in individuals with VWD.

Published
2020
Full Text
View/download PDF

8. The incidence and treatment of bleeding episodes in non-severe haemophilia A patients with inhibitors

Author

Velzen, A.S. van, Eckhardt, C.L., Streefkerk, N., Peters, M., Hart, D.P., Hamulyak, K., Klamroth, R., Meijer, K., Nijziel, M.R., Schinco, P., Yee, T.T, Bom, J.G. Van Der, Fijnvandraat, K., Brons, P.P., Laros-van Gorkom, B.A.P., Other departments, Paediatric Infectious Diseases / Rheumatology / Immunology, Interne Geneeskunde, RS: FHML non-thematic output, RS: CARIM - R1.04 - Clinical thrombosis and haemostasis, and Real World Studies in PharmacoEpidemiology, -Genetics, -Economics and -Therapy (PEGET)

Subjects
0301 basic medicine, Pediatrics, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], 030204 cardiovascular system & hematology, PROPHYLAXIS, Cohort Studies, 0302 clinical medicine, Interquartile range, Haemophilia A, MUTATION, bypassing agents, RISK, education.field_of_study, FACTOR-VIII, Incidence (epidemiology), Incidence, FEIBA, NOVOSEVEN, Hematology, Middle Aged, Phenotype, Cohort, Severe haemophilia A, factor VIII inhibitors, Female, Adult, medicine.medical_specialty, Adolescent, Population, Hemorrhage, Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], Hemophilia A, Antibodies, 03 medical and health sciences, Young Adult, medicine, Effective treatment, Humans, education, Bleeding episodes, Factor VIII, business.industry, MORTALITY, Other Research Radboud Institute for Health Sciences [Radboudumc 0], MILD, medicine.disease, FACTOR-IX INHIBITORS, management of disease, 030104 developmental biology, haemostasis, business
Abstract

SummaryThe development of an inhibitory antibody in non-severe haemophilia A patients may aggravate the bleeding phenotype considerably. Effective treatment of bleeding episodes may be challenging, with ensuing severe complications. At present, evidence is scarce for optimal treatment of bleeding episodes in this patient group. The aim of this study was to describe the incidence and the treatment of bleeding episodes in inhibitor patients in a population-based unselected cohort of non-severe haemophilia A patients with clinically relevant inhibitors. Data were available for 100 of the 107 non-severe haemophilia A patients (factor VIII (FVIII) baseline, 2–40 lU/dl) from 29 centres in Europe and one centre in Australia who had developed a clinically relevant inhibitor between 1980 and 2011. The majority (89 %) of the patients were treated during the inhibitor period for bleeding episodes or a surgical intervention: 66 % needed treatment for bleeding episodes, at a median annual bleeding rate (ABR) of 1.1 (interquartile range (IQR) 0.1–2.5) and a median total of 2 (IQR 1–6) bleeding episodes. Compared to the median ABR before inhibitor development of 0.095 bleeds per year (IQR 0.02–0.42), the increase in ABR is more than a 10-fold. More than 90 % of the bleeding episodes were treated with only one type of product, most frequently (51 %) FVIII concentrates. This study provides the incidence of bleeding episodes and treatment choices in non-severe haemophilia A patients with inhibitors. The 10-fold increase to a median ABR of 1.1 episodes per year emphasizes the impact of inhibitor development for non-severe haemophilia A patients.

Published
2016
Full Text
View/download PDF

9. Whole exome sequencing in the diagnostic workup of patients with a bleeding diathesis

Author

Saes, J.L., Simons, A., Munnik, S.A. de, Nijziel, M.R., Blijlevens, N.M.A., Jongmans, M.C., Reijden, B.A. van der, Brons, P.P., Heerde, W.L. van, Schols, S.E.M., Saes, J.L., Simons, A., Munnik, S.A. de, Nijziel, M.R., Blijlevens, N.M.A., Jongmans, M.C., Reijden, B.A. van der, Brons, P.P., Heerde, W.L. van, and Schols, S.E.M.

