Your search keyword '"Atiq F"' showing total 102 results

1. Genetic variants, thrombocytopenia, and clinical phenotype of type 2B von Willebrand disease: a median 16-year follow-up study

Author

Fijnvandraat, K., Coppens, M., Kors, A., Zweegman, S., de Meris, J., Goverde, G.J., Jonkers, M.H., Dors, N., Nijziel, M.R., Nieuwenhuizen, L., Meijer, K., Tamminga, R.Y.J., van der Linden, P.W., Ypma, P.F., Eikenboom, H.C.J., van der Bom, J.G., Smiers, F.J.W., Granzen, B., Hamulyák, K., Brons, P., Laros-van Gorkom, B.A.P., Schols, S.E.M., Leebeek, F.W.G., Cnossen, M.H., Boender, J., Atiq, F., van Kwawegen, C.B., Mauser-Bunschoten, E.P., van Galen, K.P.M., van Kwawegen, Calvin B., Atiq, Ferdows, Endenburg, Dara, Fijnvandraat, Karin, van Galen, Karin P.M., Cnossen, Marjon H., Schols, Saskia E.M., Kruip, Marieke J.H.A., van Heerde, Waander L., de Meris, Joke, van der Bom, Johanna G., Eikenboom, Jeroen, Meijer, Karina, and Leebeek, Frank W.G.

Published

2024

2. Major differences in clinical presentation, diagnosis and management of men and women with autosomal inherited bleeding disorders

Author

Atiq, F., Saes, J.L., Punt, M.C., van Galen, K.P.M., Schutgens, R.E.G., Meijer, K., Cnossen, M.H., Laros-Van Gorkom, B.A.P., Peters, M., Nieuwenhuizen, L., Kruip, M.J.H.A., de Meris, J., van der Bom, J.G., van der Meer, F.J.M., Fijnvandraat, K., Kruis, I.C., van Heerde, W.L., Eikenboom, H.C.J., Leebeek, Frank W.G., and Schols, S.E.M.

Published

2021

3. ADAMTS‐13 and bleeding phenotype in von Willebrand disease

Author

Boender, Johan, Nederlof, Angelique, Meijer, Karina, Mauser‐Bunschoten, Evelien P., Cnossen, Marjon H., Fijnvandraat, Karin, van der Bom, Johanna G., de Meris, Joke, Laros‐van Gorkom, Britta A.P., van Galen, Karin P.M., Eikenboom, Jeroen, de Maat, Moniek P.M, Leebeek, Frank W.G., Coppens, M., Nieuwenhuizen, L., Tamminga, R.Y.J., Ypma, P.F., Smiers, F.J.W., Beckers, E., Brons, P., and Atiq, F.

Published

2020

4. PB0819 Quantification of von Willebrand Factor Proteoforms by Mass Spectrometry-Based Proteomics Reveals Differential Variant-to-Wild Type Stoichiometry in Subtypes of von Willebrand Disease

Author

van Duijl, T., primary, Kreft, I., additional, van Kwawegen, C., additional, Atiq, F., additional, Phan, W., additional, Schuller, M., additional, van der Zwaan, C., additional, Meijer, A., additional, Hoogendijk, A., additional, Bierings, R., additional, Leebeek, F., additional, and van den Biggelaar, M., additional

Published

2023

5. Desmopressin response depends on the presence and type of genetic variants in patients with type 1 and type 2 von Willebrand disease

Author

Atiq, F., Heijdra, J., Snijders, F., Boender, J., Kempers, E., Heerde, W.L. van, Maas, D.P.M.S.M., Krouwel, S., Schoormans, S.C., Meris, J. de, Schols, S.E.M., Galen, K.P.M. van, Bom, J.G. van der, Cnossen, M.H., Meijer, K., Fijnvandraat, K., Eikbenboom, J., Leebeek, F.W.G., WiN study Grp, Real World Studies in PharmacoEpidemiology, -Genetics, -Economics and -Therapy (PEGET), Paediatric Haematology, ARD - Amsterdam Reproduction and Development, Hematology, and Pediatrics

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, von Willebrand Diseases, hemic and lymphatic diseases, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], von Willebrand Factor, Humans, Deamino Arginine Vasopressin, Hematology, Exons, von Willebrand Disease, Type 2, hormones, hormone substitutes, and hormone antagonists, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]

Abstract

Contains fulltext : 282506.pdf (Publisher’s version ) (Open Access) Patients with type 1 and type 2 von Willebrand disease (VWD) can be treated with desmopressin. Although a previous study has shown that the location of the causative VWF gene variant is associated with desmopressin response in type 1 VWD, the association between variants in the VWF gene and desmopressin response is not yet fully understood. Our primary aim was to compare desmopressin response in type 1 VWD patients with and without a VWF gene variant. Secondly, we investigated whether desmopressin response depends on specific VWF gene variants in type 1 and type 2 VWD. We included 250 patients from the Willebrand in the Netherlands study: 72 type 1 without a VWF gene variant, 108 type 1 with a variant, 45 type 2A, 16 type 2M, and 9 type 2N patients. VWF gene was analyzed with ion semiconductor sequencing and Multiplex Ligation-dependent Probe Amplification. Complete response to desmopressin was observed in all type 1 VWD patients without a variant, 64.3% of type 1 patients with a variant, and 31.3% of type 2 patients (P < .001). Despite a large interindividual variability in desmopressin response, patients with the same variant had comparable desmopressin responses. For instance, in 6 type 1 patients with exon 4 to 5 deletion, mean VWF activity at 1 hour after desmopressin was 0.81 IU/mL, with a coefficient of variation of 22.9%. In conclusion, all type 1 VWD patients without a VWF gene variant respond to desmopressin. In type 1 and type 2 VWD patients with a VWF variant, desmopressin response highly depends on the VWF gene variants.

Published

2022

6. Importance of Genotyping in von Willebrand Disease to Elucidate Pathogenic Mechanisms and Variability in Phenotype

Author

Atiq, F., Boender, J., Heerde, W.L. van, Garcia, J.M.T., Schoormans, S.C., Krouwel, S., Cnossen, M.H., Laros-van Gorkom, B.A.P., Meris, J. de, Fijnvandraat, K., Bom, J.G. van der, Meijer, K., Galen, K.P.M. van, Eikenboom, J., Leebeek, F.W.G., WIN Study Grp, Paediatric Haematology, ARD - Amsterdam Reproduction and Development, Hematology, Pediatrics, and Real World Studies in PharmacoEpidemiology, -Genetics, -Economics and -Therapy (PEGET)

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, All institutes and research themes of the Radboud University Medical Center, CLINICAL MARKERS, hemic and lymphatic diseases, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], VWF PROPEPTIDE, MANAGEMENT, Hematology, FACTOR SURVIVAL, DIAGNOSIS, FAMILIES, circulatory and respiratory physiology

Abstract

Genotyping is not routinely performed at diagnosis of von Willebrand disease (VWD). Therefore, the association between genetic variants and pathogenic mechanism or the clinical and laboratory phenotype is unknown in most patients, especially in type 1 VWD. To investigate whether genotyping adds to a better understanding of the pathogenic mechanisms and variability in phenotype, we analyzed the VWF gene in 390 well-defined VWD patients, included in the WiN study. A VWF gene variant was found in 155 patients (61.5%) with type 1, 122 patients (98.4%) with type 2, and 14 patients (100%) with type 3 VWD. Forty-eight variants were novel. For each VWF gene variant, the pathogenic mechanisms associated with reduced VWF levels was investigated using the FVIII:C/VWF:Ag and VWFpp/VWF:Ag ratios. In type 1 VWD, reduced synthesis or secretion of VWF was most frequently found in patients with nonsense variants, frameshift variants, and deletions, whereas rapid clearance of VWF was mainly found in patients with missense variants. Furthermore, type 1 VWD patients with and without a VWF gene variant were clearly distinct in their clinical features such as age of diagnosis, laboratory phenotype, and bleeding phenotype. In type 2 VWD, 81% of variants were associated with an increased clearance of VWF. To conclude, we identified the pathogenic mechanisms associated with various VWF gene variants in type 1, 2, and 3 VWD patients. Additionally, major differences in the phenotype of type 1 VWD patients with and without a variant were observed, which may be of importance for clinical management.

Published

2022

7. Platelet degranulation and bleeding phenotype in a large cohort of Von Willebrand disease patients

Author

Swinkels, M., Atiq, F., Burgisser, P.E., Moort, I. van, Meijer, K., Eikenboom, J., Fijnvandraat, K., Galen, K.P.M. van, Meris, J. de, Schols, S.E.M., Bom, J.G. van der, Cnossen, M.H., Voorberg, J., Leebeek, F.W.G., Bierings, R., Jansen, A.J.G., WiN Study Grp, Hematology, Pediatrics, Real World Studies in PharmacoEpidemiology, -Genetics, -Economics and -Therapy (PEGET), Landsteiner Laboratory, Paediatric Haematology, ARD - Amsterdam Reproduction and Development, Experimental Vascular Medicine, ACS - Microcirculation, Vascular Medicine, ACS - Pulmonary hypertension & thrombosis, and ACS - Amsterdam Cardiovascular Sciences

Subjects

bleeding disorders, congenital, hereditary, and neonatal diseases and abnormalities, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], Hemorrhage, Hematology, platelet factor 4, von Willebrand Diseases, Phenotype, hemic and lymphatic diseases, von Willebrand Factor, platelet activation, Humans, VWF, VWD

Abstract

Contains fulltext : 282574.pdf (Publisher’s version ) (Open Access) Von Willebrand disease (VWD) is a bleeding disorder caused by quantitative (type 1 or 3) or qualitative (type 2A/2B/2M/2N) defects of circulating von Willebrand factor (VWF). Circulating VWF levels not always fully explain bleeding phenotypes, suggesting a role for alternative factors, like platelets. Here, we investigated platelet factor 4 (PF4) in a large cohort of patients with VWD. PF4 levels were lower in type 2B and current bleeding phenotype was significantly associated with higher PF4 levels, particularly in type 1 VWD. Based on our findings we speculate that platelet degranulation and cargo release may play a role across VWD subtypes.

Published

2022

8. Von Willebrand disease type 2M: Correlation between genotype and phenotype

Author

Maas, D.P.M.S.M., Atiq, F., Blijlevens, N.M.A., Brons, P.P.T., Krouwel, S., Laros-van Gorkom, B.A.P., Leebeek, F.W.G., Nieuwenhuizen, Laurens, Schoormans, S.C.M., Simons, A., Meijer, D., Heerde, W.L. van, Schols, S.E.M., Maas, D.P.M.S.M., Atiq, F., Blijlevens, N.M.A., Brons, P.P.T., Krouwel, S., Laros-van Gorkom, B.A.P., Leebeek, F.W.G., Nieuwenhuizen, Laurens, Schoormans, S.C.M., Simons, A., Meijer, D., Heerde, W.L. van, and Schols, S.E.M.

