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1. Incidence and outcome of acquired demyelinating syndromes in Dutch children: update of a nationwide and prospective study

Author

Mol, Louk, Wong, Yu Yi, van Pelt - T Gravesteijn, Elles, Ketelslegers, IA, Bakker, DP, Boon, M, Braun, KPJ, van Dijk, KGJ, Eikelenboom, MJ, Engelen, MP, Geleijns, K, Haaxma, C A, Niermeijer, JMF, Niks, EH, Peeters, EAJ, Peeters-Scholte, C, Poll-The, BT, Portier, RP, De Rijk-Van Andel, JF, Samijn, JPA, Schippers, HM, Snoeck, IN, Stroink, H, Vermeulen, RJ, Verrips, A, Visscher, F, Vles, JSH, Willemsen, M, Catsman - Berrevoets, Coriene, Hintzen, Rogier, Neuteboom, Rinze, Mol, Louk, Wong, Yu Yi, van Pelt - T Gravesteijn, Elles, Ketelslegers, IA, Bakker, DP, Boon, M, Braun, KPJ, van Dijk, KGJ, Eikelenboom, MJ, Engelen, MP, Geleijns, K, Haaxma, C A, Niermeijer, JMF, Niks, EH, Peeters, EAJ, Peeters-Scholte, C, Poll-The, BT, Portier, RP, De Rijk-Van Andel, JF, Samijn, JPA, Schippers, HM, Snoeck, IN, Stroink, H, Vermeulen, RJ, Verrips, A, Visscher, F, Vles, JSH, Willemsen, M, Catsman - Berrevoets, Coriene, Hintzen, Rogier, and Neuteboom, Rinze

Published
2018

3. Position statement on the role of healthcare professionals, patient organizations and industry in European Reference Networks

Author

Hollak, CEM, Biegstraaten, M, Baumgartner, MR, Belmatoug, N, Bembi, B, Bosch, A, Brouwers, M, Dekker, H, Dobbelaere, D, Engelen, M, Groenendijk, M C, Lachmann, R, Langendonk, Janneke, Langeveld, Mirjam, Linthorst, G, Morava, E, Poll-The, BT, Rahman, S, Rubio-Gozalbo, ME, Spiekerkoetter, U, Treacy, E, Wanders, R, Zschocke, J, Hagendijk, R, Hollak, CEM, Biegstraaten, M, Baumgartner, MR, Belmatoug, N, Bembi, B, Bosch, A, Brouwers, M, Dekker, H, Dobbelaere, D, Engelen, M, Groenendijk, M C, Lachmann, R, Langendonk, Janneke, Langeveld, Mirjam, Linthorst, G, Morava, E, Poll-The, BT, Rahman, S, Rubio-Gozalbo, ME, Spiekerkoetter, U, Treacy, E, Wanders, R, Zschocke, J, and Hagendijk, R

Published
2016

4. Diagnostic work-up in acute conditions of inborn errors of metabolism and storage diseases

Author

Valayannopoulos and Poll-The Bt

Subjects
medicine.medical_specialty, Diagnostic methods, business.industry, medicine, Signs and symptoms, PROGRESSIVE SYMPTOMS, Early infancy, Intensive care medicine, business, Work-up, Biochemical markers, Surgery
Abstract

Inborn errors of metabolism may present with acute neurological symptoms at any age. However, especially in neonates and infants, these conditions may be acute and if untreated may lead to permanent cerebral lesions or to death. Knowledge of the main signs and symptoms of these conditions may be lifesaving, especially for conditions that are treatable. From the pathophysiological perspective, errors of metabolism can be divided into disorders causing “intoxication,” disorders impairing energy production, and disorders involving complex molecules. From the clinical perspective, errors of metabolism may present with acute symptoms in the neonatal period and early infancy; late-onset acute and recurrent attacks; chronic and progressive symptoms. Nonspecific readily available biochemical markers may suggest the underlying condition but in most cases the choice of appropriate biochemical and molecular tests is required to establish the diagnosis. Progress in the treatment of inborn errors of metabolism has been slower than progress in diagnostic methods and in understanding of the pathophysiology of these disorders. Nevertheless, outcomes are improving with the use of dialysis and drugs to promote the removal of toxic metabolites and measures to keep catabolism to a minimum. Early intervention is crucial when neurological sequelae could be avoided, which requires constant vigilance and routine measurement of diagnostic biochemical markers in suspected cases.