Abstract

Contains fulltext : 201282.pdf (publisher's version ) (Closed access)

Published
2019

11. One piece of the puzzle: Population pharmacokinetics of FVIII during perioperative Haemate P®/Humate P® treatment in von Willebrand disease patients

Author

de Jager, N.C.B. (Nico C. B.), Bukkems, L.H. (Laura H.), Heijdra, J.M. (Jessica), Hazendonk, C.H.C.A.M. (Carolien H. C. A. M.), Fijnvandraat, K., Meijer, K. (Karina), Eikenboom, J.C.J. (Jeroen), Laros-Van Gorkom, B.A.P. (Britta), Leebeek, F.W.G. (Frank), Cnossen, M.H. (Marjon), Mathot, R.A. (Ron), Collins, P.W., Kruip, M.J.H.A. (Marieke), Polinder, S. (Suzanne), Lock, J. (J.), Moort, I. (Iris) van, Goedhart, M.C.H.J. (M. C.H.J.), Coppens, M., Peters, M.A.D. (Marjolein), Preijers, T., Brons, P.P., Meer, F.J.M. (Felix) van der, Schutgens, R. (Roger), Fischer, K. (Kathelijn), Driessens, M.H.E. (M. H.E.), Zwaan, C.M. (Michel), van Vliet, I. (I.), Liesner, R. (Ri), Chowdary, P. (P.), Keeling, D. (D.), de Jager, N.C.B. (Nico C. B.), Bukkems, L.H. (Laura H.), Heijdra, J.M. (Jessica), Hazendonk, C.H.C.A.M. (Carolien H. C. A. M.), Fijnvandraat, K., Meijer, K. (Karina), Eikenboom, J.C.J. (Jeroen), Laros-Van Gorkom, B.A.P. (Britta), Leebeek, F.W.G. (Frank), Cnossen, M.H. (Marjon), Mathot, R.A. (Ron), Collins, P.W., Kruip, M.J.H.A. (Marieke), Polinder, S. (Suzanne), Lock, J. (J.), Moort, I. (Iris) van, Goedhart, M.C.H.J. (M. C.H.J.), Coppens, M., Peters, M.A.D. (Marjolein), Preijers, T., Brons, P.P., Meer, F.J.M. (Felix) van der, Schutgens, R. (Roger), Fischer, K. (Kathelijn), Driessens, M.H.E. (M. H.E.), Zwaan, C.M. (Michel), van Vliet, I. (I.), Liesner, R. (Ri), Chowdary, P. (P.), and Keeling, D. (D.)

Abstract

Introduction: Many patients with von Willebrand disease (VWD) are treated on demand with von Willebrand factor and factor VIII (FVIII) containing concentrates present with VWF and/or FVIII plasma levels outside set target levels. This carries a risk for bleeding and potentially for thrombosis. Development of a population pharmacokinetic (PK) model based on FVIII levels is a first step to more accurate on-demand perioperative dosing of this concentrate.

Published
2019
Full Text
View/download PDF

12. Population pharmacokinetics of factor IX in hemophilia B patients undergoing surgery

Author

Preijers, T., Hazendonk, H.C.A.M., Liesner, R., Chowdary, P., Driessens, M.H.E., Hart, D., Brons, P.P., Laros-van Gorkom, B.A.P., Cnossen, M.H., Mathot, R.A.A., Preijers, T., Hazendonk, H.C.A.M., Liesner, R., Chowdary, P., Driessens, M.H.E., Hart, D., Brons, P.P., Laros-van Gorkom, B.A.P., Cnossen, M.H., and Mathot, R.A.A.

Abstract

Contains fulltext : 198341.pdf (Publisher’s version ) (Open Access)

Published
2018

13. Factor VIII gene (F8) mutation and risk of inhibitor development in nonsevere hemophilia A

Author

Eckhardt, C.L., Velzen, A.S. van, Peters, M., Astermark, J., Brons, P.P., Castaman, G., Cnossen, M.H., Dors, N., Escuriola-Ettingshausen, C., Hamulyak, K., Hart, D.P., Hay, C.R.M., Haya, S., Heerde, W.L. van, Hermans, C., Holmstrom, M., Jimenez-Yuste, V., Keenan, R.D., Klamroth, R., Gorkom, B.A.P., Leebeek, F.W.G., Liesner, R., Makipernaa, A., Male, C., Mauser-Bunschoten, E., Mazzucconi, M.G., Mcrae, S., Meijer, K., Mitchell, M., Morfini, M., Nijziel, M., Oldenburg, J., Peerlinck, K., Petrini, P., Platokouki, H., Reitter-Pfoertner, S.E., Santagostino, E., Schinco, P., Smiers, F.J., Siegmund, B., Tagliaferri, A., Yee, T.T., Kamphuisen, P.W., Bom, J.G. van der, Fijnvandraat, K., INSIGHT Study Grp, UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service d'hématologie, UCL - (SLuc) Centre de malformations vasculaires congénitales, Cardiovascular Centre (CVC), Vascular Ageing Programme (VAP), RS: CARIM School for Cardiovascular Diseases, Biochemie, Interne Geneeskunde, Pediatrics, Hematology, Epidemiology, Other departments, Paediatric Infectious Diseases / Rheumatology / Immunology, ACS - Amsterdam Cardiovascular Sciences, and AII - Amsterdam institute for Infection and Immunity