Abstract

Item does not contain fulltext, BACKGROUND: An appropriate clinical diagnosis of von Willebrand disease (VWD) can be challenging because of a variable bleeding pattern and laboratory phenotype. Genotyping is a powerful diagnostic tool and may have an essential role in the diagnostic field of VWD. OBJECTIVES: To unravel the clinical and laboratory heterogeneity of genetically confirmed VWD type 2M patients and to investigate their relationship. METHODS: Patients with a confirmed VWD type 2M genetic variant in the A1 or A3 domain of von Willebrand factor (VWF) and normal or only slightly aberrant VWF multimers were selected from all subjects genotyped at the Radboud university medical center because of a high suspicion of VWD. Bleeding scores and laboratory results were analyzed. RESULTS: Fifty patients had a clinically relevant genetic variant in the A1 domain. Median bleeding score was 5. Compared with the nationwide Willebrand in the Netherlands study type 2 cohort, bleeding after surgery or delivery was reported more frequently and mucocutaneous bleedings less frequently. Median VWF activity/VWF antigen (VWF:Act/VWF:Ag) ratio was 0.32, whereas VWF collagen binding activity/VWF antigen (VWF:CB/VWF:Ag) ratio was 0.80. Variants in the A3 domain were only found in two patients with low to normal VWF:Act/VWF:Ag ratios (0.45, 1.03) and low VWF:CB/VWF:Ag ratios (0.45, 0.63). CONCLUSION: Genetically confirmed VWD type 2M patients have a relatively mild clinical phenotype, except for bleeding after surgery and delivery. Laboratory phenotype is variable and depends on the underlying genetic variant. Addition of genotyping to the current phenotypic characterization may improve diagnosis and classification of VWD.

Published

2022

9. Social participation is reduced in type 3 Von Willebrand disease patients and in patients with a severe bleeding phenotype

Author

Kempers, E.K., Kwawegen, C.B. van, Meris, J. de, Schols, S.E.M., Galen, K.P. van, Meijer, K, Cnossen, M.H., Bom, J.G. van der, Fijnvandraat, K., Eikenboom, J., Atiq, F., Leebeek, F.W.G., Kempers, E.K., Kwawegen, C.B. van, Meris, J. de, Schols, S.E.M., Galen, K.P. van, Meijer, K, Cnossen, M.H., Bom, J.G. van der, Fijnvandraat, K., Eikenboom, J., Atiq, F., and Leebeek, F.W.G.

Abstract

Item does not contain fulltext, INTRODUCTION: The negative impact of haemophilia on social participation is well established in previous studies, however, the impact of Von Willebrand disease (VWD) on social participation has not been studied. AIM: To compare the social participation of a large cohort of VWD patients in the Netherlands with the general Dutch population. In addition, to identify factors associated with social participation in VWD. METHODS: Patients participating in the "Willebrand in the Netherlands" study completed an extensive questionnaire on educational level, absenteeism from school or work, and occupational disabilities. RESULTS: Seven-hundred and eighty-eight VWD patients were included (mean age 38.9 years, 59.5% females), of whom 136 children < 16 years. Adult patients with type 3 VWD more often had a low educational level (52.9%) compared to type 1 (40.2%), type 2 VWD (36.8%) and the general population (36.4%) (p = .005). Moreover, in patients aged ≥16 years the days lost from school and/or work in the year prior to study inclusion differed significantly between the VWD types (p = .011). Using negative binomial regression analysis, the occurrence of bleeding episodes requiring treatment in the year preceding study inclusion was significantly associated with the number of days lost from school and/or work among patients aged ≥16 years. Multivariable logistic regression analysis showed that a higher total bleeding score, older age and presence of at least one comorbidity were significantly associated with occupational disability in patients aged ≥16 years. CONCLUSION: Our study shows that social participation was lower in type 3 VWD and VWD patients with a more severe bleeding phenotype.

Published

2022

10. Social participation is reduced in type 3 Von Willebrand disease patients and in patients with a severe bleeding phenotype

Author

Kempers, E.K., Kwawegen, C.B. van, Meris, J. de, Schols, S.E.M., Galen, K.P.M. van, Meijer, K., Cnossen, M.H., Bom, J.G. van der, Fijnvandraat, K., Eikenboom, J., Atiq, F., Leebeek, F.W.G., WiN Study Grp, Hematology, Pediatrics, Paediatric Haematology, Amsterdam Reproduction & Development (AR&D), and Real World Studies in PharmacoEpidemiology, -Genetics, -Economics and -Therapy (PEGET)

Subjects

Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, social participation, Adolescent, IMPACT, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], cross-sectional studies, Hemorrhage, von Willebrand Disease, Type 3, von Willebrand Disease, Type 1, CLASSIFICATION, absenteeism, educational status, QUALITY-OF-LIFE, hemic and lymphatic diseases, von Willebrand Factor, Humans, ADULT PATIENTS, JOINT BLEEDS, Genetics (clinical), HEMOPHILIA, Hematology, General Medicine, bleeding, von Willebrand Diseases, Phenotype, MODERATE, Female

Abstract

Contains fulltext : 248809.pdf (Publisher’s version ) (Open Access) INTRODUCTION: The negative impact of haemophilia on social participation is well established in previous studies, however, the impact of Von Willebrand disease (VWD) on social participation has not been studied. AIM: To compare the social participation of a large cohort of VWD patients in the Netherlands with the general Dutch population. In addition, to identify factors associated with social participation in VWD. METHODS: Patients participating in the "Willebrand in the Netherlands" study completed an extensive questionnaire on educational level, absenteeism from school or work, and occupational disabilities. RESULTS: Seven-hundred and eighty-eight VWD patients were included (mean age 38.9 years, 59.5% females), of whom 136 children

Published

2021

11. Pseudomyxoma Peritonei A Rare Abdominal Tumor

Author

IQBAL, N, primary, SHAHID, K, additional, SHOAIB, M, additional, ATIQ, F, additional, BOKHARI, S T, additional, and SIDDIQUE, K, additional

Published

2021

12. Hysteroscopy - 3 Years’ Experience at a Teaching Hospital

Author

AMBREEN, A, primary, SIDDIQI, K J, additional, ATIQ, F, additional, and IQBAL, N, additional

Published

2021

13. BMI is an important determinant of VWF and FVIII levels and bleeding phenotype in patients with von Willebrand disease

Author

Atiq, Ferdows, Fijnvandraat, Karin, van Galen, Karin P. M., Laros-van Gorkom, Britta A. P., Meijer, Karina, de Meris, Joke, Coppens, Michiel, Mauser-Bunschoten, Eveline P., Cnossen, Marjon H., van der Bom, Johanna G., Eikenboom, Jeroen, Leebeek, Frank W. G., Coppens, M., Kors, A., Zweegman, S., de Meris, J., Goverde, G. J., Jonkers, M. H., Dors, N., Nijziel, M. R., Nieuwenhuizen, L., Meijer, K., Tamminga, R. Y. J., van der LindenHagaZiekenhuis, P. W., Ypma, P. F., Eikenboom, H. C. J., van der Bom, J. G., Smiers, F. J. W., Granzen, B., Hamulyák, K., Brons, P., Laros‐van Gorkom, B. A. P., Leebeek, F. W. G., Cnossen, M. H., Atiq, F., Mauser-Bunschoten, E. P., van Galen, K. P. M., Hematology, Pediatrics, Paediatric Haematology, ACS - Pulmonary hypertension & thrombosis, Vascular Medicine, ARD - Amsterdam Reproduction and Development, VU University medical center, Kindergeneeskunde, MUMC+: MA Medische Staf Kindergeneeskunde (9), RS: FHML non-thematic output, and Real World Studies in PharmacoEpidemiology, -Genetics, -Economics and -Therapy (PEGET)

Subjects

Male, medicine.medical_specialty, Letter, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], E–Only Articles, Hemorrhage, von Willebrand Disease, Type 2, von Willebrand Disease, Type 1, Body Mass Index, Text mining, Internal medicine, von Willebrand Factor, Correspondence, Von Willebrand disease, Medicine, Humans, In patient, Hematology, Factor VIII, business.industry, Middle Aged, Blood coagulation factors, medicine.disease, Phenotype, Immunology, Female, business, Body mass index

Abstract

Contains fulltext : 208376.pdf (Publisher’s version ) (Open Access)

Published

2019

14. Sports participation and physical activity in patients with von Willebrand disease

Author

Atiq, F., Mauser-Bunschoten, E.P., Eikenboom, J., Galen, K.P.M. van, Meijer, K., Meris, J. de, Cnossen, M.H., Beckers, E.A.M., Laros-van Gorkom, B.A.P., Nieuwenhuizen, L., Bom, J.G. van der, Fijnvandraat, K., Leebeek, F.W.G., WiN Study Grp, MUMC+: MA Hematologie (9), RS: Carim - B01 Blood proteins & engineering, RS: CARIM - R1.01 - Blood proteins & engineering, Real World Studies in PharmacoEpidemiology, -Genetics, -Economics and -Therapy (PEGET), Hematology, Pediatrics, Landsteiner Laboratory, Paediatric Haematology, and ARD - Amsterdam Reproduction and Development

Subjects

Male, Activities of daily living, Health Status, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], Hemorrhage/prevention & control, physical activity, CHILDREN, 030204 cardiovascular system & hematology, RECOMMENDATIONS, Body Mass Index, 0302 clinical medicine, Quality of life, QUALITY-OF-LIFE, Surveys and Questionnaires, ADOLESCENTS, Activities of Daily Living, Genetics(clinical), ADULT PATIENTS, Young adult, Genetics (clinical), HEMOPHILIA, Von Willebrand disease, General Medicine, Hematology, Fear, Middle Aged, von Willebrand Diseases, Original Article, Female, sports, Adult, medicine.medical_specialty, Adolescent, Physical activity, Hemorrhage, Haemophilia, CLASSIFICATION, 03 medical and health sciences, Young Adult, All institutes and research themes of the Radboud University Medical Center, Internal medicine, medicine, Journal Article, Humans, In patient, Exercise, business.industry, medicine.disease, Logistic Models, quality of life, MODERATE, ORIGINAL ARTICLES, business, Body mass index, von Willebrand Diseases/pathology, 030215 immunology

Abstract

Introduction Patients with bleeding disorders may experience limitations in sports participation and physical activity. Several studies on sports participation have been performed in haemophilia patients, but studies in patients with von Willebrand disease (VWD) are lacking. Aim We assessed the sports participation and physical activity of a large cohort of VWD patients. Methods Patients were included from the "WiN study." All patients completed a questionnaire on sports participation, physical activity, quality of life and bleeding symptoms (Tosetto bleeding score). Results From the 798 included patients, 474 had type 1, 301 type 2 and 23 type 3 VWD. The mean age was 39 +/- 20 (standard deviation) years. Five hundred and fifty-two patients (69.3%) participated in various types of sports. Type 3 VWD patients more often did not participate in sports due to fear of bleeding and physical impairment, respectively, OR = 13.24 (95% CI: 2.45-71.53) and OR = 5.90 (95% CI: 1.77-19.72). Patients who did not participate in sports due to physical impairment had a higher bleeding score item for joint bleeds 1.0 (+/- 1.6) vs 0.5 (+/- 1.1) (P = 0.036). Patients with type 3 VWD and patients with a higher bleeding score frequently had severe limitations during daily activities, respectively, OR = 9.84 (95% CI: 2.83-34.24) and OR = 1.08 (95% CI: 1.04-1.12). Conclusion The majority of VWD patients participated in sports. Patients with type 3 VWD, a history of joint bleeds and a more severe bleeding phenotype frequently experienced limitations in sports participation and physical activities during daily life.

