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4. Founder mutations in hypertrophic cardiomyopathy patients in the Netherlands*

Author

Christiaans, I., primary, Nannenberg, E.A., additional, Dooijes, D., additional, Jongbloed, R.J.E., additional, Michels, M., additional, Postema, P.G., additional, Majoor-Krakauer, D., additional, van den Wijngaard, A., additional, Mannens, M.M.A.M., additional, van Tintelen, J.P., additional, van Langen, I.M., additional, and Wilde, A.A.M., additional

Published
2014
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6. A Large-Scale Full GBA1 Gene Screening in Parkinson's Disease in the Netherlands

Author

den Heijer, J.M., Cullen, V.C., Quadri, M. (Marialuisa), Schmitz, A., Hilt, D.C., Lansbury, P., Berendse, H.W. (Henk W.), van de Berg, W.D.J., Bie, R.M.A. (Rob) de, Boertien, J.M., Boon, A.J.W. (Agnita), Contarino, M.F., Hilten, J.J. (Jacobus) van, Hoff, J.I., van Mierlo, T., Munts, A.G., Plas, A.A. (Anton) van der, Ponsen, M.M., Baas, F. (Frank), Majoor-Krakauer, D, Bonifati, V. (Vincenzo), van de Laar, T., Groeneveld, G.J. (Geert Jan), den Heijer, J.M., Cullen, V.C., Quadri, M. (Marialuisa), Schmitz, A., Hilt, D.C., Lansbury, P., Berendse, H.W. (Henk W.), van de Berg, W.D.J., Bie, R.M.A. (Rob) de, Boertien, J.M., Boon, A.J.W. (Agnita), Contarino, M.F., Hilten, J.J. (Jacobus) van, Hoff, J.I., van Mierlo, T., Munts, A.G., Plas, A.A. (Anton) van der, Ponsen, M.M., Baas, F. (Frank), Majoor-Krakauer, D, Bonifati, V. (Vincenzo), van de Laar, T., and Groeneveld, G.J. (Geert Jan)

Abstract

Background: The most common genetic risk factor for Parkinson’s disease known is a damaging variant in the GBA1 gene. The entire GBA1 gene has rarely been studied in a large cohort from a single population. The objective of this study was to assess the entire GBA1 gene in Parkinson’s disease from a single large population. Methods: The GBA1 gene was assessed in 3402 Dutch Parkinson’s disease patients using nextgeneration sequencing. Frequencies were compared with Dutch controls (n = 655). Family history of Parkinson’s disease was compared in carriers and noncarriers. Results: Fifteen percent of patients had a GBA1 nonsynonymous variant (including missense, frameshift, and recombinant alleles), compared with 6.4% of co

Published
2020
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13. Distress in partners of individuals diagnosed with or at high risk of developing tumors due to rare hereditary cancer syndromes

Author

Lammens, C.R.M., Bleiker, E.M.A., Verhoef, S., Ausems, M.G.E.M., Majoor-Krakauer, D., Sijmons, R.H., Hes, F.J., Gomez-Garcia, E.B., Os, T.A.M. van, Spruijt, L., Luijt, R.B. van der, Ouweland, A.M.W. van den, Ruijs, M.W.G., Gundy, C., Nagtegaal, T., Aaronson, N.K., Guided Treatment in Optimal Selected Cancer Patients (GUTS), Human genetics, CCA - Quality of life, Klinische Psychologie (Psychologie, FMG), Faculteit der Geneeskunde, Human Genetics, Faculty of Economic and Social Sciences and Solvay Business School, International Relations and Mobility, Clinical sciences, Medical Genetics, Klinische Genetica, Humane Biologie, RS: GROW - School for Oncology and Reproduction, and Clinical Genetics

Subjects
psychosocial impact, LI-FRAUMENI-SYNDROME, DEVELOPING BREAST/OVARIAN CANCER, Hereditary cancer and cancer-related syndromes [ONCOL 1], SOCIAL CONSTRAINTS, distress, P53 MUTATIONS, Experimental and Cognitive Psychology, HEALTH SURVEY, CARRIERS, Li-Fraumeni syndrome (LFS), cancer worries, Psychiatry and Mental health, SDG 3 - Good Health and Well-being, quality of life, FAMILIAL ADENOMATOUS POLYPOSIS, oncology, VONHIPPEL-LINDAU DISEASE, BREAST-CANCER, partners, Von Hippel-Lindau disease (VHL), PSYCHOLOGICAL DISTRESS
Abstract

Contains fulltext : 95821.pdf (Publisher’s version ) (Closed access) OBJECTIVE: Li Fraumeni syndrome (LFS) and Von Hippel-Lindau disease (VHL) are two rare hereditary tumor syndromes, characterized by a high risk of developing multiple tumors at various sites and ages for which preventive and treatment options are limited. For partners, it may be difficult to deal with the on-going threat of tumors in both their spouse and children. Therefore, this study aims to evaluate the prevalence of and factors associated with psychological distress among partners of individuals with or at high risk of LFS or VHL. METHODS: As part of a nationwide, cross-sectional study, partners of individuals diagnosed with or at high risk of LFS or VHL were invited to complete a self-report questionnaire assessing distress, worries, and health-related quality of life. RESULTS: Fifty-five (58%) of those high-risk individuals with a partner consented to having their partner approached for the study. In total, 50 partners (91%) completed the questionnaire, of whom 28% reported clinically relevant levels of syndrome-related distress. Levels of distress and worries of the partners and their high-risk spouse were significantly correlated. Younger age and a lack of social support were also associated significantly with heightened levels of distress and worries. The majority of partners (76%) believed that professional psychosocial support should be routinely offered to them. CONCLUSIONS: Approximately one-quarter of the partners exhibit clinically relevant levels of distress that warrant psychological support. The distress levels of the 'patient' could potentially be used to identify partners at risk of developing clinically relevant levels of distress.