Subjects
Invasive mycoses and compromised host Translational research [N4i 2], Adult, medicine.medical_specialty, Age-related aspects of cancer [ONCOL 2], Time Factors, Adolescent, Genotype, Immunology, Mutation, Missense, Kaplan-Meier Estimate, Hemophilia A, DIAGNOSIS, Biochemistry, Gastroenterology, Young Adult, Interquartile range, Risk Factors, Internal medicine, medicine, Missense mutation, Humans, Cumulative incidence, Desmopressin, Genotyping, POLYMORPHISMS, Retrospective Studies, Hematology, Factor VIII, Cardiovascular diseases [NCEBP 14], business.industry, Incidence (epidemiology), DESMOPRESSIN, Cell Biology, Middle Aged, MILD, Antibodies, Neutralizing, Confidence interval, Treatment Outcome, business, medicine.drug, Follow-Up Studies
Abstract

Neutralizing antibodies (inhibitors) toward factor VIII form a severe complication in nonsevere hemophilia A, profoundly aggravating the bleeding pattern. Identification of high-risk patients is hampered by lack of data that take exposure days to therapeutic factor VIII concentrates into account. In the INSIGHT study, we analyzed the association between F8 mutation and inhibitor development in patients with nonsevere hemophilia A (factor VIII 2-40 IU/dL). This analysis included 1112 non-severe hemophilia A patients from 14 centers in Europe and Australia that had genotyped at least 70% of their patients. Inhibitor risk was calculated as Kaplan-Meier incidence with cumulative number of exposure days as the time variable. During 44 800 exposure days (median, 24 exposure days per patient; interquartile range [IQR], 7-90), 59 of the 1112 patients developed an inhibitor; cumulative incidence of 5.3% (95% confidence interval [CI], 4.0-6.6) after a median of 28 exposure days (IQR, 12-71). The inhibitor risk at 50 exposure days was 6.7% (95% CI, 4.5-8.9) and at 100 exposure days the risk further increased to 13.3% (95% CI, 9.6-17.0). Among a total of 214 different F8 missense mutations 19 were associated with inhibitor development. These results emphasize the importance of F8 genotyping in nonsevere hemophilia A. ( Blood . 2013; 122(11):1954-1962) © 2013 by The American Society of Hematology.

Published
2013
Full Text
View/download PDF

14. School-aged children after the end of successful treatment of non-central nervous system cancer: longitudinal assessment of health-related quality of life, anxiety and coping

Author

Maurice-Stam, H., Oort, F.J., Last, B.F., Brons, P.P., Caron, H.N., Grootenhuis, M.A., Developmental Psychopathology (RICDE, FMG), Faculteit der Geneeskunde, Cancer Center Amsterdam, Amsterdam Public Health, Paediatric Psychosocial Care, Medical Psychology, Other Research, Paediatric Oncology, and Clinical Developmental Psychology

Subjects
Male, Coping (psychology), medicine.medical_specialty, Age-related aspects of cancer [ONCOL 2], Health Status, Population, Disease, Anxiety, Cognition, Sex Factors, SDG 3 - Good Health and Well-being, Neoplasms, Adaptation, Psychological, medicine, Humans, Longitudinal Studies, Survivors, Child, education, Psychiatry, Netherlands, Health related quality of life, education.field_of_study, School age child, business.industry, humanities, Cognitive coping, Oncology, Motor Skills, Central nervous system cancer, Quality of Life, Female, medicine.symptom, business, Clinical psychology
Abstract

Contains fulltext : 81585.pdf (Publisher’s version ) (Closed access) The aim of the study was to investigate: (1) health-related quality of life (HRQoL) and anxiety in school-aged cancer survivors during the first 4 years of continuous remission after the end of treatment; and (2) correlations of disease-related coping with HRQoL and anxiety. A total of 76 survivors aged 8-15 years completed questionnaires about HRQoL, anxiety and disease-related cognitive coping at one to five measurement occasions. Their HRQoL was compared with norm data, 2 months (n = 49) and 1 year (n = 41), 2 years (n = 41), 3 years (n = 42) and 4 years (n = 27) after treatment. Through longitudinal mixed models analyses it was investigated to what extent disease-related cognitive coping was associated with HRQoL and anxiety over time, independent of the impact of demographic and medical variables. Survivors reported worse Motor Functioning (HRQoL) 2 months after the end of treatment, but from 1 year after treatment they did no longer differ from the norm population. Lower levels of anxiety were associated with male gender, being more optimistic about the further course of the disease (predictive control) and less searching for information about the disease (interpretative control). Stronger reliance on the physician (vicarious control) was associated with better mental HRQoL. As a group, survivors regained good HRQoL from 1 year after treatment. Monitoring and screening survivors are necessary to be able to trace the survivors at risk of worse HRQoL.

Published
2009
Full Text
View/download PDF

15. Facilitating the implementation of pharmacokinetic-guided dosing of prophylaxis in haemophilia care by discrete choice experiment

Author

Lock, J., Bekker-Grob, E.W. de, Urhan, G., Peters, M., Meijer, K., Brons, P.P., Meer, F.J. van der, Driessens, M.H., Collins, P.W., Fijnvandraat, K., Leebeek, F.W., Cnossen, M.H., Laros-van Gorkom, B.A.P., Wildt, S.N. de, Pediatrics, Public Health, Hematology, Real World Studies in PharmacoEpidemiology, -Genetics, -Economics and -Therapy (PEGET), Paediatric Infectious Diseases / Rheumatology / Immunology, Amsterdam Cardiovascular Sciences, Amsterdam institute for Infection and Immunity, Amsterdam Gastroenterology Endocrinology Metabolism, Cancer Center Amsterdam, Other Research, Pharmacy, Graduate School, and Vascular Medicine

Subjects
Male, Pediatrics, CONJOINT-ANALYSIS, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], Discrete choice experiment, 030204 cardiovascular system & hematology, Choice Behavior, 0302 clinical medicine, PHYSICIANS, PHARMACISTS PREFERENCES, Surveys and Questionnaires, Health care, Drug Dosage Calculations, Tissue Distribution, Genetics(clinical), Young adult, Non-U.S. Gov't, implementation, Genetics (clinical), preferences, FACTOR-VIII, 030503 health policy & services, Research Support, Non-U.S. Gov't, General Medicine, Hematology, Middle Aged, Female, prophylaxis, 0305 other medical science, Adult, medicine.medical_specialty, Factor concentrate, Adolescent, FEASIBILITY, haemophilia, Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], Haemophilia, Research Support, Hemophilia A, PATIENT, pharmacokinetic-guided dosing, 03 medical and health sciences, Young Adult, Pharmacokinetics, medicine, Journal Article, Humans, Dosing, Intensive care medicine, Aged, Models, Statistical, ECONOMICS, business.industry, discrete choice experiment, medicine.disease, Facilitator, HEALTH-CARE, Renal disorders Radboud Institute for Health Sciences [Radboudumc 11], business, INHIBITORS
Abstract

Item does not contain fulltext INTRODUCTION: Patients', parents' and providers' preferences with regard to medical innovations may have a major impact on their implementation. AIM: To evaluate barriers and facilitators for individualized pharmacokinetic (PK)-guided dosing of prophylaxis in haemophilia patients, parents of young patients, and treating professionals by discrete choice experiment (DCE) questionnaire. PATIENTS/METHODS: The study population consisted of patients with haemophilia currently or previously on prophylactic treatment with factor concentrate (n = 114), parents of patients aged 12-18 years (n = 19) and haemophilia professionals (n = 91). DCE data analysis was performed, taking preference heterogeneity into account. RESULTS: Overall, patients and parents, and especially professionals were inclined to opt for PK-guided dosing of prophylaxis. In addition, if bleeding was consequently reduced, more frequent infusions were acceptable. However, daily dosing remained an important barrier for all involved. 'Reduction of costs for society' was a facilitator for implementation in all groups. CONCLUSIONS: To achieve implementation of individualized PK-guided dosing of prophylaxis in haemophilia, reduction of bleeding risk and reduction of costs for society should be actively discussed as they are motivating for implementation; daily dosing is still reported to be a barrier for all groups. The knowledge of these preferences will enlarge support for this innovation, and aid in the drafting of implementable guidelines and information brochures for patients, parents and professionals.

Published
2016

16. WiN Study Group: CLEC4M and STXBP5 gene variations contribute to von Willebrand factor level variation in von Willebrand disease

Author

Sanders, Y.V., Bom, J.G. Van Der, Isaacs, A., Cnossen, M.H., Maat, M.P. de, Laros-van Gorkom, B.A.P., Fijnvandraat, K., Meijer, K., Duijn, C.M. van, Mauser-Bunschoten, E.P., Eikenboom, J., Leebeek, F.W., and Brons, P.P.

Subjects
Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9]
Abstract

Item does not contain fulltext

Published
2015

17. Prediction of DDAVP response in 850 non-severe hemophilia A patients

Author

Loomans, J.I., Velzen, A.S. van, Eckhardt, C.L., Peters, M., Astermark, J., Brons, P.P., Carcao, M.D., Castaman, G., Cnossen, M.H., Dors, N., Escuriola-Ettingshausen, C., Hamulyak, K., Hart, D.P., Haya, S., Heerde, W.L. van, Hermans, C., Holmstrom, M., Jackson, S.C., Jimenez-Yuste, V., Keenan, R.D., Klamroth, R., Konigs, C., Kruip, M.J.H.A., Laros-Van Gorkom, B.A.P., Leebeek, F.W.G., Makipernaa, A., Male, C., Mauser-Bunschoten, E., Mazzucconi, M.G., Mcrae, S., Meijer, K., Mitchell, M., Morfini, M., Nance, D., Nijziel, M., Oldenburg, J., Peerlinck, K., Petrini, P., Platokouki, H., Rangarajan, S., Reitter-Pfoertner, S.E., Santagostino, E., Schinco, P., Tagliaferri, A., Yee, T.T., Kamphuisen, P.W., Bom, J.G. van der, Fijnvandraat, K., and Rise Study Grp

Published
2014

18. Von Willebrand Factor antigen and age explain variation in baseline FVIII:C among nonsevere hemophilia A patients with the same F8 genotype (Arg593Cys and Asn618Ser)

Author

Loomans, J.I., Velzen, A.S. van, Eckhardt, C.L., Peters, M., Astermark, J., Brons, P.P., Castaman, G., Cnossen, M.H., Dors, N., Escuriola-Ettingshausen, C., Hamulyak, K., Hart, D.P., Hay, C.R.M., Haya, S., Heerde, W.L. van, Hermans, C., Holmstroom, M., Jimenez-Yuste, V., Keenan, R.D., Klamroth, R., Konigs, C., Kruip, M.J.H.A., Laros-Van Gorkom, B.A.P., Leebeek, F.W.G., Liesner, R., Makipernaa, A., Male, C., Mauser-Bunschoten, E., Mazzucconi, M.G., Mcrae, S., Meijer, K., Mitchell, M., Morfini, M., Nijziel, M., Oldenburg, J., Peerlinck, K., Petrini, P., Platokouki, H., Rangarajan, S., Reitter-Pfoertner, S.E., Santagostino, E., Schinco, P., Smiers, F.J., Siegmund, B., Tagliaferri, A., Yee, T.T., Kamphuisen, P.W., Bom, J.G. van der, Fijnvandraat, K., and Insight Rise Study Grp

Published
2014

19. Clinical presentation of inhibitor development in non-severe hemophilia A: half of patients have high titer inhibitors and present with bleeding complications

Author

Eckhardt, C.L., Loomans, J.I., Velzen, A.S. van, Peters, M., Astermark, J., Brons, P.P., Castaman, G., Cnossen, M.H., Dors, N., Escuriola-Ettingshausen, C., Hamulyak, K., Hart, D.P., Hay, C.R.M., Haya, S., Heerde, W.L. van, Hermans, C., Holmstrom, M., Jimenez-Yuste, V., Keenan, R.D., Klamroth, R., Laros-Gorkom, B.A.P. van, Leebeek, F.W.G., Liesner, R., Makipernaa, A., Male, C., Mauser-Bunschoten, E., Mazzucconi, M.G., Mcrae, S., Meijer, K., Mitchell, M., Morfini, M., Nijziel, M., Oldenburg, J., Peerlinck, K., Petrini, P., Platokouki, H., Rangarajan, S., Reitter-Pfoertner, S.E., Santagostino, E., Schinco, P., Smiers, F.J., Siegmund, B., Tagliaferri, A., Yee, T.T., Kamphuisen, P.W., Bom, J.G. van der, Fijnvandraat, K., and Insight Study Grp

Published
2014

20. Inhibitors increase the burden of disease in nonsevere haemophilia A patients - treatment strategies to obtain hemostasis

Author

Velzen, A.S. van, Eckhardt, C.L., Streefkerk, N., Peters, M., Astermark, J., Brons, P.P., Castaman, G., Cnossen, M.H., Dors, N., Escuriola-Ettingshausen, C., Hamulyak, K., Hart, D.P., Hay, C.R.M., Haya, S., Heerde, W.L. van, Hermans, C., Holmstrom, M., Jimenez-Yuste, V., Keenan, R.D., Klamroth, R., Gorkom, B.A.P.L. van, Leebeek, F.W.G., Liesner, R., Makipernaa, A., Male, C., Mauser-Bunschoten, E., Mazzucconi, M.G., McRae, S., Meijer, K., Morfini, M., Nijziel, M., Oldenburg, J., Peerlinck, K., Petrini, P., Platokouki, H., Rangarajan, S., Reitter-Pfoertner, S.E., Santagostino, E., Schinco, P., Smiers, F.J., Siegmund, B., Tagliaferri, A., Yee, T.T., Kamphuisen, P.W., Bom, J.G. van der, Fijnvandraat, K., and INSIGHT Study Grp

Published
2014

21. Clinical phenotype in genetically confirmed von Willebrand disease type 2N patients reflects a haemophilia A phenotype

Author

Meegeren, M.E.R. van, Mancini, T.L., Schoormans, S.C.M., Haren, B.J.T. van, Duren, C. van, Diekstra, A., Laros-van Gorkom, B.A.P., Brons, P.P., Simons, A., Hoefsloot, L.H., Heerde, W.L. van, Meegeren, M.E.R. van, Mancini, T.L., Schoormans, S.C.M., Haren, B.J.T. van, Duren, C. van, Diekstra, A., Laros-van Gorkom, B.A.P., Brons, P.P., Simons, A., Hoefsloot, L.H., and Heerde, W.L. van

Abstract

Item does not contain fulltext, INTRODUCTION: Von Willebrand disease (VWD) type 2N is characterized by a defective binding of factor VIII (FVIII) to von Willebrand factor (VWF) resulting in diminished plasma FVIII levels and a clinical phenotype mimicking mild haemophilia A. Several mutations in the FVIII binding site of VWF have been reported. AIM: This study aims to examine the effect of genotype on clinical phenotype in a cohort of VWD 2N patients. METHODS: Patients with at least one genetically confirmed 2N mutation were selected retrospectively from a cohort of patients with suspected VWD. Clinical and laboratory phenotypes including bleeding scores (BS) were obtained and analysed. RESULTS: Forty-two VWD 2N patients with a mean age of 44 years were included. Eleven patients were homozygous or compound heterozygous (genetically confirmed group) and 31 patients were heterozygously affected (carriers group). Statistically significant differences between genetically confirmed VWD 2N patients and carriers were found in FVIII activity, VWF antigen levels, VWF-FVIII binding capacity, FVIII/VWF antigen ratio (all P<0.001), VWF-ristocetin activity (p=0.001) and VWF collagen binding (P = 0.002). Median BS was 6 in genetically confirmed VWD 2N patients compared with 3 in carriers (P = 0.047). Haemarthrosis, muscle haematomas and postpartum haemorrhage were only reported in genetically confirmed 2N patients. CONCLUSION: Phenotypic analysis showed that all laboratory parameters are lower in genetically confirmed VWD 2N patients compared with heterozygous 2N carriers. The clinical phenotype in genetically confirmed VWD 2N patients is comparable to mild haemophilia A patients and more severe than heterozygous 2N carriers.

Published
2015

Catalog

Books, media, physical & digital resources
See catalog results