Published

2018

15. Criteria for low von Willebrand factor diagnosis and risk score to predict future bleeding

Author

Atiq, F. (Ferdows), Wuijster, E. (Esmee), Maat, M.P.M. (Moniek) de, Kruip, M.J.H.A. (Marieke), Cnossen, M.H. (Marjon), Leebeek, F.W.G. (Frank), Atiq, F. (Ferdows), Wuijster, E. (Esmee), Maat, M.P.M. (Moniek) de, Kruip, M.J.H.A. (Marieke), Cnossen, M.H. (Marjon), and Leebeek, F.W.G. (Frank)

Abstract

Background: Important diagnostic and clinical aspects of moderately reduced von Willebrand factor (VWF) levels are still unknown. There is no clear evidence which cutoff value (0.50 vs 0.60 IU/ml) should be used to diagnose “low VWF.” Also, the incidence of bleeding after the diagnosis has been made, and risk factors for bleeding are unknown yet. Objectives: To investigate the incidence of postsurgical bleeding, postpartum hemorrhage (PPH), and traumatic and spontaneous bleeding after low VWF diagnosis, and to develop a risk score to predict future bleeding. Methods: We performed a cohort study in patients with historically lowest VWF levels of 0.31 to 0.60 IU/ml. Clinical data of patients were retrospectively collected. Results: We included 439 patients with low VWF. During a follow-up of 6.3 ± 3.7 years, 259 surgical procedures, 81 deliveries, and 109 spontaneous and traumatic bleeding episodes were reported. The incidence of postsurgical bleeding was 2.7%, whereas 10% of deliveries was complicated by PPH. Overall, 65 patients (14.8%) had bleeding requiring treatment, which was not different between patients with historically lowest VWF levels of 0.31–0.50 and 0.51–0.60 IU/ml (p =.154). Age <18 years, abnormal bleeding score at diagnosis, and being referred for bleeding symptoms at the time of diagnosis were independent risk factors for bleeding during follow-up, and therefore included in the risk score. Conclusions: The cutoff value of low VWF diagnosis should be set at 0.60 IU/ml. Furthermo

Published

2020

16. 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

17. BMI is an important determinant of VWF and FVIII levels and bleeding phenotype in patients with von Willebrand disease

Author

Atiq, F., Fijnvandraat, K., Galen, K.P. van, Laros-van Gorkom, B.A.P., Meijer, K, Meris, J. de, Coppens, M., Mauser-Bunschoten, E.P., Cnossen, M.H., Bom, J.G. van der, Eikenboom, J., Leebeek, F.W.G., Atiq, F., Fijnvandraat, K., Galen, K.P. van, Laros-van Gorkom, B.A.P., Meijer, K, Meris, J. de, Coppens, M., Mauser-Bunschoten, E.P., Cnossen, M.H., Bom, J.G. van der, Eikenboom, J., and Leebeek, F.W.G.

Abstract

Contains fulltext : 208376.pdf (publisher's version ) (Open Access)

Published

2019

18. How I manage severe von Willebrand disease

Author

Leebeek, F.W.G. (Frank), Atiq, F. (Ferdows), Leebeek, F.W.G. (Frank), and Atiq, F. (Ferdows)

Abstract

Von Willebrand disease (VWD) is the most common inherited bleeding disorder. Most patients with mild and moderate VWD can be treated effectively with desmopressin. The management of severe VWD patients, mostly affected by type 2 and type 3 disease, can be challenging. In this article we review the current diagnosis and treatment of severe VWD patients. We will also discuss the management of severe VWD patients in specific situations, such as pregnancy, delivery, patients developing alloantibodies against von Willebrand factor and VWD patients with recurrent gastrointestinal bleeding. Moreover, we review emerging treatments that may be applied in future management of patients with severe VWD.

Published

2019

19. Comorbidities associated with higher von Willebrand factor (VWF) levels may explain the age-related increase of VWF in von Willebrand disease

Author

Atiq, F., Meijer, K., Eikenboom, J., Fijnvandraat, K., Mauser-Bunschoten, E.P., Galen, K.P. van, Nijziel, M.R., Ypma, P.F., Meris, J. de, Laros-van Gorkom, B.A.P., Bom, J.G. van der, Maat, M.P. de, Cnossen, M.H., Leebeek, F.W., Atiq, F., Meijer, K., Eikenboom, J., Fijnvandraat, K., Mauser-Bunschoten, E.P., Galen, K.P. van, Nijziel, M.R., Ypma, P.F., Meris, J. de, Laros-van Gorkom, B.A.P., Bom, J.G. van der, Maat, M.P. de, Cnossen, M.H., and Leebeek, F.W.

Abstract

Contains fulltext : 193336.pdf (publisher's version ) (Open Access), Some comorbidities, such as hypertension, are associated with higher von Willebrand factor (VWF) levels in the general population. No studies have been conducted to assess this association in patients with von Willebrand disease (VWD). Therefore, we studied this association in patients with type 1 (n = 333) and type 2 (n = 203) VWD from the 'WiN" study. VWF antigen (VWF:Ag) was higher in type 1 VWD patients with hypertension [difference: 0.23 iu/ml, 95% confidence interval (CI): 0.11-0.35], diabetes mellitus (0.11 iu/ml, 95% CI: -0.02 to 0.23), cancer (0.14 iu/ml, 95% CI: 0.03-0.25) and thyroid dysfunction (0.14 iu/ml, 95% CI: 0.03-0.26) than in patients without these comorbidities (all corrected for age, sex and blood group). Similar results were observed for VWF collagen binding capacity (VWF:CB), VWF activity as measured by the VWF monoclonal antibody assay (VWF:Ab) and factor VIII (FVIII) coagulant activity (FVIII:C). In type 1 VWD, age was associated with higher VWF:Ag (0.03 iu/ml; 95% CI: 0.01-0.04), VWF:CB (0.02 iu/ml; 95% CI: 0.00-0.04), VWF:Ab (0.04 iu/ml; 95% CI: 0.02-0.06) and FVIII:C (0.03 iu/ml; 95% CI: 0.01-0.06) per decade increase. After adjustment for relevant comorbidities, these associations were no longer significant. Despite the higher VWF and FVIII levels, type 1 VWD patients with comorbidities had more bleeding episodes, particularly during surgery. There was no association between comorbidities and VWF/FVIII levels or bleeding phenotype in type 2 VWD patients. In conclusion, comorbidities are associated with higher VWF and FVIII levels in type 1 VWD and may explain the age-related increase of VWF and FVIII levels.

Published

2018

20. Sports participation and physical activity in patients with von Willebrand disease

Author

Atiq, F. (Ferdows), Mauser-Bunschoten, E.P. (Eveline), Eikenboom, J.C.J. (Jeroen), Galen, K.P.M. van, Meijer, K. (Karina), Meris, J. (Joke) de, Cnossen, M.H. (Marjon), Beckers, E.A.M. (Erick A. M.), Laros-Van Gorkom, B.A.P. (Britta), Nieuwenhuizen, L. (Laurens), Bom, J.G. (Anske) van der, Fijnvandraat, K., Leebeek, F.W.G. (Frank), Atiq, F. (Ferdows), Mauser-Bunschoten, E.P. (Eveline), Eikenboom, J.C.J. (Jeroen), Galen, K.P.M. van, Meijer, K. (Karina), Meris, J. (Joke) de, Cnossen, M.H. (Marjon), Beckers, E.A.M. (Erick A. M.), Laros-Van Gorkom, B.A.P. (Britta), Nieuwenhuizen, L. (Laurens), Bom, J.G. (Anske) van der, Fijnvandraat, K., and Leebeek, F.W.G. (Frank)

Abstract

Introduction: Patients with bleeding disorders may experience limitations in sports participation and physical activity. Several studies on sports participation have been performed in haemophilia patients, but studies in patients with von Willebrand disease (VWD) are lacking. Aim: We assessed the sports participation and physical activity of a large cohort of VWD patients. Methods: Patients were included from the “WiN study.

Published

2018

21. Converting cyclosporine A from intravenous to oral administration in hematopoietic stem cell transplant recipients and the role of azole antifungals

Author

Atiq, F. (Ferdows), Hameli, E. (Edon), Broers, A.E.C. (Annoek), Doorduijn, J.K. (Jeanette), Gelder, T. (Teun) van, Andrews, L.M. (Louise), Koch, B.C.P. (Birgit), Versmissen, J. (Jorie), Winter, B.C.M. (Brenda) de, Atiq, F. (Ferdows), Hameli, E. (Edon), Broers, A.E.C. (Annoek), Doorduijn, J.K. (Jeanette), Gelder, T. (Teun) van, Andrews, L.M. (Louise), Koch, B.C.P. (Birgit), Versmissen, J. (Jorie), and Winter, B.C.M. (Brenda) de

Abstract

Purpose: Cyclosporine A (CsA) is the most widely used immunosuppressive agent after a hematopoietic stem cell transplantation (HSCT). Although recommendations for CsA dose conversion from intravenous to oral administration differ from 1:1 to 1:3, most studies did not consider the role of azole antifungals as an important confounder. Therefore, we assess the optimal conversion rate of CsA from intravenous to oral administration in HSCT recipients, taking into account the concomitant use of azole antifungals. Methods: We retrospectively included patients from a large database of 483 patients who underwent a HSCT and received intravenous CsA as part of the conditioning regimen and peritransplant immunosuppression. All patients were converted from intravenous to oral administration in a 1:1 conversion rate. We collected for each patient three CsA trough concentrations during intravenous and oral administration, directly before and after conversion to oral administration. Results: We included 71 patients; 50 patients co-treated with fluconazole, 10 with voriconazole, and 11 without azole co-medication. In patients with voriconazole, the dose-corrected CsA concentration (CsA concentration divided by CsA dosage) was not different between intravenous and oral administration (2.6% difference, p = 0.754), suggesting a CsA oral bioavailability of nearly 100%. In patients with fluconazole and without azole co-medication, the dose-corrected CsA concentration was respectively 21.5% (p < 0.001) and 25.2% (p = 0.069) lower during oral administration. Conclusions: In patients with voriconazole, CsA should be converted 1:1 from intravenous to oral administration. In patients with fluconazole and without azole co-medication, a 1:1.3 substitution is advised to prevent subtherapeutic CsA concentrations.