Published
2013
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5. Clinical, neuroradiological and genetic findings in pontocerebellar hypoplasia

Author

Namavar, Y, Barth, Pg, Kasher, Pr, van Ruissen, F, Brockmann, K, Bernert, G, Writzl, K, Ventura, K, Cheng, Ey, Ferriero, Dm, Basel-Vanagaite, L, Eggens, Vr, Krägeloh-Mann, I, De Meirleir, L, King, M, Graham JM Jr, von Moers, A, Knoers, N, Sztriha, L, Korinthenberg, R, Dobyns, Wb, Baas, F, Poll-The, Bt, Pch, Consortium, and Battini, R

Published
2011

6. Impaired Visual Integration in Children with Traumatic Brain Injury: An Observational Study

Author

Konigs, M, Weeda, WD, van Heurn, LWE, Vermeulen, Joyce, Goslings, JC, Luitse, JSK, Poll-The, BT, Beelen, A, van der Wees, M, Kemps, RJJK, Catsman - Berrevoets, Coriene, Oosterlaan, J, Konigs, M, Weeda, WD, van Heurn, LWE, Vermeulen, Joyce, Goslings, JC, Luitse, JSK, Poll-The, BT, Beelen, A, van der Wees, M, Kemps, RJJK, Catsman - Berrevoets, Coriene, and Oosterlaan, J

Abstract

Background Axonal injury after traumatic brain injury (TBI) may cause impaired sensory integration. We aim to determine the effects of childhood TBI on visual integration in relation to general neurocognitive functioning. Methods We compared children aged 6-13 diagnosed with TBI (n = 103; M = 1.7 years post-injury) to children with traumatic control (TC) injury (n = 44). Three TBI severity groups were distinguished: mild TBI without risk factors for complicated TBI (mild(RF-)TBI, n = 22), mild TBI with >= 1 risk factor (mild(RF+) TBI, n = 46) or moderate/severe TBI (n = 35). An experimental paradigm measured speed and accuracy of goal-directed behavior depending on: (1) visual identification; (2) visual localization; or (3) both, measuring visual integration. Group-differences on reaction time (RT) or accuracy were tracked down to task strategy, visual processing efficiency and extra-decisional processes (e.g. response execution) using diffusion model analysis. General neurocognitive functioning was measured by a Wechsler Intelligence Scale short form. Results The TBI group had poorer accuracy of visual identification and visual integration than the TC group (Ps <= .03; ds <= -0.40). Analyses differentiating TBI severity revealed that visual identification accuracy was impaired in the moderate/severe TBI group (P = .05, d = -0.50) and that visual integration accuracy was impaired in the mild(RF+) TBI group and moderate/severe TBI group (Ps < .02, ds <= -0.56). Diffusion model analyses tracked impaired visual integration accuracy down to lower visual integration efficiency in the mild(RF+) TBI group and moderate/severe TBI group (Ps < .001, ds <= -0.73). Importantly, intelligence impairments observed in the TBI group (P = .009, d = -0.48) were statistically explained by visual integration efficiency (P = .002). Conclusions Children with mild(RF+) TBI or moderate/severe TBI have impaired visual integration efficiency, which may contribute to poore

Published
2015

8. Genetic basis of hyperlysinemia

Author

Houten, SM, te Brinke, H, Denis, S, Ruiter, JPN, Knegt, AC, Klerk, Hans, Augoustides-Savvopoulou, P, Haberle, J, Baumgartner, MR, Coskun, T, Zschocke, J, Sass, JO, Poll-The, BT, Wanders, RJA, Duran, M (Mercedes), Houten, SM, te Brinke, H, Denis, S, Ruiter, JPN, Knegt, AC, Klerk, Hans, Augoustides-Savvopoulou, P, Haberle, J, Baumgartner, MR, Coskun, T, Zschocke, J, Sass, JO, Poll-The, BT, Wanders, RJA, and Duran, M (Mercedes)

Published
2013

9. Clinical and molecular variability in childhood periodic fever with hyperimmunoglobulinaemia D

Author

Frenkel, J, Houten, SM, Waterham, HR, Rijkers, GT, Duran, M, Kuijpers, TW, van Luijk, W, Poll-The, BT, Kuis, W, and Faculteit Medische Wetenschappen/UMCG

Subjects
fever, mevalonic acid, familial Mediterranean fever, mevalonate kinase, MUTATIONS, KINASE, IgD, periodicity, hypergammaglobulinaemia, MEVALONIC ACIDURIA
Abstract

Objectives. The hyperimmunoglobulinaemia D and periodic fever syndrome (HIDS) was found recently to be caused by a deficiency of mevalonate kinase (MK). The aim of this study was to examine whether a relationship exists between the clinical expression of HIDS and the extent of MK deficiency. Methods. The medical records of children diagnosed with HIDS were reviewed for clinical features and serum immunoglobulin values. The mevalonic acid excretion in urine and MK enzyme activity in patients' cells were measured and the cDNA of the MVK gene was sequenced. Results. Fifteen patients with recurrent fever and raised serum immunoglobulin (Ig) D were included. Their clinical features varied. Eleven patients had a deficiency of MK, caused by mutations in the MVK gene. One mutation (V377I) was common to all 11 patients. Nine patients were compound heterozygotes for V377I and various other MVK mutations. There was no apparent relationship between the observed mutations and the clinical features. Surprisingly, four boys had normal MK activity and no MVK mutations. Conclusions. Most HIDS patients have mutations in the MVK gene. The clinical variability observed cannot be explained by genotypic differences. Periodic fever and elevated IgD can result from other, still unknown, causes. Hence, testing for MK deficiency is necessary in patients with unexplained periodic fever.

Published
2001

10. Incidence of acquired demyelinating syndromes of the CNS in Dutch children: a nationwide study

Author

Ketelslegers, Immy, Catsman - Berrevoets, Coriene, Neuteboom, Rinze, Boon, M, van Dijk, KGJ, Eikelenboom, MJ, Gooskens, RHJM, Niks, EH (Erik), Overweg-Plandsoen, WCG, Peeters, EAJ, Peeters-Scholte, CMPCD, Poll-The, BT, De Rijk-Van Andel, JF, Samijn, JPA, Snoeck, IN, Stroink, H (Hans), Vermeulen, RJ, Verrips, A, Vles, JSH, Willemsen, MAAP, Pereira, RR, Hintzen, Rogier, Ketelslegers, Immy, Catsman - Berrevoets, Coriene, Neuteboom, Rinze, Boon, M, van Dijk, KGJ, Eikelenboom, MJ, Gooskens, RHJM, Niks, EH (Erik), Overweg-Plandsoen, WCG, Peeters, EAJ, Peeters-Scholte, CMPCD, Poll-The, BT, De Rijk-Van Andel, JF, Samijn, JPA, Snoeck, IN, Stroink, H (Hans), Vermeulen, RJ, Verrips, A, Vles, JSH, Willemsen, MAAP, Pereira, RR, and Hintzen, Rogier

Abstract

Acquired demyelinating syndromes (ADS) can be a first presentation of multiple sclerosis (MS) in children. The incidence of these disorders in Europe is currently unknown. Children (< 18 years old) living in the Netherlands who presented with ADS were included from January 1, 2007 to December 31, 2010 by the Dutch pediatric MS study group and the Dutch surveillance of rare pediatric disorders. Demographic and clinical data were collected. Eighty-six patients were identified over 4 years, resulting in an incidence of 0.66/1,00,000 per year. Most patients presented with polyfocal ADS without encephalopathy (30%), followed by polyfocal ADS with encephalopathy (24%), optic neuritis (ON, 22%), monofocal ADS (16%), transverse myelitis (3%), and neuromyelitis optica (3%). Patients with polyfocal ADS with encephalopathy were younger (median 3.9 years) than patients with ON (median 14.6 years, p < 0.001) or monofocal ADS (median 16.0 years, p < 0.001). Patients with polyfocal ADS without encephalopathy (median 9.2 years) were also younger than monofocal ADS patients (median 16.0 years, p < 0.001). There was a slight female preponderance in all groups except the ON group, and a relatively large number of ADS patients (29%) reported a non-European ancestry. Familial autoimmune diseases were reported in 23%, more often in patients with relapsing disease than monophasic disease (46 vs. 15%, p = 0.002) and occurring most often in the maternal family (84%, p < 0.001). During the study period, 23% of patients were subsequently diagnosed with MS. The annual incidence of ADS in the Netherlands is 0.66/1,00,000 children/year. A polyfocal disease onset of ADS was most common.

Published
2012

16. The natural course of infantile Pompe's disease: 20 original cases compared with 133 cases from the literature

Author

van den Hout, Hannerieke, Hop, Wim C.J., Diggelen, Otto, Smeitink, JAM, Smit, GPA, Poll-The, BT, Bakker, HD, Loonen, MCB (Christa), Klerk, Hans, Reuser, Arnold, van der Ploeg, Ans, van den Hout, Hannerieke, Hop, Wim C.J., Diggelen, Otto, Smeitink, JAM, Smit, GPA, Poll-The, BT, Bakker, HD, Loonen, MCB (Christa), Klerk, Hans, Reuser, Arnold, and van der Ploeg, Ans

Published
2003

17. Congenital microcephaly and seizures due to 3-phosphoglycerate dehydrogenase deficiency: Outcome of treatment with amino acids

Author

UCL, De Koning, TJ, Duran, M., Van Maldergem, L., Pineda, M, Dorland, L, Gooskens, R, Jaeken, J., Poll-The, BT, UCL, De Koning, TJ, Duran, M., Van Maldergem, L., Pineda, M, Dorland, L, Gooskens, R, Jaeken, J., and Poll-The, BT

Abstract

Congenital microcephaly, intractable seizures and severe psycho-motor retardation characterize 3-phosphoglycerate dehydrogenase (3-PGDH) deficiency, a disorder of L-serine biosynthesis. The enzyme defect results in low concentrations of serine and to a variable degree of glycine in plasma and cerebrospinal fluid. Short-term beneficial effects have been reported of oral treatment with the deficient amino acids. In this paper, we report the first follow-up data of amino acid therapy in five patients treated for 3-7.5 years. Different treatment regimes were used, but a favourable response to amino acids was observed in all patients. A major reduction in seizure frequency occurred in all patients; two patients became free of seizures. Amino acids were well tolerated and no adverse effects were documented. A progress of psychomotor development was only observed in one patient, diagnosed early and treated with a high dosage of L-serine. A favourable outcome of 3-PGDH deficiency depends on early diagnosis and treatment.

Published
2002

18. Hypomyelination and reversible white matter attenuation in 3-phosphoglycerate dehydrogenase deficiency

Author

UCL, de Koning, TJ, Jaeken, J., Pineda, M, Van Maldergem, L., Poll-The, BT, van der Knaap, MS, UCL, de Koning, TJ, Jaeken, J., Pineda, M, Van Maldergem, L., Poll-The, BT, and van der Knaap, MS

Abstract

White matter abnormalities are a feature of many inborn errors of metabolism and magnetic resonance imaging (MRI) of the brain has become an important tool in the diagnostic workup of these disorders. Recently, patients were reported with a potentially treatable disorder of serine biosynthesis. They presented with congenital microcephaly, severe psychomotor retardation and intractable seizures. Low concentrations of the amino acids serine, glycine as well as 5-methyltetrahydrofolate were found in plasma and CSF and were due to a deficiency of the enzyme 3-phosphoglycerate dehydrogenase (3-PGDH). We studied four patients aged 10 months to 7 years by MRI before and after treatment with amino acids with a follow-up of 16 months to 6 years. Magnetic resonance spectroscopy (MRS) was performed in two patients at 4 and 16 months of treatment. Pre-treatment MRI demonstrated hypomyelination and profound white matter attenuation in all patients. During treatment, a significant increase in white matter volume was found and a progress of myelination in two patients. The most striking finding on MRS during treatment was an elevated level of white matter choline. