Your search keyword '"Frohn-Mulder, I.M."' showing total 11 results

1. Delayed Diagnosis of Danon Disease in Patients Presenting With Isolated Cardiomyopathy

Author

Demirdas, S., Slegtenhorst, M.A. van, Verdijk, R.M., Lee, M., Hout, H.M. van den, Wessels, M.W., Frohn-Mulder, I.M., Gardeitchik, T., Ploeg, A.T. van der, Schaaf, G.J., Demirdas, S., Slegtenhorst, M.A. van, Verdijk, R.M., Lee, M., Hout, H.M. van den, Wessels, M.W., Frohn-Mulder, I.M., Gardeitchik, T., Ploeg, A.T. van der, and Schaaf, G.J.

Abstract

Contains fulltext : 204213.pdf (publisher's version ) (Closed access)

Published

2019

2. Fluorinated steroids do not improve outcome of isolated atrioventricular block

Author

Berg, N.W. Van den, Slieker, M.G., Beynum, I.M. van, Bilardo, C.M., Bruijn, D. de, Clur, S.A., Cornette, J.M., Frohn-Mulder, I.M., Haak, M.C., Loo-Maurus, K.E. van, Manten, G.T., Rackowitz, A.B., Rammeloo, L.A., Reimer, A., Rijlaarsdam, M.E., Freund, M.W., Berg, N.W. Van den, Slieker, M.G., Beynum, I.M. van, Bilardo, C.M., Bruijn, D. de, Clur, S.A., Cornette, J.M., Frohn-Mulder, I.M., Haak, M.C., Loo-Maurus, K.E. van, Manten, G.T., Rackowitz, A.B., Rammeloo, L.A., Reimer, A., Rijlaarsdam, M.E., and Freund, M.W.

Abstract

Item does not contain fulltext, INTRODUCTION: Congenital atrioventricular block (CAVB) is a rare disorder with a significant morbidity and mortality. Consensus regarding the prescription and efficacy of prenatal corticosteroids is lacking. This nationwide study was initiated to evaluate the effects of prenatal treatment with corticosteroids on the outcome of CAVB in The Netherlands. METHODS: All fetuses identified with isolated congenital AVB-II degrees or AVB-III degrees in any of the eight academic fetal heart centers of The Netherlands between 2003 and 2013 were included and reviewed. RESULTS: Fifty-six fetuses were included. Fourteen (25%) fetuses were treated with dexamethasone. We found no differences between the steroid-treated and untreated cases regarding in utero progression of the AVB (63% vs 67% respectively), survival to birth (86% vs 84%), pacemaker implantations (74% vs 58%) or long-term dilated cardiomyopathy (13% vs 17%). Steroid treated fetuses demonstrated more in utero growth restriction (38% vs 11%). CONCLUSION: No benefit from prenatal corticosteroid treatment was demonstrated for fetuses with isolated CAVB in this study. However, we found negative side effects. Our data provide no evidence to support the routine administration of corticosteroids for the treatment of fetal CAVB.

Published

2016

3. Three new families with arterial tortuosity syndrome

Author

Wessels, M.W., Catsman-Berrevoets, C.E., Mancini, G.M.S., Breuning, M.H., Hoogeboom, J.J., Stroink, H., Frohn-Mulder, I.M., Coucke, P.J., Paepe, A.D., Niermeijer, M.F., and Willems, P.J.

Subjects

Genetic defects of metabolism [UMCN 5.1]

Abstract

Contains fulltext : 59229.pdf (Publisher’s version ) (Closed access) Arterial tortuosity syndrome (ATS) is a rare condition with autosomal recessive inheritance characterized by connective tissue abnormalities. The most specific clinical findings are cardiovascular anomalies including tortuosity, lengthening, aneurysm, and stenosis formation of major arteries. Also ventricular hypertrophy is frequently present. Other anomalies are skin hyperextensibility and cutis laxa, joint laxity or contractures of the joints, and inguinal herniae. Histology shows disruption of elastic fibers of the media. These features suggest that ATS is a connective tissue disorder. A biochemical or molecular defect has not yet been identified. We describe here nine additional ATS patients from three consanguineous Moroccan families and review a total of 35 patients with this uncommon condition.

Published

2004

4. Autosomal dominant inheritance of left ventricular outflow tract obstruction

Author

Wessels, M.W., Berger, R.M., Frohn-Mulder, I.M., Roos-Hesselink, J.W., Hoogeboom, J.J., Mancini, G.S., Bartelings, M.M., Krijger, R.R. de, Wladimiroff, J.W., Niermeijer, M.F., Grossfeld, P., and Willems, P.J.

Subjects

Genomic disorders and inherited multi-system disorders [IGMD 3], Genetic defects of metabolism [UMCN 5.1], cardiovascular system

Abstract

Contains fulltext : 47582.pdf (Publisher’s version ) (Closed access) Most nonsyndromic congenital heart malformations (CHMs) in humans are multifactorial in origin, although an increasing number of monogenic cases have been reported recently. We describe here four new families with presumed autosomal dominant inheritance of left ventricular outflow tract obstruction (LVOTO), consisting of hypoplastic left heart (HLHS) or left ventricle (HLV), aortic valve stenosis (AS) and bicuspid aortic valve (BAV), hypoplastic aortic arch (HAA), and coarctation of the aorta (CoA). LVOTO in these families shows a wide clinical spectrum with some family members having severe anomalies such as hypoplastic left heart, and others only minor anomalies such as mild aortic valve stenosis. This supports the suggestion that all anomalies of the LVOTO spectrum are developmentally related and can be caused by a single gene defect.

Published

2005

5. Low agreement between cardiologists diagnosing left ventricular hypertrophy in children with end-stage renal disease.

Author

Schoenmaker, N.J., Lee, J.H. van der, Groothoff, J.W., Iperen, G.G. van, Frohn-Mulder, I.M., Tanke, R.B., Ottenkamp, J., Kuipers, I.M., Schoenmaker, N.J., Lee, J.H. van der, Groothoff, J.W., Iperen, G.G. van, Frohn-Mulder, I.M., Tanke, R.B., Ottenkamp, J., and Kuipers, I.M.

Abstract

Contains fulltext : 144663.pdf (publisher's version ) (Open Access), BACKGROUND: Monitoring of the appearance of left ventricular hypertrophy (LVH) by echocardiography is currently recommended for in the management of children with End-stage renal disease (ESRD). In order to investigate the validity of this method in ESRD children, we assessed the intra- and inter-observer reproducibility of the diagnosis LVH. METHODS: Echocardiographic measurements in 92 children (0-18 years) with ESRD, made by original analysists, were reassessed offline, twice, by 3 independent observers. Smallest detectable changes (SDC) were calculated for continuous measurements of diastolic interventricular septum (IVSd), Left ventricle posterior wall thickness (LVPWd), Left ventricle end-diastolic diameter (LVEDd), and Left ventricle mass index (LVMI). Cohen's kappa was calculated to assess the reproducibility of LVH defined in two different ways. LVH(WT) was defined as Z-value of IVSd and/or LVPWd>2 and LVH(MI) was defined as LVMI> 103 g/m(2) for boys and >84 g/m(2) for girls. RESULTS: The intra-observer SDCs ranged from 1.6 to 1.7 mm, 2.0 to 2.6 mm and 17.7 to 30.5 g/m(2) for IVSd, LVPWd and LVMI, respectively. The inter-observer SDCs were 2.6 mm, 2.9 mm and 24.6 g/m(2) for IVSd, LVPWd and LVMI, respectively. Depending on the observer, the prevalence of LVH(WT) and LVH(MI) ranged from 2 to 30% and from 8 to 25%, respectively. Kappas ranged from 0.4 to 1.0 and from 0.1 to 0.5, for intra-and inter- observer reproducibility, respectively. CONCLUSIONS: Changes in diastolic wall thickness of less than 1.6 mm or LVMI less than 17.7 g/m(2) cannot be distinguished from measurement error in individual children, even when measured by the same observer. This limits the use of echocardiography to detect changes in wall thickness in children with ESRD in routine practice.

Published

2013

6. Phenotypic spectrum of the SMAD3-related aneurysms-osteoarthritis syndrome.

Author

Laar, I.M. van de, Linde, D. van der, Oei, E.H., Bos, P.K., Bessems, J.H., Bierma-Zeinstra, S.M., Meer, B.L. van, Pals, G., Oldenburg, R.A., Bekkers, J.A., Moelker, A., Graaf, B.M. de, Matyas, G., Frohn-Mulder, I.M., Timmermans, J., Hilhorst-Hofstee, Y., Cobben, J.M., Bruggenwirth, H.T., Laer, L. van, Loeys, B.L., Backer, J. de, Coucke, P.J., Dietz, H.C., Willems, P.J., Oostra, B.A., Paepe, A. de, Roos-Hesselink, J.W., Bertoli-Avella, A.M., Wessels, M.W., Laar, I.M. van de, Linde, D. van der, Oei, E.H., Bos, P.K., Bessems, J.H., Bierma-Zeinstra, S.M., Meer, B.L. van, Pals, G., Oldenburg, R.A., Bekkers, J.A., Moelker, A., Graaf, B.M. de, Matyas, G., Frohn-Mulder, I.M., Timmermans, J., Hilhorst-Hofstee, Y., Cobben, J.M., Bruggenwirth, H.T., Laer, L. van, Loeys, B.L., Backer, J. de, Coucke, P.J., Dietz, H.C., Willems, P.J., Oostra, B.A., Paepe, A. de, Roos-Hesselink, J.W., Bertoli-Avella, A.M., and Wessels, M.W.

Abstract

1 januari 2012, Item does not contain fulltext, BACKGROUND: Aneurysms-osteoarthritis syndrome (AOS) is a new autosomal dominant syndromic form of thoracic aortic aneurysms and dissections characterised by the presence of arterial aneurysms and tortuosity, mild craniofacial, skeletal and cutaneous anomalies, and early-onset osteoarthritis. AOS is caused by mutations in the SMAD3 gene. METHODS: A cohort of 393 patients with aneurysms without mutation in FBN1, TGFBR1 and TGFBR2 was screened for mutations in SMAD3. The patients originated from The Netherlands, Belgium, Switzerland and USA. The clinical phenotype in a total of 45 patients from eight different AOS families with eight different SMAD3 mutations is described. In all patients with a SMAD3 mutation, clinical records were reviewed and extensive genetic, cardiovascular and orthopaedic examinations were performed. RESULTS: Five novel SMAD3 mutations (one nonsense, two missense and two frame-shift mutations) were identified in five new AOS families. A follow-up description of the three families with a SMAD3 mutation previously described by the authors was included. In the majority of patients, early-onset joint abnormalities, including osteoarthritis and osteochondritis dissecans, were the initial symptom for which medical advice was sought. Cardiovascular abnormalities were present in almost 90% of patients, and involved mainly aortic aneurysms and dissections. Aneurysms and tortuosity were found in the aorta and other arteries throughout the body, including intracranial arteries. Of the patients who first presented with joint abnormalities, 20% died suddenly from aortic dissection. The presence of mild craniofacial abnormalities including hypertelorism and abnormal uvula may aid the recognition of this syndrome. CONCLUSION: The authors provide further insight into the phenotype of AOS with SMAD3 mutations, and present recommendations for a clinical work-up.

Published

2012

7. NPHP4 variants are associated with pleiotropic heart malformations.

Author

French, V.M., Laar, I.M. van de, Wessels, M.W., Rohe, C., Roos-Hesselink, J.W., Wang, G., Frohn-Mulder, I.M., Severijnen, L.A., Graaf, B.M. de, Schot, R., Breedveld, G., Mientjes, E., Tienhoven, M. van, Jadot, E., Jiang, Z., Verkerk, A., Swagemakers, S., Venselaar, H., Rahimi, Z., Najmabadi, H., Meijers-Heijboer, H., Graaff, E. de, Helbing, W.A., Willemsen, R., Devriendt, K., Belmont, J.W., Oostra, B.A., Amack, J.D., Bertoli-Avella, A.M., French, V.M., Laar, I.M. van de, Wessels, M.W., Rohe, C., Roos-Hesselink, J.W., Wang, G., Frohn-Mulder, I.M., Severijnen, L.A., Graaf, B.M. de, Schot, R., Breedveld, G., Mientjes, E., Tienhoven, M. van, Jadot, E., Jiang, Z., Verkerk, A., Swagemakers, S., Venselaar, H., Rahimi, Z., Najmabadi, H., Meijers-Heijboer, H., Graaff, E. de, Helbing, W.A., Willemsen, R., Devriendt, K., Belmont, J.W., Oostra, B.A., Amack, J.D., and Bertoli-Avella, A.M.

Abstract

Item does not contain fulltext, RATIONALE: Congenital heart malformations are a major cause of morbidity and mortality, especially in young children. Failure to establish normal left-right (L-R) asymmetry often results in cardiovascular malformations and other laterality defects of visceral organs. OBJECTIVE: To identify genetic mutations causing cardiac laterality defects. METHODS AND RESULTS: We performed a genome-wide linkage analysis in patients with cardiac laterality defects from a consanguineous family. The patients had combinations of defects that included dextrocardia, transposition of great arteries, double-outlet right ventricle, atrioventricular septal defects, and caval vein abnormalities. Sequencing of positional candidate genes identified mutations in NPHP4. We performed mutation analysis of NPHP4 in 146 unrelated patients with similar cardiac laterality defects. Forty-one percent of these patients also had laterality defects of the abdominal organs. We identified 8 additional missense variants that were absent or very rare in control subjects. To study the role of nphp4 in establishing L-R asymmetry, we used antisense morpholinos to knockdown nphp4 expression in zebrafish. Depletion of nphp4 disrupted L-R patterning as well as cardiac and gut laterality. Cardiac laterality defects were partially rescued by human NPHP4 mRNA, whereas mutant NPHP4 containing genetic variants found in patients failed to rescue. We show that nphp4 is involved in the formation of motile cilia in Kupffer's vesicle, which generate asymmetrical fluid flow necessary for normal L-R asymmetry. CONCLUSIONS: NPHP4 mutations are associated with cardiac laterality defects and heterotaxy. In zebrafish, nphp4 is essential for the development and function of Kupffer's vesicle cilia and is required for global L-R patterning.

Published

2012

8. Aggressive Cardiovascular Phenotype of Aneurysms-Osteoarthritis Syndrome Caused by Pathogenic SMAD3 Variants.

Author

Linde, D. van der, Laar, I.M. van de, Bertoli-Avella, A.M., Oldenburg, R.A., Bekkers, J.A., Mattace-Raso, F.U., Meiracker, A.H. van den, Moelker, A., Kooten, F. van, Frohn-Mulder, I.M., Timmermans, J., Moltzer, E., Cobben, J.M., Laer, L. van, Loeys, B.L., Backer, J. de, Coucke, P.J., Paepe, A. de, Hilhorst-Hofstee, Y., Wessels, M.W., Roos-Hesselink, J.W., Linde, D. van der, Laar, I.M. van de, Bertoli-Avella, A.M., Oldenburg, R.A., Bekkers, J.A., Mattace-Raso, F.U., Meiracker, A.H. van den, Moelker, A., Kooten, F. van, Frohn-Mulder, I.M., Timmermans, J., Moltzer, E., Cobben, J.M., Laer, L. van, Loeys, B.L., Backer, J. de, Coucke, P.J., Paepe, A. de, Hilhorst-Hofstee, Y., Wessels, M.W., and Roos-Hesselink, J.W.

Abstract

Item does not contain fulltext, OBJECTIVES: The purpose of this study was describe the cardiovascular phenotype of the aneurysms-osteoarthritis syndrome (AOS) and to provide clinical recommendations. BACKGROUND: AOS, caused by pathogenic SMAD3 variants, is a recently described autosomal dominant syndrome characterized by aneurysms and arterial tortuosity in combination with osteoarthritis. METHODS: AOS patients in participating centers underwent extensive cardiovascular evaluation, including imaging, arterial stiffness measurements, and biochemical studies. RESULTS: We included 44 AOS patients from 7 families with pathogenic SMAD3 variants (mean age: 42 +/- 17 years). In 71%, an aortic root aneurysm was found. In 33%, aneurysms in other arteries in the thorax and abdomen were diagnosed, and in 48%, arterial tortuosity was diagnosed. In 16 patients, cerebrovascular imaging was performed, and cerebrovascular abnormalities were detected in 56% of them. Fifteen deaths occurred at a mean age of 54 +/- 15 years. The main cause of death was aortic dissection (9 of 15; 60%), which occurred at mildly increased aortic diameters (range: 40 to 63 mm). Furthermore, cardiac abnormalities were diagnosed, such as congenital heart defects (6%), mitral valve abnormalities (51%), left ventricular hypertrophy (19%), and atrial fibrillation (22%). N-terminal brain natriuretic peptide (NT-proBNP) was significantly higher in AOS patients compared with matched controls (p < 0.001). Aortic pulse wave velocity was high-normal (9.2 +/- 2.2 m/s), indicating increased aortic stiffness, which strongly correlated with NT-proBNP (r = 0.731, p = 0.005). CONCLUSIONS: AOS predisposes patients to aggressive and widespread cardiovascular disease and is associated with high mortality. Dissections can occur at relatively mildly increased aortic diameters; therefore, early elective repair of the ascending aorta should be considered. Moreover, cerebrovascular abnormalities were encountered in most patients.

Published

2012

9. 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

10. Effect of enzyme therapy in juvenile patients with Pompe disease: a three-year open-label study.

Author

Capelle, C.I. van, Beek, N.A. van der, Hagemans, M.L., Arts, W.F.M., Hop, W.C.J., Lee, P., Jaeken, J., Frohn-Mulder, I.M., Merkus, P.J.F.M., Corzo, D., Puga, A.C., Reuser, A.J.J., Ploeg, A.T. van der, Capelle, C.I. van, Beek, N.A. van der, Hagemans, M.L., Arts, W.F.M., Hop, W.C.J., Lee, P., Jaeken, J., Frohn-Mulder, I.M., Merkus, P.J.F.M., Corzo, D., Puga, A.C., Reuser, A.J.J., and Ploeg, A.T. van der

Abstract

1 december 2010, Contains fulltext : 88739.pdf (publisher's version ) (Closed access), Pompe disease is a rare neuromuscular disorder caused by deficiency of acid alpha-glucosidase. Treatment with recombinant human alpha-glucosidase recently received marketing approval based on prolonged survival of affected infants. The current open-label study was performed to evaluate the response in older children (age 5.9-15.2 years). The five patients that we studied had limb-girdle muscle weakness and three of them also had decreased pulmonary function in upright and supine position. They received 20-mg/kg recombinant human alpha-glucosidase every two weeks over a 3-year period. No infusion-associated reactions were observed. Pulmonary function remained stable (n = 4) or improved slightly (n = 1). Muscle strength increased. Only one patient approached the normal range. Patients obtained higher scores on the Quick Motor Function Test. None of the patients deteriorated. Follow-up data of two unmatched historical cohorts of adults and children with Pompe disease were used for comparison. They showed an average decline in pulmonary function of 1.6% and 5% per year. Data on muscle strength and function of untreated children were not available. Further studies are required.

Published

2010

11. Poor outcome in Down syndrome fetuses with cardiac anomalies or growth retardation.

Author

Wessels, M.W., Los, F.J., Frohn-Mulder, I.M., Niermeijer, M.F., Willems, P.J., Wladimiroff, J.W., Wessels, M.W., Los, F.J., Frohn-Mulder, I.M., Niermeijer, M.F., Willems, P.J., and Wladimiroff, J.W.

Abstract

Contains fulltext : 186384.pdf (Publisher’s version ) (Closed access), The outcome of Down syndrome fetuses presenting with sonographic abnormalities in the second or third trimester is unclear. Therefore, we studied 55 pregnancies referred because of sonographically suspected fetal structural anomalies or growth retardation due to trisomy 21. A detailed ultrasound scan was performed in all cases to delineate the structural anomalies. Congenital heart malformations (CHMs) were diagnosed pre- and postnatally in 29 out of 55 Down fetuses (53%), with complete or incomplete atrioventricular septal defects (AVSDs) and ventricular septal defects (VSDs) being the most frequent anomalies. The most frequent noncardiac findings were a short femur (45%) and a small-for-gestational age (SGA) fetus (27%). Termination of pregnancy was carried out in 25 out of 55 pregnancies (45%). Of the 30 continued pregnancies, 10 ended with intrauterine death. The remaining 20 pregnancies resulted in the delivery of a live-born infant whose prognosis was poor, with a 1-year survival of only 60%. Combining intrauterine death and death in the first year indicated that the overall survival rate was only 40%. Fatal outcome was noted in 68% (13/19) in the presence of CHM, in 83% (10/12) in SGA fetuses, in 86% (6/7) in combined CHM and SGA, but only in 17% (1/6) in the absence of CHM and SGA. This study indictes that second- and third-trimester in utero diagnosis of Down syndrome has a poor outcome when associated with CHM and/or SGA. This is important in the genetic counseling of the parents.

Published

2003