Published

2018

22. Comorbidities associated with higher von Willebrand factor (VWF) levels may explain the age-related increase of VWF in von Willebrand disease

Author

Atiq, F. (Ferdows), Meijer, K. (Karina), Eikenboom, J.C.J. (Jeroen), Fijnvandraat, K., Mauser-Bunschoten, E.P. (Eveline), Galen, K.P.M. van, Nijziel, M.R. (Marten), Ypma, P.F. (Paula), Meris, J. (Joke) de, Laros-Van Gorkom, B.A.P. (Britta), Bom, J.G. (Anske) van der, Maat, M.P.M. (Moniek) de, Cnossen, M.H. (Marjon), Leebeek, F.W.G. (Frank), Atiq, F. (Ferdows), Meijer, K. (Karina), Eikenboom, J.C.J. (Jeroen), Fijnvandraat, K., Mauser-Bunschoten, E.P. (Eveline), Galen, K.P.M. van, Nijziel, M.R. (Marten), Ypma, P.F. (Paula), Meris, J. (Joke) de, Laros-Van Gorkom, B.A.P. (Britta), Bom, J.G. (Anske) van der, Maat, M.P.M. (Moniek) de, Cnossen, M.H. (Marjon), and Leebeek, F.W.G. (Frank)

Abstract

Some comorbidities, such as hypertension, are associated with higher von Willebrand factor (VWF) levels in the general population. No studies have been conducted to assess this association in patients with von Willebrand disease (VWD). Therefore, we studied this association in patients with type 1 (n = 333) and type 2 (n = 203) VWD from the ‘WiN” study. VWF antigen (VWF:Ag) was higher in type 1 VWD patients with hypertension [difference: 0·23 iu/ml, 95% confidence interval (CI): 0·11–0·35], diabetes mellitus (0·11 iu/ml, 95% CI: −0·02 to 0·23), cancer (0·14 iu/ml, 95% CI: 0·03–0·25) and thyroid dysfunction (0·14 iu/ml, 95% CI: 0·03–0·26) than in patients without these comorbidities (all corrected for age, sex and blood group). Similar results were observed for VWF collagen binding capacity (VWF:CB), VWF activity as measured by the VWF monoclonal antibody assay (VWF:Ab) and factor VIII (FVIII) coagulant activity (FVIII:C). In type 1 VWD, age was associated with higher VWF:Ag (0·03 iu/ml; 95% CI: 0·01–0·04), VWF:CB (0·02 iu/ml; 95% CI: 0·00–0·04), VWF:Ab (0·04 iu/ml; 95% CI: 0·02–0·06) and FVIII:C (0·03 iu/ml; 95% CI: 0·01–0·06) per decade increase. After adjustment for relevant comorbidities, these associations were no longer significant. Despite the higher VWF and FVIII levels, type 1 VWD patients with comorbidities had more bleeding episodes, particularly during surgery. There was no association between comorbidities and VWF/FVIII levels or bleeding phenotype in type 2 VWD patients. In conclusion, comorbidities are associated with higher VWF and FVIII levels in type 1 VWD and may explain the age-related increase of VWF and FVIII levels.

Published

2018

23. Genetic variants, thrombocytopenia, and clinical phenotype of type 2B von Willebrand disease: a median 16-year follow-up study

Author

van Kwawegen, Calvin B., Atiq, Ferdows, Endenburg, Dara, Fijnvandraat, Karin, van Galen, Karin P.M., Cnossen, Marjon H., Schols, Saskia E.M., Kruip, Marieke J.H.A., van Heerde, Waander L., de Meris, Joke, van der Bom, Johanna G., Eikenboom, Jeroen, Meijer, Karina, Leebeek, Frank W.G., Fijnvandraat, K., Coppens, M., Kors, A., Zweegman, S., de Meris, J., Goverde, G.J., Jonkers, M.H., Dors, N., Nijziel, M.R., Nieuwenhuizen, L., Meijer, K., Tamminga, R.Y.J., van der Linden, P.W., Ypma, P.F., Eikenboom, H.C.J., van der Bom, J.G., Smiers, F.J.W., Granzen, B., Hamulyák, K., Brons, P., Laros-van Gorkom, B.A.P., Schols, S.E.M., Leebeek, F.W.G., Cnossen, M.H., Boender, J., Atiq, F., van Kwawegen, C.B., Mauser-Bunschoten, E.P., and van Galen, K.P.M.

Abstract

Type 2B von Willebrand disease (VWD) is a bleeding disorder caused by gain-of-function variants in the VWFgene. The laboratory and clinical phenotype of type 2B VWD is heterogeneous.

Published

2024

24. A clinically relevant pharmacokinetic interaction between cyclosporine and imatinib

Author

Atiq, F. (Ferdows), Broers, A.E.C. (Annoek), Andrews, L.M. (Louise), Doorduijn, J.K. (Jeanette), Koch, B.C.P. (Birgit), Gelder, T. (Teun) van, Versmissen, J. (Jorie), Atiq, F. (Ferdows), Broers, A.E.C. (Annoek), Andrews, L.M. (Louise), Doorduijn, J.K. (Jeanette), Koch, B.C.P. (Birgit), Gelder, T. (Teun) van, and Versmissen, J. (Jorie)

Abstract

Purpose: Cyclosporine A (CsA) and imatinib are both CYP3A4 and P-glycoprotein substrates. Concomitant use after hematopoietic stem cell transplantation (HSCT) for chronic myeloid leukemia (CML) or Philadelphia chromosome-positive (Ph+) acute lymphatic leukemia (ALL) may therefore result in a pharmacokinetic interaction. Although case reports and a recent small study in children indeed suggested there is a relevant pharmacokinetic interaction, a larger study in adults is lacking. In this study, we assessed the presence and extent of this interaction in patients with CML or Ph+ ALL undergoing HSCT. Methods: From a large database containing data of all patients receiving HSCT in our center between 2005 and 2015, we selected 16 patients using this drug combination. The average dose-corrected CsA concentration was calculated before and after initiation of imatinib. Results: The average dose-corrected CsA concentration increased during imatinib use in all patients, on average by 94 % (p < 0.001). Based on measured drug conc

Published

2016

25. No Accumulation of a high Prophylactic Nadroparin dosage in Patients with moderate renal insufficiency assessed by peak Anti-XA activity

Author

Atiq, F., primary, van den Bemt, P.M.L.A., additional, Leebeek, F.W.G., additional, van Gelder, T., additional, and Versmissen, J., additional

Published

2015

26. Fetal hypophysis as the main source of serum TSH in fetal rat

Author

Pic, P., Bouquin, J. P., and El Atiq, F.

Published

1986

27. Warsaw Breakage Syndrome associated DDX11 helicase resolves G-quadruplex structures to support sister chromatid cohesion

Author

Janne J. M. van Schie, Atiq Faramarz, Jesper A. Balk, Grant S. Stewart, Erika Cantelli, Anneke B. Oostra, Martin A. Rooimans, Joanna L. Parish, Cynthia de Almeida Estéves, Katja Dumic, Ingeborg Barisic, Karin E. M. Diderich, Marjon A. van Slegtenhorst, Mohammad Mahtab, Francesca M. Pisani, Hein te Riele, Najim Ameziane, Rob M. F. Wolthuis, and Job de Lange

Subjects

Science

Abstract

WABS patient derived cells display loss of sister chromatid cohesion. Here the authors by analyzing WABS patient derived cells, reveal a role of the DDX11 helicase in resolving G-Quadruplex structures to support sister chromatid cohesion.

Published

2020

28. Non-redundant roles in sister chromatid cohesion of the DNA helicase DDX11 and the SMC3 acetyl transferases ESCO1 and ESCO2.

Author

Atiq Faramarz, Jesper A Balk, Janne J M van Schie, Anneke B Oostra, Cherien A Ghandour, Martin A Rooimans, Rob M F Wolthuis, and Job de Lange

Subjects

Medicine, Science

Abstract

In a process linked to DNA replication, duplicated chromosomes are entrapped in large, circular cohesin complexes and functional sister chromatid cohesion (SCC) is established by acetylation of the SMC3 cohesin subunit. Roberts Syndrome (RBS) and Warsaw Breakage Syndrome (WABS) are rare human developmental syndromes that are characterized by defective SCC. RBS is caused by mutations in the SMC3 acetyltransferase ESCO2, whereas mutations in the DNA helicase DDX11 lead to WABS. We found that WABS-derived cells predominantly rely on ESCO2, not ESCO1, for residual SCC, growth and survival. Reciprocally, RBS-derived cells depend on DDX11 to maintain low levels of SCC. Synthetic lethality between DDX11 and ESCO2 correlated with a prolonged delay in mitosis, and was rescued by knockdown of the cohesin remover WAPL. Rescue experiments using human or mouse cDNAs revealed that DDX11, ESCO1 and ESCO2 act on different but related aspects of SCC establishment. Furthermore, a DNA binding DDX11 mutant failed to correct SCC in WABS cells and DDX11 deficiency reduced replication fork speed. We propose that DDX11, ESCO1 and ESCO2 control different fractions of cohesin that are spatially and mechanistically separated.

Published

2020

29. Cell polarity of the insulin-like growth factor system in human intestinal epithelial cells. Unique apical sorting of insulin-like growth factor binding protein-6 in differentiated human colon cancer cells.

Author

Remacle-Bonnet, M, primary, Garrouste, F, additional, el Atiq, F, additional, Marvaldi, J, additional, and Pommier, G, additional

Published

1995

30. Forskolin stimulates cAMP production and the onset of the functional differentiation in the fetal rat thyroid in vitro

Author

Pic, P., primary, Michel‐Bechet, M., additional, el Atiq, F., additional, and Athouel‐Haon, A. M., additional

Published

1986

31. The molecular background of quantitative defects of von Willebrand factor.

Author

Atiq F

Abstract

Competing Interests: Declaration of competing interests F.A. received research support from CSL Behring, Takeda, Octapharma, and Sobi.

Published

2024

32. Patient-reported data on the severity of Von Willebrand disease.

Author

van Kwawegen CB, Fijnvandraat K, Kruip MJHA, de Meris J, Schols SEM, Meijer K, van der Bom JG, Cnossen MH, van Galen KPM, Atiq F, Eikenboom J, and Leebeek FWG

Abstract

Introduction: The severity of Von Willebrand disease (VWD) is currently based on laboratory phenotype. However, little is known about the severity of the patient's experience with the disease. The most recent VWD guidelines highlight the need for patient-reported outcomes (PROs) in VWD., Aim: The study aimed to investigate the patient-perspective on VWD severity and to identify key factors that determine the severity of disease experienced by patients., Materials and Methods: Patients participated in a nationwide cross-sectional study on VWD in the Netherlands (WiN-study). Patients filled in a questionnaire containing questions on the experienced severity of VWD (4-point scale), bleeding score (BS) and quality of life (QoL)., Results: We included 736 patients, median age of 41.0 years (IQR 23.0-55.0) and 59.5% were women. A total of 443 had type 1, 269 type 2 and 24 type 3 VWD. Self-reported severity of VWD was categorized as severe (n = 52), moderate (n = 171), mild (n = 393) or negligible (n = 120). Classification by historically lowest FVIII:C levels < 0.20 IU/mL as a proxy for severe VWD aligned with patient-reported severity classification with a 72% accuracy. Type 3 VWD (OR = 4.02, 95%CI: 1.72-9.45), higher BS (OR = 1.09, 95%CI: 1.06-1.11), female sex (OR = 1.36, 95%CI: 1.01-1.83), haemostatic treatment in the year preceding study inclusion (OR = 1.53, 95%CI: 1.10-2.13) and historically lowest VWF:Act levels (OR = 0.26, 95%CI: 0.07-1.00) were independent determinants of patient-reported severity., Conclusion: This study shows that patient-reported data provide novel insights into the determinants of experienced disease severity. Our findings highlight the need for studies on PROs with validated questionnaires to assess the burden of VWD., (© 2024 The Author(s). Haemophilia published by John Wiley & Sons Ltd.)