Published
2011

14. Erratum

Author

Hes, F. J., Van der Luijt, R. B., Janssen, A. L.W., Zewald, R. A., De Jong, G. J., Lenders, J. W., Links, T. P., Luyten, G. P.M., Sijmons, R. H., Eussen, H. J., Halley, D. J.J., Lips, C. J.M., Pearson, P. L., van den Ouweland, A. M.W., Majoor-Krakauer, D. F., Clinical sciences, Medical Genetics, and Geology

Subjects
genetics, Genetics(clinical)
Published
2008

15. The clinical and pathological phenotype of C9ORF72 hexanucleotide repeat expansions.

Author

Simon-Sanchez, J., Dopper, E.G., Cohn-Hokke, P.E., Hukema, R.K., Nicolaou, N., Seelaar, H., Graaf, J.R.A. de, Koning, I. de, Schoor, N.M. van, Deeg, D.J.G., Smits, M., Raaphorst, J., Berg, L.H. van den, Schelhaas, H.J., Die-Smulders, C.E.M. de, Majoor-Krakauer, D., Rozemuller, A.J., Willemsen, R., Pijnenburg, Y.A.L., Heutink, P., Swieten, J.C. van, Simon-Sanchez, J., Dopper, E.G., Cohn-Hokke, P.E., Hukema, R.K., Nicolaou, N., Seelaar, H., Graaf, J.R.A. de, Koning, I. de, Schoor, N.M. van, Deeg, D.J.G., Smits, M., Raaphorst, J., Berg, L.H. van den, Schelhaas, H.J., Die-Smulders, C.E.M. de, Majoor-Krakauer, D., Rozemuller, A.J., Willemsen, R., Pijnenburg, Y.A.L., Heutink, P., and Swieten, J.C. van

Abstract

01 maart 2012, Item does not contain fulltext, There is increasing evidence that frontotemporal dementia and amyotrophic lateral sclerosis are part of a disease continuum. Recently, a hexanucleotide repeat expansion in C9orf72 was identified as a major cause of both sporadic and familial frontotemporal dementia and amyotrophic lateral sclerosis. The aim of this study was to investigate clinical and neuropathological characteristics of hexanucleotide repeat expansions in C9orf72 in a large cohort of Dutch patients with frontotemporal dementia. Repeat expansions were successfully determined in a cohort of 353 patients with sporadic or familial frontotemporal dementia with or without amyotrophic lateral sclerosis, and 522 neurologically normal controls. Immunohistochemistry was performed in a series of 10 brains from patients carrying expanded repeats using a panel of antibodies. In addition, the presence of RNA containing GGGGCC repeats in paraffin-embedded sections of post-mortem brain tissue was investigated using fluorescence in situ hybridization with a locked nucleic acid probe targeting the GGGGCC repeat. Hexanucleotide repeat expansions in C9orf72 were found in 37 patients with familial (28.7%) and five with sporadic frontotemporal dementia (2.2%). The mean age at onset was 56.9 +/- 8.3 years (range 39-76), and disease duration 7.6 +/- 4.6 years (range 1-22). The clinical phenotype of these patients varied between the behavioural variant of frontotemporal dementia (n = 34) and primary progressive aphasia (n = 8), with concomitant amyotrophic lateral sclerosis in seven patients. Predominant temporal atrophy on neuroimaging was present in 13 of 32 patients. Pathological examination of the 10 brains from patients carrying expanded repeats revealed frontotemporal lobar degeneration with neuronal transactive response DNA binding protein-positive inclusions of variable type, size and morphology in all brains. Fluorescence in situ hybridization analysis of brain material from patients with the repeat expansion, a

Published
2012

16. Presence of ATM protein and residual kinase activity correlates with the phenotype in ataxia-telangiectasia: a genotype-phenotype study.

Author

Verhagen, M.M.M., Last, J.I., Hogervorst, F.B.L., Smeets, D.F.C.M., Roeleveld, N., Verheijen, F., Catsman-Berrevoets, C.E., Wulffraat, N.M., Cobben, J.M., Hiel, J., Brunt, E.R., Peeters, E.A., Gomez Garcia, E.B., Knaap, M.S. van der, Lincke, C.R., Laan, L.A.E.M., Tijssen, M.P.W., Rijn, M.A. van, Majoor-Krakauer, D., Visser, M. de, Veer, L.J. van 't, Kleijer, W.J., Warrenburg, B.P.C. van de, Warris, A., Groot, I.J.M. de, Groot, R. de, Broeks, A., Preijers, F.W., Kremer, B., Weemaes, C.M.R., Taylor, M.A., Deuren, M. van, Willemsen, M.A.A.P., Verhagen, M.M.M., Last, J.I., Hogervorst, F.B.L., Smeets, D.F.C.M., Roeleveld, N., Verheijen, F., Catsman-Berrevoets, C.E., Wulffraat, N.M., Cobben, J.M., Hiel, J., Brunt, E.R., Peeters, E.A., Gomez Garcia, E.B., Knaap, M.S. van der, Lincke, C.R., Laan, L.A.E.M., Tijssen, M.P.W., Rijn, M.A. van, Majoor-Krakauer, D., Visser, M. de, Veer, L.J. van 't, Kleijer, W.J., Warrenburg, B.P.C. van de, Warris, A., Groot, I.J.M. de, Groot, R. de, Broeks, A., Preijers, F.W., Kremer, B., Weemaes, C.M.R., Taylor, M.A., Deuren, M. van, and Willemsen, M.A.A.P.

Abstract

1 maart 2012, Item does not contain fulltext, Ataxia-telangiectasia (A-T) is an autosomal recessive neurodegenerative disorder with multisystem involvement and cancer predisposition, caused by mutations in the A-T mutated (ATM) gene. To study genotype-phenotype correlations, we evaluated the clinical and laboratory data of 51 genetically proven A-T patients, and additionally measured ATM protein expression and kinase activity. Patients without ATM kinase activity showed the classical phenotype. The presence of ATM protein, correlated with slightly better immunological function. Residual kinase activity correlated with a milder and essentially different neurological phenotype, absence of telangiectasia, normal endocrine and pulmonary function, normal immunoglobulins, significantly lower X-ray hypersensitivity in lymphocytes, and extended lifespan. In these patients, cancer occurred later in life and generally consisted of solid instead of lymphoid malignancies. The genotypes of severely affected patients generally included truncating mutations resulting in total absence of ATM kinase activity, while patients with milder phenotypes harbored at least one missense or splice site mutation resulting in expression of ATM with some kinase activity. Overall, the phenotypic manifestations in A-T show a continuous spectrum from severe classical childhood-onset A-T to a relatively mild adult-onset disorder, depending on the presence of ATM protein and kinase activity. Each patient is left with a tremendously increased cancer risk.

Published
2012

17. Distress in partners of individuals diagnosed with or at high risk of developing tumors due to rare hereditary cancer syndromes

Author

Lammens, C.R., Bleiker, E.M., Verhoef, S., Ausems, M.G., Majoor-Krakauer, D., Sijmons, R.H., Hes, F.J., Gomez-Garcia, E.B., Os, T.A. van, Spruijt, L., Luijt, R.B. van der, Ouweland, A.M. van den, Ruijs, M.W., Gundy, C., Nagtegaal, T., Aaronson, N.K., Lammens, C.R., Bleiker, E.M., Verhoef, S., Ausems, M.G., Majoor-Krakauer, D., Sijmons, R.H., Hes, F.J., Gomez-Garcia, E.B., Os, T.A. van, Spruijt, L., Luijt, R.B. van der, Ouweland, A.M. van den, Ruijs, M.W., Gundy, C., Nagtegaal, T., and Aaronson, N.K.

Abstract

Contains fulltext : 95821.pdf (publisher's version ) (Closed access), OBJECTIVE: Li Fraumeni syndrome (LFS) and Von Hippel-Lindau disease (VHL) are two rare hereditary tumor syndromes, characterized by a high risk of developing multiple tumors at various sites and ages for which preventive and treatment options are limited. For partners, it may be difficult to deal with the on-going threat of tumors in both their spouse and children. Therefore, this study aims to evaluate the prevalence of and factors associated with psychological distress among partners of individuals with or at high risk of LFS or VHL. METHODS: As part of a nationwide, cross-sectional study, partners of individuals diagnosed with or at high risk of LFS or VHL were invited to complete a self-report questionnaire assessing distress, worries, and health-related quality of life. RESULTS: Fifty-five (58%) of those high-risk individuals with a partner consented to having their partner approached for the study. In total, 50 partners (91%) completed the questionnaire, of whom 28% reported clinically relevant levels of syndrome-related distress. Levels of distress and worries of the partners and their high-risk spouse were significantly correlated. Younger age and a lack of social support were also associated significantly with heightened levels of distress and worries. The majority of partners (76%) believed that professional psychosocial support should be routinely offered to them. CONCLUSIONS: Approximately one-quarter of the partners exhibit clinically relevant levels of distress that warrant psychological support. The distress levels of the 'patient' could potentially be used to identify partners at risk of developing clinically relevant levels of distress.

Published
2011

18. Mutations in SMAD3 cause a syndromic form of aortic aneurysms and dissections with early-onset osteoarthritis

Author

Laar, I.M. van de, Oldenburg, R.A., Pals, G., Roos-Hesselink, J.W., Graaf, B.M. de, Verhagen, J.M., Hoedemaekers, Y.M., Willemsen, R., Severijnen, L.A., Venselaar, H., Vriend, G., Pattynama, P.M., Collee, M., Majoor-Krakauer, D., Poldermans, D., Frohn-Mulder, I.M., Micha, D., Timmermans, J., Hilhorst-Hofstee, Y., Bierma-Zeinstra, S.M., Willems, P.J., Kros, J.M., Oei, E.H., Oostra, B.A., Wessels, M.W., Bertoli-Avella, A.M., Laar, I.M. van de, Oldenburg, R.A., Pals, G., Roos-Hesselink, J.W., Graaf, B.M. de, Verhagen, J.M., Hoedemaekers, Y.M., Willemsen, R., Severijnen, L.A., Venselaar, H., Vriend, G., Pattynama, P.M., Collee, M., Majoor-Krakauer, D., Poldermans, D., Frohn-Mulder, I.M., Micha, D., Timmermans, J., Hilhorst-Hofstee, Y., Bierma-Zeinstra, S.M., Willems, P.J., Kros, J.M., Oei, E.H., Oostra, B.A., Wessels, M.W., and Bertoli-Avella, A.M.

Abstract

Contains fulltext : 92104.pdf (publisher's version ) (Closed access)

Published
2011

19. Compliance with periodic surveillance for Von-Hippel-Lindau disease

Author

Lammens, C.R., Aaronson, N.K., Hes, F.J., Links, T.P., Zonnenberg, B.A., Lenders, J.W.M., Majoor-Krakauer, D., Os, T.A. van, Gomez-Garcia, E.B., Herder, W.W. de, Luijt, R.B. van der, Ouweland, A.M. van den, Hest, L.P. van, Verhoef, S., Bleiker, E.M., Lammens, C.R., Aaronson, N.K., Hes, F.J., Links, T.P., Zonnenberg, B.A., Lenders, J.W.M., Majoor-Krakauer, D., Os, T.A. van, Gomez-Garcia, E.B., Herder, W.W. de, Luijt, R.B. van der, Ouweland, A.M. van den, Hest, L.P. van, Verhoef, S., and Bleiker, E.M.

Abstract

Item does not contain fulltext, PURPOSE: To assess compliance with a periodic surveillance regimen for Von Hippel-Lindau disease. METHODS: In this nationwide study, Von Hippel-Lindau disease mutation carriers and those at 50% risk were invited to complete a questionnaire assessing (compliance with) advice given for periodic surveillance. Medical record data on compliance with recommended radiologic surveillance examinations were also collected. RESULTS: Of the 84 (77%) participants, 78 indicated having received advice to undergo periodic surveillance. Of these, 71 reported being fully compliant with that advice. In 64% of the cases, this advice was only partially consistent with published guidelines. Based on medical record data, between one quarter and one third of individuals did not undergo surveillance as recommended in the guidelines for central nervous system lesions and one half for visceral lesions. Screening delay for central nervous system lesions was significantly higher in one hospital and in those cases where "the advice given" deviated from the guidelines. CONCLUSIONS: The majority of those with or at risk of Von Hippel-Lindau disease reported having received and being fully compliant with screening advice. However, in many cases, the advice given was only partially consistent with published guidelines, and screening delays were observed. Efforts should be undertaken to stimulate guideline-based surveillance advice and to minimize screening delay.

Published
2011

20. Manifest disease, risk factors for sudden cardiac death, and cardiac events in a large nationwide cohort of predictively tested hypertrophic cardiomyopathy mutation carriers: determining the best cardiological screening strategy

Author

Christiaans, I., Birnie, E., Bonsel, G.J., Mannens, M.M.A.M., Michels, M., Majoor-Krakauer, D., Dooijes, D., Tintelen, J.P. van, Berg, M.P van den, Volders, P.G., Arens, Y.H., Wijngaard, A. van den, Atsma, D.E., Helderman-van den Enden, A.T., Houweling, A.C., Boer, K. de, Smagt, J.J. van der, Hauer, R.N.W., Marcelis, C.L.M., Timmermans, J., Langen, I.M. van, Wilde, A.A.M., Christiaans, I., Birnie, E., Bonsel, G.J., Mannens, M.M.A.M., Michels, M., Majoor-Krakauer, D., Dooijes, D., Tintelen, J.P. van, Berg, M.P van den, Volders, P.G., Arens, Y.H., Wijngaard, A. van den, Atsma, D.E., Helderman-van den Enden, A.T., Houweling, A.C., Boer, K. de, Smagt, J.J. van der, Hauer, R.N.W., Marcelis, C.L.M., Timmermans, J., Langen, I.M. van, and Wilde, A.A.M.

Abstract

Item does not contain fulltext, AIMS: We investigated the presence of a clinical diagnosis of hypertrophic cardiomyopathy (HCM), risk factors for sudden cardiac death (SCD), and cardiac events during follow-up in predictively tested-not known to have a clinical diagnosis of HCM before the DNA test-carriers of a sarcomeric gene mutation and associations with age and gender to determine the best cardiological screening strategy. METHODS AND RESULTS: One hundred and thirty-six (30%) of 446 mutation carriers were diagnosed with HCM at one or more cardiological evaluation(s). Male gender and higher age were associated with manifest disease. Incidence of newly diagnosed manifest HCM was <10% per person-year under the age of 40 years and >10% in older carriers, although numbers were small in carriers <15 years. Twenty-three percent of carriers, with and without manifest disease, had established risk factor(s) for SCD (no significant difference). During an average follow-up of 3.5 +/- 1.7 years two carriers, both with manifest disease, died suddenly (0.13% per person-year). A high-risk status for SCD (>/=2 risk factors and manifest HCM) was present in 17 carriers during follow-up (2.4% per person-year). Age but not gender was associated with a high-risk status for SCD. CONCLUSION: Thirty percent of carriers had or developed manifest HCM after predictive DNA testing and risk factors for SCD were frequently present. Our data suggest that the SCD risk is low and risk stratification for SCD can be omitted in carriers without manifest disease and that frequency of cardiological evaluations can possibly be decreased in carriers between 15 and 40 years as long as hypertrophy is absent.

Published
2011

21. Psychosocial impact of Von Hippel-Lindau disease: levels and sources of distress.

Author

Lammens, C.R., Bleiker, E.M., Verhoef, S., Hes, F.J., Ausems, M.G., Majoor-Krakauer, D., Sijmons, R.H., Luijt, R.B. van der, Ouweland, A.M. van den, Os, T.A. van, Hoogerbrugge, N., Gomez Garcia, E.B., Dommering, C.J., Gundy, C.M., Aaronson, N.K., Lammens, C.R., Bleiker, E.M., Verhoef, S., Hes, F.J., Ausems, M.G., Majoor-Krakauer, D., Sijmons, R.H., Luijt, R.B. van der, Ouweland, A.M. van den, Os, T.A. van, Hoogerbrugge, N., Gomez Garcia, E.B., Dommering, C.J., Gundy, C.M., and Aaronson, N.K.

Abstract

1 mei 2010, Contains fulltext : 89552.pdf (publisher's version ) (Closed access), Von Hippel-Lindau disease (VHL) is a hereditary tumor susceptibility syndrome, characterized by an increased risk of developing multiple benign and malignant tumors at various sites and ages with limited preventive options. This study evaluates the prevalence of distress among VHL family members and factors associated significantly with such distress. Forty-eight families with a VHL mutation were identified via the nine family cancer clinics in the Netherlands. In total, 171 family members (carriers, 50% at-risk, non-carriers) were approached, of whom 123 (72%) completed a self-report questionnaire. Approximately 40% of the VHL family members reported clinically relevant levels of distress, approaching 50% among the carriers and, possibly even more striking, 36% among the non-carriers. Having lost a first degree relative due to VHL during adolescence (OR 11.2; 95% CI 1.4-86.9) was related significantly to heightened levels of distress. Approximately, only one-third of those who reported heightened levels of distress had received professional psychosocial support. A substantial percentage of family members experience clinically relevant levels of distress. We would recommend the introduction of a procedure for screening for distress in this vulnerable population. Special attention should be paid to those individuals who have lost a close relative due to VHL during adolescence.

Published
2010

22. Clinical spectrum of ataxia-telangiectasia in adulthood.

Author

Verhagen, M.M.M., Abdo, W.F., Willemsen, M.A.A.P., Hogervorst, F.B.L., Smeets, D.F.C.M., Hiel, J.A.P., Brunt, E.R., Rijn, M.A. van, Majoor Krakauer, D., Oldenburg, R.A., Broeks, A., Last, J.I., Veer, L.J. van 't, Tijssen, M.A., Dubois, A.M., Kremer, H.P.H., Weemaes, C.M.R., Taylor, A.M., Deuren, M. van, Verhagen, M.M.M., Abdo, W.F., Willemsen, M.A.A.P., Hogervorst, F.B.L., Smeets, D.F.C.M., Hiel, J.A.P., Brunt, E.R., Rijn, M.A. van, Majoor Krakauer, D., Oldenburg, R.A., Broeks, A., Last, J.I., Veer, L.J. van 't, Tijssen, M.A., Dubois, A.M., Kremer, H.P.H., Weemaes, C.M.R., Taylor, A.M., and Deuren, M. van

Abstract

Contains fulltext : 79696.pdf (publisher's version ) (Closed access), OBJECTIVE: To describe the phenotype of adult patients with variant and classic ataxia-telangiectasia (A-T), to raise the degree of clinical suspicion for the diagnosis variant A-T, and to assess a genotype-phenotype relationship for mutations in the ATM gene. METHODS: Retrospective analysis of the clinical characteristics and course of disease in 13 adult patients with variant A-T of 9 families and 6 unrelated adults with classic A-T and mutation analysis of the ATM gene and measurements of ATM protein expression and kinase activity. RESULTS: Patients with variant A-T were only correctly diagnosed in adulthood. They often presented with extrapyramidal symptoms in childhood, whereas cerebellar ataxia appeared later. Four patients with variant A-T developed a malignancy. Patients with classic and variant A-T had elevated serum alpha-fetoprotein levels and chromosome 7/14 rearrangements. The mildest variant A-T phenotype was associated with missense mutations in the ATM gene that resulted in expression of some residual ATM protein with kinase activity. Two splicing mutations, c.331 + 5G>A and c.496 + 5G>A, caused a more severe variant A-T phenotype. The splicing mutation c.331 + 5G>A resulted in less ATM protein and kinase activity than the missense mutations. CONCLUSIONS: Ataxia-telangiectasia (A-T) should be considered in patients with unexplained extrapyramidal symptoms. Early diagnosis is important given the increased risk of malignancies and the higher risk for side effects of subsequent cancer treatment. Measurement of serum alpha-fetoprotein and chromosomal instability precipitates the correct diagnosis. There is a clear genotype-phenotype relation for A-T, since the severity of the phenotype depends on the amount of residual kinase activity as determined by the genotype.

Published
2009

25. Cardiac abnormalities in a follow-up study on carriers of Duchenne and Becker muscular dystrophy

Author

van Westrum, S. M. S., primary, Hoogerwaard, E. M., additional, Dekker, L., additional, Standaar, T. S., additional, Bakker, E., additional, Ippel, P. F., additional, Oosterwijk, J. C., additional, Majoor-Krakauer, D. F., additional, van Essen, A. J., additional, Leschot, N. J., additional, Wilde, A. A. M., additional, de Haan, R. J., additional, de Visser, M., additional, and van der Kooi, A. J., additional

Published
2011
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26. Manifest disease, risk factors for sudden cardiac death, and cardiac events in a large nationwide cohort of predictively tested hypertrophic cardiomyopathy mutation carriers: determining the best cardiological screening strategy

Author

Christiaans, I., primary, Birnie, E., additional, Bonsel, G. J., additional, Mannens, M. M. A. M., additional, Michels, M., additional, Majoor-Krakauer, D., additional, Dooijes, D., additional, van Tintelen, J. P., additional, van den Berg, M. P., additional, Volders, P. G. A., additional, Arens, Y. H., additional, van den Wijngaard, A., additional, Atsma, D. E., additional, Helderman-van den Enden, A. T. J. M., additional, Houweling, A. C., additional, de Boer, K., additional, van der Smagt, J. J., additional, Hauer, R. N. W., additional, Marcelis, C. L. M., additional, Timmermans, J., additional, van Langen, I. M., additional, and Wilde, A. A. M., additional

Published
2011
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27. Founder mutations in hypertrophic cardiomyopathy patients in the Netherlands

Author

Christiaans*, I., primary, Nannenberg*, E. A., additional, Dooijes, D., additional, Jongbloed, R. J. E., additional, Michels, M., additional, Postema, P. G., additional, Majoor-Krakauer, D., additional, van den Wijngaard, A., additional, Mannens, M. M. A. M., additional, van Tintelen, J. P., additional, van Langen, I. M., additional, and Wilde, A. A. M., additional

Published
2010
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28. Clinical spectrum of ataxia-telangiectasia in adulthood

Author

Verhagen, M.M.M., primary, Abdo, W. F., additional, Willemsen, M. A.A.P., additional, Hogervorst, F. B.L., additional, Smeets, D. F.C.M., additional, Hiel, J. A.P., additional, Brunt, E. R., additional, van Rijn, M. A., additional, Majoor Krakauer, D., additional, Oldenburg, R. A., additional, Broeks, A., additional, Last, J. I., additional, van't Veer, L. J., additional, Tijssen, M. A.J., additional, Dubois, A. M.I., additional, Kremer, H. P.H., additional, Weemaes, C. M.R., additional, Taylor, A. M.R., additional, and van Deuren, M., additional

Published
2009
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29. Genetic diagnostics and genetic counselling in Hypertrophic Cardiomyopathy (HCM)

Author

Langen, I. M., Arens, Y., Baars, H., Bokenkamp, R., Delhaas, T., Dooijes, D., Lekanne Deprez, R., Majoor-Krakauer, D., Folkert ten Cate, Michels, M., Mil, A., Pinto, Y., Schiphorst, A., Smagt, J. J., Tintelen, J. P., Amsterdam Cardiovascular Sciences, Amsterdam Gastroenterology Endocrinology Metabolism, Other Research, Human Genetics, Cardiology, Other departments, Faculteit Medische Wetenschappen/UMCG, Reproductive Origins of Adult Health and Disease (ROAHD), Cardiovascular Centre (CVC), and Health Psychology Research (HPR)

Subjects
medicine.medical_specialty, business.industry, health care facilities, manpower, and services, Genetic counseling, education, Hypertrophic cardiomyopathy, Guideline, medicine.disease, University hospital, humanities, Paediatric cardiology, Family medicine, Physical therapy, Medicine, Medical genetics, Outpatient clinic, cardiovascular diseases, Multidisciplinary Guideline, Cardiology and Cardiovascular Medicine, business, Psychosocial, health care economics and organizations
Abstract

Dutch professional groups involved in drawing up this guideline: cardiologists, paediatric cardiologists, clinical geneticists, clinical molecular geneticists, genetic counsellors, psychosocial workers, associated with or cooperating with the university hospitals’ outpatient clinics for cardiogenetics. Approved by the NVVC, VKGN and NVK (paediatric cardiology section). NVVC - Nederlandse Vereniging voor Cardiologie – Dutch Society for Cardiology; VKGN - Vereniging Klinische Genetica Nederland – the Netherlands Society for Clinical Genetics; NVK - Nederlandse Vereniging Kindergeneeskunde – Dutch Society for Paediatrics. First published in Dutch in June 2009.

Published
2010

32. TDP-43 pathology in familial frontotemporal dementia and motor neuron disease without Progranulin mutations

Author

Seelaar, H., primary, Jurgen Schelhaas, H., additional, Azmani, A., additional, Kusters, B., additional, Rosso, S., additional, Majoor-Krakauer, D., additional, de Rijik, M. C., additional, Rizzu, P., additional, ten Brummelhuis, M., additional, van Doorn, P. A., additional, Kamphorst, W., additional, Willemsen, R., additional, and van Swieten, J. C., additional

Published
2007
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33. A homozygous mutation in the endothelin-3 gene associated with a combined Waardenburg type 2 and Hirschsprung phenotype (Shah-Waardenburg syndrome)

Author

Hofstra, R.M., Osinga, J., Sindhunata, G.T., Wu, Y., Kamsteeg, E.J., Stulp, R.P., Ravenswaaij-Arts, C. van, Majoor-Krakauer, D., Angrist, M., Chakravarti, A., Meijers, C., Buijs, C.H.C.M., Hofstra, R.M., Osinga, J., Sindhunata, G.T., Wu, Y., Kamsteeg, E.J., Stulp, R.P., Ravenswaaij-Arts, C. van, Majoor-Krakauer, D., Angrist, M., Chakravarti, A., Meijers, C., and Buijs, C.H.C.M.

Abstract

Contains fulltext : 23620___.PDF (publisher's version ) (Open Access)

Published
1996

34. First-trimester diagnosis of late-infantile neuronal ceroid lipofuscinosis (LINCL) by tripeptidyl peptidase I assay and CLN2 mutation analysis

Author

Kleijer, W. J., primary, van Diggelen, O. P., additional, Keulemans, J. L. M., additional, Losekoot, M., additional, Garritsen, V. H., additional, Stroink, H., additional, Majoor-Krakauer, D., additional, Franken, P. F., additional, Eurlings, M. C. M., additional, Taschner, P. E. M., additional, Los, F. J., additional, and Galjaard, R. J. H., additional

Published
2001
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35. The clinical and pathological phenotype of C9ORF72 hexanucleotide repeat expansions.

Author

Simón-Sánchez J, Dopper EG, Cohn-Hokke PE, Hukema RK, Nicolaou N, Seelaar H, de Graaf JR, de Koning I, van Schoor NM, Deeg DJ, Smits M, Raaphorst J, van den Berg LH, Schelhaas HJ, De Die-Smulders CE, Majoor-Krakauer D, Rozemuller AJ, Willemsen R, Pijnenburg YA, and Heutink P

Abstract

There is increasing evidence that frontotemporal dementia and amyotrophic lateral sclerosis are part of a disease continuum. Recently, a hexanucleotide repeat expansion in C9orf72 was identified as a major cause of both sporadic and familial frontotemporal dementia and amyotrophic lateral sclerosis. The aim of this study was to investigate clinical and neuropathological characteristics of hexanucleotide repeat expansions in C9orf72 in a large cohort of Dutch patients with frontotemporal dementia. Repeat expansions were successfully determined in a cohort of 353 patients with sporadic or familial frontotemporal dementia with or without amyotrophic lateral sclerosis, and 522 neurologically normal controls. Immunohistochemistry was performed in a series of 10 brains from patients carrying expanded repeats using a panel of antibodies. In addition, the presence of RNA containing GGGGCC repeats in paraffin-embedded sections of post-mortem brain tissue was investigated using fluorescence in situ hybridization with a locked nucleic acid probe targeting the GGGGCC repeat. Hexanucleotide repeat expansions in C9orf72 were found in 37 patients with familial (28.7%) and five with sporadic frontotemporal dementia (2.2%). The mean age at onset was 56.9 ± 8.3 years (range 39-76), and disease duration 7.6 ± 4.6 years (range 1-22). The clinical phenotype of these patients varied between the behavioural variant of frontotemporal dementia (n = 34) and primary progressive aphasia (n = 8), with concomitant amyotrophic lateral sclerosis in seven patients. Predominant temporal atrophy on neuroimaging was present in 13 of 32 patients. Pathological examination of the 10 brains from patients carrying expanded repeats revealed frontotemporal lobar degeneration with neuronal transactive response DNA binding protein-positive inclusions of variable type, size and morphology in all brains. Fluorescence in situ hybridization analysis of brain material from patients with the repeat expansion, a microtubule-associated protein tau or a progranulin mutation, and controls did not show RNA-positive inclusions specific for brains with the GGGGCC repeat expansion. The hexanucleotide repeat expansion in C9orf72 is an important cause of frontotemporal dementia with and without amyotrophic lateral sclerosis, and is sometimes associated with primary progressive aphasia. Neuropathological hallmarks include neuronal and glial inclusions, and dystrophic neurites containing transactive response DNA binding protein. Future studies are needed to explain the wide variation in clinical presentation. [ABSTRACT FROM AUTHOR]

Published
2012
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37. DNA probe analysis for carrier detection and prenatal diagnosis of Duchenne muscular dystrophy: a standard diagnostic procedure.

Author

Bakker, E, Bonten, E J, De Lange, L F, Veenema, H, Majoor-Krakauer, D, Hofker, M H, Van Ommen, G J, and Pearson, P L

Abstract

Thirteen marker loci localised on the short arm of the X chromosome are available for use in genetic studies for Duchenne muscular dystrophy (DMD). This large number of probes detecting about 20 RFLPs encouraged us to set up a standard procedure using a sequence of selected probes and restriction enzymes for the diagnosis of DMD families. The application of DNA probe analysis for carrier detection and prenatal diagnosis, involving 61 pedigrees of both familial and isolated cases, has yielded the following results. Carrier detection using flanking markers was possible in more than 75% of the cases (104 out of 136 females) with a reliability of better than 98%. Prenatal diagnosis was possible in 95% of the cases (65 out of 68 proven carriers or women at risk). Twenty-three prenatal diagnoses were performed on male fetuses; 13 appeared to have a low risk for DMD (less than 1%) and thus the pregnancies continued. Seven have since come to term and the male infants have normal CK levels. The genetic distances of the loci relative to the DMD locus and their order on the short arm of the X chromosome were deduced from our total DMD family material and are not significantly different from those reported earlier. For 754 (DXS84) we found a genetic distance of 5 cM with a lod score of +12.4 and 95% confidence limits between 2 and 12 cM. Similar data were obtained for pERT87 (DXS164), suggesting that in our family material both loci are tightly linked. Multiply informative recombination showed that both 754 and pERT87 map proximal to the DMD mutations in the cases studied. The high frequency of DMD mutations and its relation to the observed instability in this part of the genome will be discussed. Unequal crossing over is proposed as one of the mechanisms contributing to the high mutation frequency. [ABSTRACT FROM PUBLISHER]

Published
1986

38. PRENATAL DIAGNOSIS AND CARRIER DETECTION OF DUCHENNE MUSCULAR DYSTROPHY WITH CLOSELY LINKED RFLPs

Author

Bakker, E, Goor, N, Wrogemann, K, Kunkel, L.M, Fenton, W.A, Majoor-Krakauer, D, Jahoda, M.G.J, Ommen, G.J.B.Van, Hofker, M.H, Mandel, J.L, Davies, K.E, Willard, H.F, Sandkuyl, L, Essen, A.J.V, Sachs, E.S, and Pearson, P.L

Abstract

By the use of a series of closely linked DNA probes detecting restriction fragment length polymorphisms (RFLPs) distributed over the short arm of the X chromosome, a double crossover was detected in a Duchenne muscular dystrophy carrier and an affected male fetus was diagnosed at 12 weeks of gestation, with a probable accuracy of more than 99·0%. A new mutation was identified in another family with the same degree of reliability; three females in this family were thus deemed not to be DMD carriers. The eleven RFLP-markers presently available on the short arm of the X chromosome are useful in the diagnosis of DMD since they bridge the Duchenne locus at genetic distances varying between 3 and 20 cmo. Moreover, recombination within the set of markers provides an independent way of regionally mapping these probes relative to each other along the short arm of the X chromosome.

Published
1985
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40. Von Hippel–Lindau disease maps to the region of chromosome 3 associated with renal cell carcinoma

Author

Seizinger, B. R., primary, Rouleau, G. A., additional, Ozelius, L. J., additional, Lane, A. H., additional, Farmer, G. E., additional, Lamiell, J. M., additional, Haines, J., additional, Yuen, J. W. M., additional, Collins, D., additional, Majoor-Krakauer, D., additional, Bonner, T., additional, Mathew, C., additional, Rubenstein, A., additional, Halperin, J., additional, McConkie-Rosell, A., additional, Green, J. S., additional, Trofatter, J. A., additional, Ponder, B. A., additional, Eierman, L., additional, Bowmer, M. I., additional, Schimke, R., additional, Oostra, B., additional, Aronin, N., additional, Smith, D. I., additional, Drabkin, H., additional, Waziri, M. H., additional, Hobbs, W. J., additional, Martuza, R. L., additional, Conneally, P. M., additional, Hsia, Y. E., additional, and Gusella, J. F., additional

Published
1988
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43. Von Hippel–Lindau disease maps to the region of chromosome 3 associated with renal cell carcinoma

Author

Seizinger, B. R., Rouleau, G. A., Ozelius, L. J., Lane, A. H., Farmer, G. E., Lamiell, J. M., Haines, J., Yuen, J. W. M., Collins, D., Majoor-Krakauer, D., Bonner, T., Mathew, C., Rubenstein, A., Halperin, J., McConkie-Rosell, A., Green, J. S., Trofatter, J. A., Ponder, B. A., Eierman, L., Bowmer, M. I., Schimke, R., Oostra, B., Aronin, N., Smith, D. I., Drabkin, H., Waziri, M. H., Hobbs, W. J., Martuza, R. L., Conneally, P. M., Hsia, Y. E., and Gusella, J. F.

Abstract

Von Hippel–Lindau disease (VHL) is an autosomal dominant disorder with inherited susceptibility to various forms of cancer, including hemangioblastomas of the central nervous system, phaeochromocytomas, pancreatic malignancies, and renal cell carcinomas1–3. Renal cell carcinomas constitute a particularly frequent cause of death in this disorder, occurring as bilateral and multifocal tumours, and presenting at an earlier age than in sporadic, non-familial cases of this tumour type. We report here that the VHL gene is linked to the locus encoding the human homologoue of the RAF1 oncogene, which maps to chromosome 3p25 (ref. 4). Crossovers with the VHL locus suggest that the defect responsible for the VHL phenotype is not a mutation in the RAF1 gene itself. An alternative or prior event to oncogene activation in tumour formation may be the inactivation of a putative 'tumour suppressor' which can be associated with both the inherited and sporadic forms of the cancer. Sporadic renal cell carcinomas have previously been associated with the loss of regions on chromosome 3p (refs 5, 6). Consequently, sporadic and VHL-associated forms of renal cell carcinoma might both result from alterations causing loss of function of the same 'tumour suppressor' gene on this chromosome.

Published
1988
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45. Whole aorta imaging shows increased risk for thoracic aortic aneurysms and dilatations in relatives of abdominal aortic aneurysm patients.

Author

Liu H, IJpma AS, de Bruin JL, Verhagen HJM, Roos-Hesselink JW, Bekkers JA, Brüggenwirth HT, van Beusekom HMM, and Majoor-Krakauer D

Abstract

Objective: For relatives of abdominal aortic aneurysm (AAA) patients, guidelines recommend abdominal imaging aimed at early detection and management of AAA, and do not include screening for thoracic aortic aneurysms (TAA). We aimed to investigate if TAA occur in undiagnosed relatives of AAA patients without a known genetic susceptibility for aneurysms, similar to families with identified genetic susceptibilities for aneurysms like in Marfan and Loeys-Dietz syndrome, where both AAA and TAA occur., Methods: Relatives of AAA patients were invited for non-contrast whole aorta CT screening. Systematic measurements of the CT scans were used to detect aneurysms and dilatations. Classification into familial and non-familial was based on reported family histories. In addition, aneurysm gene panel testing of AAA index cases was used for the classification of high vs unknown genetic risk (high genetic risk: familial aneurysm or a (likely) pathogenic variant (P/LP) in an aneurysm gene; unknown genetic risk: no family history or P/LP)., Results: Whole aorta imaging of 301 relatives of 115 abdominal aortic aneurysm index-patients with non-contrast CT scans showed a 28-fold increase in thoracic aortic aneurysms in relatives (1.7%, p<0.001 versus the age adjusted population) and a high frequency of thoracic dilatations in 18% of the relatives. Thoracic aneurysms and dilatations in relatives occurred even when index patients were unaware of familial aneurysms. AAA was increased in the relatives compared to the age adjusted population (8%, p<0.001)., Conclusions: An increased risk for thoracic aneurysms and dilatations was detected by whole aorta imaging of relatives of AAA index patients, even when index patients were unaware of familial aneurysms. These results indicate -still unknown- shared genetic susceptibilities for thoracic and abdominal aneurysms. Therefore, imaging of the whole aorta of relatives of all abdominal aneurysm patients, will improve early detection of aortic aneurysms in relatives of all AAA patients., (Copyright © 2024. Published by Elsevier Inc.)

Published
2024
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46. Increased vascular smooth muscle cell senescence in aneurysmal Fibulin-4 mutant mice.

Author

Stefens SJM, van Vliet N, IJpma A, Burger J, Li Y, van Heijningen PM, Lindeman JHN, Majoor-Krakauer D, Verhagen HJM, Kanaar R, Essers J, and van der Pluijm I

Abstract

Aortic aneurysms are dilatations of the aorta that can rupture when left untreated. We used the aneurysmal Fibulin-4 R/R mouse model to further unravel the underlying mechanisms of aneurysm formation. RNA sequencing of 3-month-old Fibulin-4 R/R aortas revealed significant upregulation of senescence-associated secretory phenotype (SASP) factors and key senescence factors, indicating the involvement of senescence. Analysis of aorta histology and of vascular smooth muscle cells (VSMCs) in vitro confirmed the senescent phenotype of Fibulin-4 R/R VSMCs by revealing increased SA-β-gal, p21, and p16 staining, increased IL-6 secretion, increased presence of DNA damage foci and increased nuclei size. Additionally, we found that p21 luminescence was increased in the dilated aorta of Fibulin-4 R/R |p21-luciferase mice. Our studies identify a cellular aging cascade in Fibulin-4 aneurysmal disease, by revealing that Fibulin-4 R/R aortic VSMCs have a pronounced SASP and a senescent phenotype that may underlie aortic wall degeneration. Additionally, we demonstrated the therapeutic effect of JAK/STAT and TGF-β pathway inhibition, as well as senolytic treatment on Fibulin-4 R/R VSMCs in vitro. These findings can contribute to improved therapeutic options for aneurysmal disease aimed at reducing senescent cells., (© 2024. The Author(s).)

Published
2024
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47. Vascular Ehlers-Danlos Syndrome: A Comprehensive Natural History Study in a Dutch National Cohort of 142 Patients.

Author

Demirdas S, van den Bersselaar LM, Lechner R, Bos J, Alsters SIM, Baars MJH, Baas AF, Baysal Ö, van der Crabben SN, Dulfer E, Giesbertz NAA, Helderman-van den Enden ATJM, Hilhorst-Hofstee Y, Kempers MJE, Komdeur FL, Loeys B, Majoor-Krakauer D, Ockeloen CW, Overwater E, van Tintelen PJ, Voorendt M, de Waard V, Maugeri A, Brüggenwirth HT, van de Laar IMBH, and Houweling AC

Subjects
Humans, Female, Male, Netherlands epidemiology, Adult, Middle Aged, Retrospective Studies, Cohort Studies, Phenotype, Adolescent, Genetic Association Studies, Young Adult, Aged, Ehlers-Danlos Syndrome, Type IV, Ehlers-Danlos Syndrome genetics, Ehlers-Danlos Syndrome epidemiology, Collagen Type III genetics
Abstract

Background: Vascular Ehlers-Danlos syndrome (vEDS) is a rare connective tissue disorder with a high risk for arterial, bowel, and uterine rupture, caused by heterozygous pathogenic variants in COL3A1 . The aim of this cohort study is to provide further insights into the natural history of vEDS and describe genotype-phenotype correlations in a Dutch multicenter cohort to optimize patient care and increase awareness of the disease., Methods: Individuals with vEDS throughout the Netherlands were included. The phenotype was charted by retrospective analysis of molecular and clinical data, combined with a one-time physical examination., Results: A total of 142 individuals (50% female) participated the study, including 46 index patients (32%). The overall median age at genetic diagnosis was 41.0 years. More than half of the index patients (54.3%) and relatives (53.1%) had a physical appearance highly suggestive of vEDS. In these individuals, major events were not more frequent ( P =0.90), but occurred at a younger age ( P =0.01). A major event occurred more often and at a younger age in men compared with women ( P <0.001 and P =0.004, respectively). Aortic aneurysms ( P =0.003) and pneumothoraces ( P =0.029) were more frequent in men. Aortic dissection was more frequent in individuals with a COL3A1 variant in the first quarter of the collagen helical domain ( P =0.03)., Conclusions: Male sex, type and location of the COL3A1 variant, and physical appearance highly suggestive of vEDS are risk factors for the occurrence and early age of onset of major events. This national multicenter cohort study of Dutch individuals with vEDS provides a valuable basis for improving guidelines for the diagnosing, follow-up, and treatment of individuals with vEDS., Competing Interests: Disclosures None.

Published
2024
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48. The proprotein convertase FURIN is a novel aneurysm predisposition gene impairing TGF-β signaling.

Author

He Z, IJpma AS, Vreeken D, Heijsman D, Rosier K, Verhagen HJM, de Bruin J, Brüggenwirth HT, Roos-Hesselink JW, Bekkers JA, Huylebroeck D, van Beusekom H, Creemers JWM, and Majoor-Krakauer D

Abstract

Aim: Aortic aneurysms (AA) frequently involve dysregulation of transforming growth factor β (TGF-β)-signaling in the aorta. Here, FURIN was tested as aneurysm predisposition gene given its role as proprotein convertase in pro-TGF-β maturation., Methods and Results: Rare FURIN variants were detected by whole-exome sequencing of 781 unrelated aortic aneurysm patients and affected relatives. Thirteen rare heterozygous FURIN variants occurred in 3.7% (29) unrelated index AA patients, of which 72% had multiple aneurysms or a dissection.FURIN maturation and activity of these variants were decreased in vitro. Patient-derived fibroblasts showed decreased pro-TGF-β processing, phosphorylation of downstream effector SMAD2 and kinases ERK1/2, and steady-state mRNA levels of the TGF-β-responsive ACTA2 gene. In aortic tissue, collagen and fibrillin fibers were affected. One variant (R745Q), observed in 10 unrelated cases, affected TGF-β signaling variably, indicating effect modification by individual genetic backgrounds., Conclusion: FURIN is a novel, frequent genetic predisposition for abdominal-, thoracic-, and multiple aortic or middle sized artery aneurysms in older patients, by affecting intracellular TGF-β signaling, depending on individual genetic backgrounds., (© The Author(s) 2024. Published by Oxford University Press on behalf of the European Society of Cardiology.)

Published
2024
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49. Contraction pressure analysis using optical imaging in normal and MYBPC3-mutated hiPSC-derived cardiomyocytes grown on matrices with tunable stiffness.

Author

Snelders M, Koedijk IH, Schirmer J, Mulleners O, van Leeuwen J, de Wagenaar NP, Bartulos O, Voskamp P, Braam S, Guttenberg Z, Danser AHJ, Majoor-Krakauer D, Meijering E, van der Pluijm I, and Essers J

Abstract

Current in vivo disease models and analysis methods for cardiac drug development have been insufficient in providing accurate and reliable predictions of drug efficacy and safety. Here, we propose a custom optical flow-based analysis method to quantitatively measure recordings of contracting cardiomyocytes on polydimethylsiloxane (PDMS), compatible with medium-throughput systems. Movement of the PDMS was examined by covalently bound fluorescent beads on the PDMS surface, differences caused by increased substrate stiffness were compared, and cells were stimulated with β-agonist. We further validated the system using cardiomyocytes treated with endothelin-1 and compared their contractions against control and cells incubated with receptor antagonist bosentan. After validation we examined two MYBPC3-mutant patient-derived cell lines. Recordings showed that higher substrate stiffness resulted in higher contractile pressure, while beating frequency remained similar to control. β-agonist stimulation resulted in both higher beating frequency as well as higher pressure values during contraction and relaxation. Cells treated with endothelin-1 showed an increased beating frequency, but a lower contraction pressure. Cells treated with both endothelin-1 and bosentan remained at control level of beating frequency and pressure. Lastly, both MYBPC3-mutant lines showed a higher beating frequency and lower contraction pressure. Our validated method is capable of automatically quantifying contraction of hiPSC-derived cardiomyocytes on a PDMS substrate of known shear modulus, returning an absolute value. Our method could have major benefits in a medium-throughput setting., Competing Interests: The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2022 Published by Elsevier Ltd.)

Published
2022
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50. State-of-the art review: Noncompaction cardiomyopathy in pediatric patients.

Author

Rohde S, Muslem R, Kaya E, Dalinghaus M, van Waning JI, Majoor-Krakauer D, Towbin J, and Caliskan K

Subjects
Adult, Arrhythmias, Cardiac, Child, Heart, Humans, Infant, Infant, Newborn, Cardiomyopathies diagnosis, Cardiomyopathies epidemiology, Heart Defects, Congenital complications, Heart Defects, Congenital diagnosis, Heart Defects, Congenital epidemiology, Thromboembolism
Abstract

Noncompaction cardiomyopathy (NCCM) is a disease characterized by hypertrabeculation, commonly hypothesized due to an arrest in compaction during fetal development. In 2006, NCCM was classified as a distinct form of cardiomyopathy (CMP) by the American Heart Association. NCCM in childhood is more frequently familial than when diagnosed in adulthood and is associated with other congenital heart diseases (CHDs), other genetic CMPs, and neuromuscular diseases (NMDs). It is yet a rare cardiac diseased with an estimated incidence of 0.12 per 100.000 in children up to 10 years of age. Diagnosing NCCM can be challenging due to non-uniform diagnostic criteria, unawareness, presumed other CMPs, and presence of CHD. Therefore, the incidence of NCCM in children might be an underestimation. Nonetheless, NCCM is the third most common cardiomyopathy in childhood and is associated with heart failure, arrhythmias, and/or thromboembolic events. This state-of-the-art review provides an overview on pediatric NCCM. In addition, we discuss the natural history, epidemiology, genetics, clinical presentation, outcome, and therapeutic options of NCCM in pediatric patients, including fetuses, neonates, infants, and children. Furthermore, we provide a simple classification of different forms of the disease. Finally, the differences between the pediatric population and the adult population are described., (© 2021. The Author(s).)

Published
2022
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