Published

2024

33. R1205H (Vicenza) causes conformational changes in the von Willebrand factor D'D3 domains and enhances von Willebrand factor binding to clearance receptors LRP1 and SR-AI.

Author

Atiq F, Rawley O, O'Sullivan JM, Özbil M, Doherty D, Cooke N, Terraube V, Chion A, Amin A, Hulshof AM, Baci B, Byrne C, Aburawi HE, Lillicrap D, and O'Donnell JS

Subjects

Animals, Humans, Mice, Macrophages metabolism, Mice, Inbred C57BL, Mice, Knockout, Protein Conformation, Scavenger Receptors, Class B, Low Density Lipoprotein Receptor-Related Protein-1 metabolism, Protein Binding, Protein Domains, von Willebrand Factor metabolism

Abstract

Background: von Willebrand factor (VWF)-R1205H variant (Vicenza) results in markedly enhanced VWF clearance in humans that has been shown to be largely macrophage-mediated. However, the biological mechanisms underlying this enhanced clearance remain poorly understood., Objectives: This study aimed to investigate the roles of (i) specific VWF domains and (ii) different macrophage receptors in regulating enhanced VWF-R1205H clearance., Methods: In vivo clearance of full-length and truncated wild-type (WT)-VWF and VWF with R1205 substitutions was investigated in VWF -/- mice. Plate-binding assays were employed to characterize VWF binding to purified scavenger receptor class A member 1 (SR-AI), low-density lipoprotein receptor-related protein-1 (LRP1) cluster II or cluster IV receptors, and macrophage galactose-type lectin., Results: In full-length VWF missing the A1 domain, introduction of R1205H led to significantly enhanced clearance in VWF -/- mice compared with WT-VWF missing the A1 domain. Importantly, R1205H in a truncated VWF-D'D3 fragment also triggered increased clearance compared with WT-VWF-D'D3. Additional in vivo studies demonstrated that VWF-R1205K (which preserves the positive charge at 1205) exhibited normal clearance, whereas VWF-R1205E (which results in loss of the positive charge) caused significantly enhanced clearance, pinpointing the importance of the positive charge at VWF-R1205. In vitro plate-binding studies confirmed increased VWF-R1205H interaction with SR-AI compared with WT-VWF. Furthermore, significantly enhanced VWF-R1205H binding to LRP1 cluster IV (P < .001) and less marked enhanced binding to LRP1 cluster II (P = .034) was observed. In contrast, VWF-R1205H and WT-VWF demonstrated no difference in binding affinity to macrophage galactose-type lectin., Conclusion: Disruption of the positive charge at amino acid R1205 causes conformational changes in the VWF-D'D3 domains and triggers enhanced LRP1-mediated and SR-AI-mediated clearance., Competing Interests: Declaration of competing interests J.S.O.D. has served on the speaker’s bureau for Baxter, Bayer, Novo Nordisk, Sobi, Boehringer Ingelheim, Leo Pharma, Takeda, and Octapharma. He has also served on the advisory boards of Baxter, Sobi, Bayer, OctapharmaCSL Behring, Daiichi Sankyo, Boehringer Ingelheim, Takeda, and Pfizer. J.S.O.D. has also received research grant funding awards from 3M, Baxter, Bayer, Pfizer, Shire, Takeda, and Novo Nordisk. F.A. received research support from CSL Behring, Takeda, Octapharma, and Sobi. D.L. has received research support from BioMarin, CSL Behring, and Sanofi; he has acted in an advisory role for BioMarin, CSL Behring, Novo Nordisk, Pfizer, Sanofi, and Takeda. The remaining authors declare no competing financial interests., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

34. The aptamer BT200 blocks interaction of K1405-K1408 in the VWF-A1 domain with macrophage LRP1.

Author

Chion A, Byrne C, Atiq F, Doherty D, Aguila S, Fazavana J, Lopes P, Karampini E, Amin A, Preston RJS, Baker RI, McKinnon TAJ, Zhu S, Gilbert JC, Emsley J, Jilma B, and O'Donnell JS

Subjects

Humans, Animals, HEK293 Cells, Mice, Protein Binding, Protein Domains, von Willebrand Factor metabolism, von Willebrand Factor genetics, Aptamers, Nucleotide pharmacology, Aptamers, Nucleotide metabolism, Low Density Lipoprotein Receptor-Related Protein-1 metabolism, Low Density Lipoprotein Receptor-Related Protein-1 genetics, Macrophages metabolism, Macrophages drug effects

Abstract

Abstract: Rondaptivon pegol (previously BT200) is a pegylated RNA aptamer that binds to the A1 domain of von Willebrand factor (VWF). Recent clinical trials demonstrated that BT200 significantly increased plasma VWF-factor VIII levels by attenuating VWF clearance. The biological mechanism(s) through which BT200 attenuates in vivo clearance of VWF has not been defined. We hypothesized that BT200 interaction with the VWF-A1 domain may increase plasma VWF levels by attenuating macrophage-mediated clearance. We observed that full-length and VWF-A1A2A3 binding to macrophages and VWF-A1 domain binding to lipoprotein receptor-related protein 1 (LRP1) cluster II and cluster IV were concentration-dependently inhibited by BT200. Additionally, full-length VWF binding to LRP1 expressed on HEK293T (HEK-LRP1) cells was also inhibited by BT200. Importantly, BT200 interacts with the VWF-A1 domain in proximity to a conserved cluster of 4 lysine residues (K1405, K1406, K1407, and K1408). Alanine mutagenesis of this K1405-K1408 cluster (VWF-4A) significantly (P < .001) attenuated binding of VWF to both LRP1 clusters II and IV. Furthermore, in vivo clearance of VWF-4A was significantly (P < .001) reduced than that of wild-type VWF. BT200 did not significantly inhibit binding of VWF-4A to LRP1 cluster IV or HEK-LRP1 cells. Finally, BT200 interaction with the VWF-A1 domain also inhibited binding to macrophage galactose lectin and the SR-AI scavenger receptor. Collectively, our findings demonstrate that BT200 prolongs VWF half-life by attenuating macrophage-mediated clearance and specifically the interaction of K1405-K1408 in the VWF-A1 domain with macrophage LRP1. These data support the concept that targeted inhibition of VWF clearance pathways represents a novel therapeutic approach for von Willebrand disease and hemophilia A., (© 2024 American Society of Hematology. Published by Elsevier Inc. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2024

35. Novel functions for von Willebrand factor.

Author

Atiq F and O'Donnell JS

Subjects

Humans, Animals, Ligands, Protein Binding, Wound Healing, Hemostasis physiology, Inflammation metabolism, von Willebrand Factor metabolism, von Willebrand Factor chemistry

Abstract

Abstract: For many years, it has been known that von Willebrand factor (VWF) interacts with factor VIII, collagen, and platelets. In addition, the key roles played by VWF in regulating normal hemostasis have been well defined. However, accumulating recent evidence has shown that VWF can interact with a diverse array of other novel ligands. To date, over 60 different binding partners have been described, with interactions mapped to specific VWF domains in some cases. Although the biological significance of these VWF-binding interactions has not been fully elucidated, recent studies have identified some of these novel ligands as regulators of various aspects of VWF biology, including biosynthesis, proteolysis, and clearance. Conversely, VWF binding has been shown to directly affect the functional properties for some of its ligands. In keeping with those observations, exciting new roles for VWF in regulating a series of nonhemostatic biological functions have also emerged. These include inflammation, wound healing, angiogenesis, and bone metabolism. Finally, recent evidence supports the hypothesis that the nonhemostatic functions of VWF directly contribute to pathogenic mechanisms in a variety of diverse diseases including sepsis, malaria, sickle cell disease, and liver disease. In this manuscript, we review the accumulating data regarding novel ligand interactions for VWF and critically assess how these interactions may affect cellular biology. In addition, we consider the evidence that nonhemostatic VWF functions may contribute to the pathogenesis of human diseases beyond thrombosis and bleeding., (© 2024 American Society of Hematology. Published by Elsevier Inc. All rights are reserved, including those for text and data mining, AI training, and similar technologies.)

Published

2024

36. Low von Willebrand factor-unraveling an enigma wrapped in a conundrum.

Author

O'Donnell JS, Baker RI, and Atiq F

Abstract

The 2021 ASH ISTH NHF WFH guidelines recommendation that patients with von Willebrand factor (VWF) levels of 30 to 50 IU/dL and an increased bleeding phenotype be categorized as type 1 von Willebrand disease (VWD) rather than Low VWF has proved controversial. However, in support of that decision, recent data have demonstrated that individuals with partial quantitative VWF deficiency exhibit an age-dependent evolving phenotype and confirmed that Low VWF represents a subgroup within heterogeneous type 1 VWD. Nonetheless, type 1 VWD heterogeneity continues to pose significant diagnostic challenges. In this Forum article, we address outstanding issues critical to preventing the inappropriate overdiagnosis of type 1 VWD while maximizing access to healthcare and minimizing diagnostic delays. In addition, we propose an algorithm for type 1 VWD diagnosis. This algorithm pays special attention to individuals with plasma VWF levels in the 30 to 50 IU/dL range who have no or minimal bleeding history and have not yet been exposed to significant hemostatic challenges., Competing Interests: Declaration of competing interests J.S.O.D. has served on the speaker’s bureau for Baxter, Bayer, Novo Nordisk, Sobi, Boehringer Ingelheim, Leo Pharma, Takeda, and Octapharma. He has also served on the advisory boards of Baxter, Sobi, Bayer, OctapharmaCSL Behring, Daiichi Sankyo, Boehringer Ingelheim, Takeda, and Pfizer. J.S.O.D. has also received research grant funding awards from 3M, Baxter, Bayer, Pfizer, Shire, Takeda, and Novo Nordisk. R.I.B.’s institution has received research support/clinical trial funding from Bayer, Takeda, Pfizer, Daiichi Sankyo, CSL Behring, Roche, Amgen, Astra Zeneca, Abbvie, Sanofi, Acerta Pharma, Jansen-Cileg, Bristol-Myers Squibb, Boehringer Ingelheim, Werfen, and Technoclone unrelated to the current study. F.A. received research support from CSL Behring, Takeda, Octapharma, and Sobi., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

37. Variant mapping using mass spectrometry-based proteotyping as a diagnostic tool in von Willebrand disease.

Author

Kreft IC, van Duijl TT, van Kwawegen C, Atiq F, Phan W, Schuller MBP, Boon-Spijker M, van der Zwaan C, Meijer AB, Hoogendijk AJ, Bierings R, Eikenboom JCJ, Leebeek FWG, and van den Biggelaar M

Subjects

Humans, Netherlands, Phenotype, Female, Factor VIII genetics, Factor VIII analysis, Factor VIII metabolism, Mass Spectrometry, Male, Predictive Value of Tests, von Willebrand Factor genetics, von Willebrand Factor analysis, von Willebrand Factor metabolism, von Willebrand Diseases diagnosis, von Willebrand Diseases blood, von Willebrand Diseases genetics, Proteomics methods

Abstract

Background: von Willebrand disease (VWD) is the most common inherited bleeding disorder, characterized by either partial or complete von Willebrand factor (VWF) deficiency or by the occurrence of VWF proteoforms of altered functionality. The gene encoding VWF is highly polymorphic, giving rise to a variety of proteoforms with varying plasma concentrations and clinical significance., Objectives: To address this complexity, we translated genomic variation in VWF to corresponding VWF proteoforms circulating in blood., Methods: VWF was characterized in VWD patients (n = 64) participating in the Willebrand in the Netherlands study by conventional laboratory testing, DNA sequencing and complementary discovery, and targeted mass spectrometry-based plasma proteomic strategies., Results: Unbiased plasma profiling combined with immune enrichment of VWF verified VWF and its binding partner factor VIII as key determinants of VWD and revealed a remarkable heterogeneity in VWF amino acid sequence coverage among patients. Subsequent VWF proteotyping enabled identification of both polymorphisms (eg, p.Thr789Ala, p.Gln852Arg, and p.Thr1381Ala), as well as pathogenic variants (n = 16) along with their corresponding canonical sequences. Targeted proteomics using stable isotope-labeled peptides confirmed unbiased proteotyping for 5 selected variants and suggested differential proteoform quantities in plasma. The variant-to-wild-type peptide ratio was determined in 6 type 2B patients heterozygous for p.Arg1306Trp, confirming the relatively low proteoform concentration of the pathogenic variant. The elevated VWF propeptide/VWF ratio indicated increased clearance of specific VWF proteoforms., Conclusion: This study highlights how VWF proteotyping from plasma could be the first step to bridge the gap between genotyping and functional testing in VWD., Competing Interests: Declaration of competing interests There are no competing interests to disclose., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

38. Type 1 VWD classification revisited: novel insights from combined analysis of the LoVIC and WiN studies.

Author

Atiq F, Blok R, van Kwawegen CB, Doherty D, Lavin M, van der Bom JG, O'Connell NM, de Meris J, Ryan K, Schols SEM, Byrne M, Heubel-Moenen FCJI, van Galen KPM, Preston RJS, Cnossen MH, Fijnvandraat K, Baker RI, Meijer K, James P, Di Paola J, Eikenboom J, Leebeek FWG, and O'Donnell JS

Subjects

Humans, von Willebrand Factor genetics, Netherlands epidemiology, Hemorrhage pathology, von Willebrand Disease, Type 1 diagnosis, von Willebrand Diseases diagnosis, von Willebrand Diseases genetics

Abstract

Abstract: There is significant ongoing debate regarding type 1 von Willebrand disease (VWD) defintion. Previous guidelines recommended patients with von Willebrand factor (VWF) levels <30 IU/dL be diagnosed type 1 VWD, whereas patients with significant bleeding and VWF levels from 30 to 50 IU/dL be diagnosed with low VWF. To elucidate the relationship between type 1 VWD and low VWF in the context of age-induced increases in VWF levels, we combined data sets from 2 national cohort studies: 162 patients with low VWF from the Low VWF in Ireland Cohort (LoVIC) and 403 patients with type 1 VWD from the Willebrand in The Netherlands (WiN) studies. In 47% of type 1 VWD participants, VWF levels remained <30 IU/dL despite increasing age. Conversely, VWF levels increased to the low VWF range (30-50 IU/dL) in 30% and normalized (>50 IU/dL) in 23% of type 1 VWD cases. Crucially, absolute VWF antigen (VWF:Ag) levels and increase of VWF:Ag per year overlapped between low VWF and normalized type 1 VWD participants. Moreover, multiple regression analysis demonstrated that VWF:Ag levels in low VWF and normalized type 1 VWD patients would not have been different had they been diagnosed at the same age (β = 0.00; 95% confidence interval, -0.03 to 0.04). Consistently, no difference was found in the prevalence of VWF sequence variants; factor VIII activity/VWF:Ag or VWF propeptide/VWF:Ag ratios; or desmopressin responses between low VWF and normalized type 1 VWD patients. In conclusion, our findings demonstrate that low VWF does not constitute a discrete clinical or pathological entity. Rather, it is part of an age-dependent type 1 VWD evolving phenotype. Collectively, these data have important implications for future VWD classification criteria., (© 2024 American Society of Hematology. Published by Elsevier Inc. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2024

39. VWF-ADAMTS13 axis dysfunction in children with sickle cell disease treated with hydroxycarbamide vs blood transfusion.

Author

Fogarty H, Ahmad A, Atiq F, Doherty D, Ward S, Karampini E, Rehill A, Leon G, Byrne C, Geoghegan R, Conroy H, Byrne M, Budde U, Schneppenheim S, Sheehan C, Ngwenya N, Baker RI, Preston RJS, Tuohy E, McMahon C, and O'Donnell JS

Subjects

Humans, Child, von Willebrand Factor metabolism, Hemolysis, Hydroxyurea therapeutic use, Blood Transfusion, ADAMTS13 Protein, Anemia, Sickle Cell drug therapy, Vascular Diseases, Hemostatics

Abstract

Previous studies have reported elevated von Willebrand factor (VWF) levels in patients with sickle cell disease (SCD) and demonstrated a key role for the VWF-ADAMTS13 axis in the pathobiology of SCD vaso-occlusion. Although blood transfusion is the gold standard for stroke prevention in SCD, the biological mechanisms underpinning its improved efficacy compared with hydroxycarbamide are not fully understood. We hypothesized that the improved efficacy of blood transfusion might relate to differences in VWF-ADAMTS13 axis dysfunction. In total, 180 children with a confirmed diagnosis of SCD (hemoglobin SS) on hydroxycarbamide (n = 96) or blood transfusion (n = 84) were included. Despite disease-modifying treatment, plasma VWF and VWF propeptide were elevated in a significant proportion of children with SCD (33% and 47%, respectively). Crucially, all VWF parameters were significantly higher in the hydroxycarbamide compared with the blood transfusion cohort (P < .05). Additionally, increased levels of other Weibel-Palade body-stored proteins, including factor VIII (FVIII), angiopoietin-2, and osteoprotegerin were observed, indicated ongoing endothelial cell activation. Children treated with hydroxycarbamide also had higher FVIII activity and enhanced thrombin generation compared with those in the blood transfusion cohort (P < .001). Finally, hemolysis markers strongly correlated with VWF levels (P < .001) and were significantly reduced in the blood transfusion cohort (P < .001). Cumulatively, to our knowledge, our findings demonstrate for the first time that despite treatment, ongoing dysfunction of the VWF-ADAMTS13 axis is present in a significant subgroup of pediatric patients with SCD, especially those treated with hydroxycarbamide., (© 2023 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2023

40. Desmopressin response depends on the presence and type of genetic variants in patients with type 1 and type 2 von Willebrand disease.

Author

Atiq F, Heijdra J, Snijders F, Boender J, Kempers E, van Heerde WL, Maas DPMSM, Krouwel S, Schoormans SC, de Meris J, Schols SEM, van Galen KPM, van der Bom JG, Cnossen MH, Meijer K, Fijnvandraat K, Eikenboom J, and Leebeek FWG

Subjects

Deamino Arginine Vasopressin pharmacology, Deamino Arginine Vasopressin therapeutic use, Exons, Humans, von Willebrand Factor genetics, von Willebrand Disease, Type 2 drug therapy, von Willebrand Disease, Type 2 genetics, von Willebrand Diseases genetics

Abstract

Patients with type 1 and type 2 von Willebrand disease (VWD) can be treated with desmopressin. Although a previous study has shown that the location of the causative VWF gene variant is associated with desmopressin response in type 1 VWD, the association between variants in the VWF gene and desmopressin response is not yet fully understood. Our primary aim was to compare desmopressin response in type 1 VWD patients with and without a VWF gene variant. Secondly, we investigated whether desmopressin response depends on specific VWF gene variants in type 1 and type 2 VWD. We included 250 patients from the Willebrand in the Netherlands study: 72 type 1 without a VWF gene variant, 108 type 1 with a variant, 45 type 2A, 16 type 2M, and 9 type 2N patients. VWF gene was analyzed with ion semiconductor sequencing and Multiplex Ligation-dependent Probe Amplification. Complete response to desmopressin was observed in all type 1 VWD patients without a variant, 64.3% of type 1 patients with a variant, and 31.3% of type 2 patients (P < .001). Despite a large interindividual variability in desmopressin response, patients with the same variant had comparable desmopressin responses. For instance, in 6 type 1 patients with exon 4 to 5 deletion, mean VWF activity at 1 hour after desmopressin was 0.81 IU/mL, with a coefficient of variation of 22.9%. In conclusion, all type 1 VWD patients without a VWF gene variant respond to desmopressin. In type 1 and type 2 VWD patients with a VWF variant, desmopressin response highly depends on the VWF gene variants., (© 2022 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2022

41. Desmopressin testing in von Willebrand disease: Lowering the burden.

Author

Heijdra JM, Atiq F, Al Arashi W, Kieboom Q, Wuijster E, Meijer K, Kruip MJHA, Leebeek FWG, and Cnossen MH

Abstract

Background: Individuals with von Willebrand disease (VWD) require desmopressin testing because of interindividual response differences. However, testing is burdensome, while not all patients may need extensive testing., Objectives: To provide von Willebrand factor (VWF) cutoffs that predict desmopressin nonresponse and thereby identify individuals who do not need extensive testing in a retrospective cohort. We validated these cutoffs in a prospective cohort., Patients and Methods: We included 376 patients (Type 1 VWD with VWF activity [VWF:Act] <0.30 IU/ml: n  = 112; with VWF:Act 0.30-0.50 IU/ml: n  = 206; Type 2 VWD: n  = 58; ages, 5-76 years) from January 2000 to July 2020. We collected VWF:Act and factor VIII activity (FVIII:C) at baseline and several time points after desmopressin (T1-T6). We defined response as VWF:Act and FVIII:C 0.50 IU/ml or greater at T1 and T4. We compared VWF:Act and FVIII:C distribution (historically lowest level, baseline, and T1) between responders and nonresponders and determined cutoffs discriminating between these groups. Results were validated in a group of 30 individuals., Results: All individuals with Type 1 VWD and Type 2 VWD, respectively, with baseline VWF:Act 0.34 IU/ml or greater or 0.28 IU/ml or greater were responders. In individuals with T1 VWF:Act ≥0.89 IU/ml (Type 1 VWD) or T1 VWF:Act 1.10 IU/ml or greater (Type 2 VWD), response remained at T4., Conclusion: Desmopressin testing is not needed when lowest historical VWF:Act is 0.30 IU/ml or greater. In patients with Type 1 VWD who require testing, measurements after T1 are often not needed. In patients with Type 2 VWD who require testing, we advise performing T1 and T4 measurements., (© 2022 The Authors. Research and Practice in Thrombosis and Haemostasis published by Wiley Periodicals LLC on behalf of International Society on Thrombosis and Haemostasis (ISTH).)

Published

2022

42. Platelet degranulation and bleeding phenotype in a large cohort of Von Willebrand disease patients.

Author

Swinkels M, Atiq F, Bürgisser PE, van Moort I, Meijer K, Eikenboom J, Fijnvandraat K, van Galen KPM, de Meris J, Schols SEM, van der Bom JG, Cnossen MH, Voorberg J, Leebeek FWG, Bierings R, and Jansen AJG

Subjects

Hemorrhage etiology, Humans, Phenotype, Platelet Factor 4, von Willebrand Factor genetics, von Willebrand Diseases genetics

Abstract

Von Willebrand disease (VWD) is a bleeding disorder caused by quantitative (type 1 or 3) or qualitative (type 2A/2B/2M/2N) defects of circulating von Willebrand factor (VWF). Circulating VWF levels not always fully explain bleeding phenotypes, suggesting a role for alternative factors, like platelets. Here, we investigated platelet factor 4 (PF4) in a large cohort of patients with VWD. PF4 levels were lower in type 2B and current bleeding phenotype was significantly associated with higher PF4 levels, particularly in type 1 VWD. Based on our findings we speculate that platelet degranulation and cargo release may play a role across VWD subtypes., (© 2022 The Authors. British Journal of Haematology published by British Society for Haematology and John Wiley & Sons Ltd.)

Published

2022

43. Social participation is reduced in type 3 Von Willebrand disease patients and in patients with a severe bleeding phenotype.

Author

Kempers EK, van Kwawegen CB, de Meris J, Schols SEM, van Galen KPM, Meijer K, Cnossen MH, van der Bom JG, Fijnvandraat K, Eikenboom J, Atiq F, and Leebeek FWG

Subjects

Adolescent, Adult, Female, Hemorrhage complications, Humans, Male, Phenotype, Social Participation, von Willebrand Factor genetics, von Willebrand Disease, Type 1 complications, von Willebrand Disease, Type 3 complications, von Willebrand Diseases complications

Abstract

Introduction: The negative impact of haemophilia on social participation is well established in previous studies, however, the impact of Von Willebrand disease (VWD) on social participation has not been studied., Aim: To compare the social participation of a large cohort of VWD patients in the Netherlands with the general Dutch population. In addition, to identify factors associated with social participation in VWD., Methods: Patients participating in the "Willebrand in the Netherlands" study completed an extensive questionnaire on educational level, absenteeism from school or work, and occupational disabilities., Results: Seven-hundred and eighty-eight VWD patients were included (mean age 38.9 years, 59.5% females), of whom 136 children < 16 years. Adult patients with type 3 VWD more often had a low educational level (52.9%) compared to type 1 (40.2%), type 2 VWD (36.8%) and the general population (36.4%) (p = .005). Moreover, in patients aged ≥16 years the days lost from school and/or work in the year prior to study inclusion differed significantly between the VWD types (p = .011). Using negative binomial regression analysis, the occurrence of bleeding episodes requiring treatment in the year preceding study inclusion was significantly associated with the number of days lost from school and/or work among patients aged ≥16 years. Multivariable logistic regression analysis showed that a higher total bleeding score, older age and presence of at least one comorbidity were significantly associated with occupational disability in patients aged ≥16 years., Conclusion: Our study shows that social participation was lower in type 3 VWD and VWD patients with a more severe bleeding phenotype., (© 2021 The Authors. Haemophilia published by John Wiley & Sons Ltd.)

Published

2022

44. Von Willebrand disease type 2M: Correlation between genotype and phenotype.

Author

Maas DPMSM, Atiq F, Blijlevens NMA, Brons PPT, Krouwel S, Laros-van Gorkom BAP, Leebeek FWG, Nieuwenhuizen L, Schoormans SCM, Simons A, Meijer D, van Heerde WL, and Schols SEM

Subjects

Genotype, Humans, Phenotype, von Willebrand Factor chemistry, von Willebrand Factor genetics, von Willebrand Disease, Type 2 diagnosis, von Willebrand Disease, Type 2 genetics, von Willebrand Diseases diagnosis, von Willebrand Diseases genetics

Abstract

Background: An appropriate clinical diagnosis of von Willebrand disease (VWD) can be challenging because of a variable bleeding pattern and laboratory phenotype. Genotyping is a powerful diagnostic tool and may have an essential role in the diagnostic field of VWD., Objectives: To unravel the clinical and laboratory heterogeneity of genetically confirmed VWD type 2M patients and to investigate their relationship., Methods: Patients with a confirmed VWD type 2M genetic variant in the A1 or A3 domain of von Willebrand factor (VWF) and normal or only slightly aberrant VWF multimers were selected from all subjects genotyped at the Radboud university medical center because of a high suspicion of VWD. Bleeding scores and laboratory results were analyzed., Results: Fifty patients had a clinically relevant genetic variant in the A1 domain. Median bleeding score was 5. Compared with the nationwide Willebrand in the Netherlands study type 2 cohort, bleeding after surgery or delivery was reported more frequently and mucocutaneous bleedings less frequently. Median VWF activity/VWF antigen (VWF:Act/VWF:Ag) ratio was 0.32, whereas VWF collagen binding activity/VWF antigen (VWF:CB/VWF:Ag) ratio was 0.80. Variants in the A3 domain were only found in two patients with low to normal VWF:Act/VWF:Ag ratios (0.45, 1.03) and low VWF:CB/VWF:Ag ratios (0.45, 0.63)., Conclusion: Genetically confirmed VWD type 2M patients have a relatively mild clinical phenotype, except for bleeding after surgery and delivery. Laboratory phenotype is variable and depends on the underlying genetic variant. Addition of genotyping to the current phenotypic characterization may improve diagnosis and classification of VWD., (© 2021 The Authors. Journal of Thrombosis and Haemostasis published by Wiley Periodicals LLC on behalf of International Society on Thrombosis and Haemostasis.)

Published

2022

45. Quantitative 3D microscopy highlights altered von Willebrand factor α-granule storage in patients with von Willebrand disease with distinct pathogenic mechanisms.

Author

Swinkels M, Atiq F, Bürgisser PE, Slotman JA, Houtsmuller AB, de Heus C, Klumperman J, Leebeek FWG, Voorberg J, Jansen AJG, and Bierings R

Abstract

Background: Platelets play a key role in hemostasis through plug formation and secretion of their granule contents at sites of endothelial injury. Defects in von Willebrand factor (VWF), a platelet α-granule protein, are implicated in von Willebrand disease (VWD), and may lead to defective platelet adhesion and/or aggregation. Studying VWF quantity and subcellular localization may help us better understand the pathophysiology of VWD., Objective: Quantitative analysis of the platelet α-granule compartment and VWF storage in healthy individuals and VWD patients., Patients/methods: Structured illumination microscopy (SIM) was used to study VWF content and organization in platelets of healthy individuals and patients with VWD in combination with established techniques., Results: SIM capably quantified clear morphological and granular changes in platelets stimulated with proteinase-activated receptor 1 (PAR-1) activating peptide and revealed a large intra- and interdonor variability in VWF-positive object numbers within healthy resting platelets, similar to variation in secreted protein acidic and rich in cysteine (SPARC). We subsequently characterized VWD platelets to identify changes in the α-granule compartment of patients with different VWF defects, and were able to stratify two patients with type 3 VWD rising from different pathological mechanisms. We further analyzed VWF storage in α-granules of a patient with homozygous p .C1190R using electron microscopy and found discrepant VWF levels and different degrees of multimerization in platelets of patients with heterozygous p .C1190 in comparison to VWF in plasma., Conclusions: Our findings highlight the utility of quantitative imaging approaches in assessing platelet granule content, which may help to better understand VWF storage in α-granules and to gain new insights in the etiology of VWD., (© 2021 The Authors. Research and Practice in Thrombosis and Haemostasis published by Wiley Periodicals LLC on behalf of International Society on Thrombosis and Haemostasis (ISTH).)

Published

2021

46. Endothelial Dysfunction, Atherosclerosis, and Increase of von Willebrand Factor and Factor VIII: A Randomized Controlled Trial in Swine.

Author

Atiq F, van de Wouw J, Sorop O, Heinonen I, de Maat MPM, Merkus D, Duncker DJ, and Leebeek FWG

Subjects

Animals, Blood Coagulation Tests, Hypercholesterolemia, Swine, Atherosclerosis metabolism, Atherosclerosis pathology, Biomarkers metabolism, Diabetes Mellitus, Experimental metabolism, Diabetes Mellitus, Experimental pathology, Endothelium, Vascular pathology, Factor VIII metabolism, Swine, Miniature immunology, von Willebrand Factor metabolism

Abstract

It is well known that high von Willebrand factor (VWF) and factor VIII (FVIII) levels are associated with an increased risk of cardiovascular disease. It is still debated whether VWF and FVIII are biomarkers of endothelial dysfunction and atherosclerosis or whether they have a direct causative role. Therefore, we aimed to unravel the pathophysiological pathways of increased VWF and FVIII levels associated with cardiovascular risk factors. First, we performed a randomized controlled trial in 34 Göttingen miniswine. Diabetes mellitus (DM) was induced with streptozotocin and hypercholesterolemia (HC) via a high-fat diet in 18 swine (DM + HC), while 16 healthy swine served as controls. After 5 months of follow-up, FVIII activity (FVIII:C) was significantly higher in DM + HC swine (5.85 IU/mL [5.00-6.81]) compared with controls (4.57 [3.76-5.40], p  = 0.010), whereas VWF antigen (VWF:Ag) was similar (respectively 0.34 IU/mL [0.28-0.39] vs. 0.34 [0.31-0.38], p  = 0.644). DM + HC swine had no endothelial dysfunction or atherosclerosis during this short-term follow-up. Subsequently, we performed a long-term (15 months) longitudinal cohort study in 10 Landrace-Yorkshire swine, in five of which HC and in five combined DM + HC were induced. VWF:Ag was higher at 15 months compared with 9 months in HC (0.37 [0.32-0.42] vs. 0.27 [0.23-0.40], p  = 0.042) and DM + HC (0.33 [0.32-0.37] vs. 0.25 [0.24-0.33], p  = 0.042). Both long-term groups had endothelial dysfunction compared with controls and atherosclerosis after 15 months. In conclusion, short-term hyperglycemia and dyslipidemia increase FVIII, independent of VWF. Long-term DM and HC increase VWF via endothelial dysfunction and atherosclerosis. Therefore, VWF seems to be a biomarker for advanced cardiovascular disease., Competing Interests: F.A. received the CSL Behring-Professor Heimburger Award 2018 and a travel grant from Sobi. F.W.G.L. received research support from CSL Behring and Shire/Takeda for performing the WiN study; is a consultant for uniQure, Novo Nordisk, and Shire/Takeda, the fees of which go to the institution; and has received a travel grant from Sobi. He is also a DSMB member for a study by Roche., (Thieme. All rights reserved.)

Published

2021

47. Criteria for low von Willebrand factor diagnosis and risk score to predict future bleeding.

Author

Atiq F, Wuijster E, de Maat MPM, Kruip MJHA, Cnossen MH, and Leebeek FWG

Subjects

Adolescent, Cohort Studies, Female, Humans, Retrospective Studies, Risk Factors, von Willebrand Factor, von Willebrand Disease, Type 1, von Willebrand Diseases diagnosis, von Willebrand Diseases epidemiology

Abstract

Background: Important diagnostic and clinical aspects of moderately reduced von Willebrand factor (VWF) levels are still unknown. There is no clear evidence which cutoff value (0.50 vs 0.60 IU/ml) should be used to diagnose "low VWF." Also, the incidence of bleeding after the diagnosis has been made, and risk factors for bleeding are unknown yet., Objectives: To investigate the incidence of postsurgical bleeding, postpartum hemorrhage (PPH), and traumatic and spontaneous bleeding after low VWF diagnosis, and to develop a risk score to predict future bleeding., Methods: We performed a cohort study in patients with historically lowest VWF levels of 0.31 to 0.60 IU/ml. Clinical data of patients were retrospectively collected., Results: We included 439 patients with low VWF. During a follow-up of 6.3 ± 3.7 years, 259 surgical procedures, 81 deliveries, and 109 spontaneous and traumatic bleeding episodes were reported. The incidence of postsurgical bleeding was 2.7%, whereas 10% of deliveries was complicated by PPH. Overall, 65 patients (14.8%) had bleeding requiring treatment, which was not different between patients with historically lowest VWF levels of 0.31-0.50 and 0.51-0.60 IU/ml (p = .154). Age <18 years, abnormal bleeding score at diagnosis, and being referred for bleeding symptoms at the time of diagnosis were independent risk factors for bleeding during follow-up, and therefore included in the risk score., Conclusions: The cutoff value of low VWF diagnosis should be set at 0.60 IU/ml. Furthermore, a risk score is developed to identify individuals with a high risk for bleeding after low VWF diagnosis., (© 2021 The Authors. Journal of Thrombosis and Haemostasis published by Wiley Periodicals LLC on behalf of International Society on Thrombosis and Haemostasis.)

Published

2021

48. Von Willebrand Factor Multimer Densitometric Analysis: Validation of the Clinical Accuracy and Clinical Implications in Von Willebrand Disease.

Author

Boender J, Atiq F, Cnossen MH, van der Bom JG, Fijnvandraat K, de Meris J, de Maat MPM, van Galen KPM, Laros-van Gorkom BAP, Meijer K, Eikenboom J, and Leebeek FWG

Abstract

Von Willebrand factor (VWF) multimer analysis is important in the classification of von Willebrand disease (VWD). Current visual VWF multimer analysis is time consuming and inaccurate in detecting subtle changes in multimer patterns. Although VWF multimer densitometric analysis may be useful, the accuracy needs further investigation before it can be widely applied. In this study we aimed to validate VWF multimer densitometric analysis in a large cohort of VWD patients and to identify patient characteristics associated with densitometric outcomes. Patients were included from the Willebrand in the Netherlands (WiN) study, in which a bleeding score (BS) was obtained, and blood was drawn. For multimer analysis, citrated blood was separated on an agarose gel and visualized by Western blotting. IMAGEJ was used to generate densitometric images and medium-large VWF multimer index was calculated. We included 560 VWD patients: 328 type 1, 211 type 2, and 21 type 3 patients. Medium-large VWF multimer index performed excellent in distinguishing visually classified normal VWF multimers from reduced high-molecular-weight (HMW) multimers (area under the curve [AUC]: 0.96 [0.94-0.98], P < 0.001), normal multimers from absence of HMW multimers (AUC 1.00 [1.00-1.00], P < 0.001), and type 2A and 2B from type 2M and 2N (AUC: 0.96 [0.94-0.99], P < 0.001). Additionally, higher medium-large VWF multimer index was associated with lower BS in type 1 VWD: β = -7.6 (-13.0 to -2.1), P = 0.007, adjusted for confounders. Densitometric analysis of VWF multimers had an excellent accuracy compared with visual multimer analysis and may contribute to a better understanding of the clinical features such as the bleeding phenotype of VWD patients., Competing Interests: JB started working at Sobi after finishing this research project. FA received the CSL Behring-professor Heimburger Award 2018 and a travel grant from Sobi. MHC has received grants from governmental research institutes, such as the Dutch Research institute (NWO), ZonMW, Innovation fund, NWO-Dutch Research Agenda, and unrestricted investigator-initiated research grants as well as educational and travel funding from various companies over the years (Pfizer, Baxter/Baxalta/Shire, Bayer Schering Pharma, CSL Behring, Sobi, Novo Nordisk, Novartis, and Nordic Pharma); he served as a member on steering boards of Roche and Bayer. All grants, awards, and fees go to the Erasmus MC as an institution. MPMM has received travel support and speaker fees from Roche Diagnostics, Sysmex, Siemens, and Werfen. The institution of KF has received unrestricted research grants from CSL Behring, Sobi, and NovoNordisk, and her institution received consultancy fees from Grifols, Takeda, Novo Nordisk, and Roche. KM received research support from Bayer, Sanquin, and Pfizer; speaker fees from Bayer, Sanquin, Boehringer Ingelheim, BMS, and Aspen; and consulting fees from Uniqure, of which all fees go to the institution. BAPLG has received unrestricted educational grants from Baxter and CSL Behring. JE received research support from CSL Behring, and he has been a teacher on educational activities of Roche. KPMG received unrestricted research support from CSL Behring and Bayer and speakers fee from Takeda. JGB has been a teacher on educational activities of Bayer and received consultancy fees from Novo Nordisk, paid to the Leiden University Medical Center. FWGL received research support from CSL Behring and Shire/Takeda for performing the Willebrand in the Netherlands (WiN) study and uniQure for a study not related to this article, and he is a consultant for uniQure, Novo Nordisk, BioMarin, and Shire/Takeda, of which the fees go to the institution, and he received a travel grant from Sobi. He is also a data safety monitoring board member for a study by Roche. JM has no conflicts of interest to disclose., (Copyright © 2021 the Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the European Hematology Association.)

Published

2021

49. Silent cerebral infarcts in patients with sickle cell disease: a systematic review and meta-analysis.

Author

Houwing ME, Grohssteiner RL, Dremmen MHG, Atiq F, Bramer WM, de Pagter APJ, Zwaan CM, White TJH, Vernooij MW, and Cnossen MH

Subjects

Adolescent, Adult, Anemia, Sickle Cell diagnosis, Anemia, Sickle Cell psychology, Asymptomatic Diseases psychology, Cerebral Infarction complications, Cerebral Infarction diagnosis, Cerebral Infarction psychology, Child, Cognition physiology, Female, Humans, Magnetic Resonance Imaging, Male, Prevalence, Prospective Studies, Risk Factors, Stroke complications, Stroke diagnosis, Stroke epidemiology, Stroke psychology, Anemia, Sickle Cell complications, Anemia, Sickle Cell epidemiology, Asymptomatic Diseases epidemiology, Cerebral Infarction epidemiology

Abstract

Background and Purpose: Silent cerebral infarcts (SCIs) are the most common neurological complication in children and adults with sickle cell disease (SCD). In this systematic review, we provide an overview of studies that have detected SCIs in patients with SCD by cerebral magnetic resonance imaging (MRI). We focus on the frequency of SCIs, the risk factors involved in their development and their clinical consequences., Methods: The databases of Embase, MEDLINE ALL via Ovid, Web of Science Core Collection, Cochrane Central Register of Trials via Wiley and Google Scholar were searched from inception to June 1, 2019., Results: The search yielded 651 results of which 69 studies met the eligibility criteria. The prevalence of SCIs in patients with SCD ranges from 5.6 to 80.6% with most studies reported in the 20 to 50% range. The pooled prevalence of SCIs in HbSS and HbSβ 0 SCD patients is 29.5%. SCIs occur more often in patients with the HbSS and HbSβ 0 genotype in comparison with other SCD genotypes, as SCIs are found in 9.2% of HbSC and HbSβ + patients. Control subjects showed a mean pooled prevalence of SCIs of 9.8%. Data from included studies showed a statistically significant association between increasing mean age of the study population and mean SCI prevalence. Thirty-three studies examined the risk factors for SCIs. The majority of the risk factors show no clear association with prevalence, since more or less equal numbers of studies give evidence for and against the causal association., Conclusions: This systematic review and meta-analysis shows SCIs are common in patients with SCD. No clear risk factors for their development were identified. Larger, prospective and controlled clinical, neuropsychological and neuroimaging studies are needed to understand how SCD and SCIs affect cognition.

Published

2020

50. Ex vivo Improvement of a von Willebrand Disease Type 2A Phenotype Using an Allele-Specific Small-Interfering RNA.

Author

de Jong A, Dirven RJ, Boender J, Atiq F, Anvar SY, Leebeek FWG, van Vlijmen BJM, and Eikenboom J

Subjects

Alleles, Amino Acid Substitution, Endothelial Cells drug effects, Endothelial Cells metabolism, HEK293 Cells, Humans, Mutation, Missense, RNA, Small Interfering genetics, Transfection, von Willebrand Disease, Type 2 genetics, von Willebrand Factor analysis, von Willebrand Factor antagonists & inhibitors, Polymorphism, Single Nucleotide, RNA Interference, RNA, Small Interfering therapeutic use, von Willebrand Disease, Type 2 drug therapy, von Willebrand Factor genetics

Abstract

Von Willebrand disease (VWD) is the most common inherited bleeding disorder and is mainly caused by dominant-negative mutations in the multimeric protein von Willebrand factor (VWF). These mutations may either result in quantitative or qualitative defects in VWF. VWF is an endothelial protein that is secreted to the circulation upon endothelial activation. Once secreted, VWF multimers bind platelets and chaperone coagulation factor VIII in the circulation. Treatment of VWD focuses on increasing VWF plasma levels, but production and secretion of mutant VWF remain uninterrupted. Presence of circulating mutant VWF might, however, still affect normal hemostasis or functionalities of VWF beyond hemostasis. We hypothesized that inhibition of the production of mutant VWF improves the function of VWF overall and ameliorates VWD phenotypes. We previously proposed the use of allele-specific small-interfering RNAs (siRNAs) that target frequent VWF single nucleotide polymorphisms to inhibit mutant VWF . The aim of this study is to prove the functionality of these allele-specific siRNAs in endothelial colony-forming cells (ECFCs). We isolated ECFCs from a VWD type 2A patient with an intracellular multimerization defect, reduced VWF collagen binding, and a defective processing of proVWF to VWF. After transfection of an allele-specific siRNA that specifically inhibited expression of mutant VWF, we showed amelioration of the laboratory phenotype, with normalization of the VWF collagen binding, improvement in VWF multimers, and enhanced VWF processing. Altogether, we prove that allele-specific inhibition of the production of mutant VWF by siRNAs is a promising therapeutic strategy to improve VWD phenotypes., Competing Interests: J.B. received research funding from CSL Behring and is an employee of Sobi. F.A. received research funding from CSL Behring and a travel grant from Sobi. F.W.G.L received research funding from CSL Behring, Takeda/Shire, and uniQure. He is member of a DSMB for Roche. He is consultant for Takeda, Biomarin, and uniQure of which fees go to the institution. J.E. received research funding from CSL Behring. J.E. reports grants from Landsteiner Foundation for Blood Transfusion Research, during the conduct of the study.other authors declare no conflicts of interest., (The Author(s). This is an open access article published by Thieme under the terms of the Creative Commons Attribution-NonDerivative-NonCommercial-License, permitting copying and reproduction so long as the original work is given appropriate credit. Contents may not be used for commercial purposes, or adapted, remixed, transformed or built upon. (https://creativecommons.org/licenses/by-nc-nd/4.0/).)

Published

2020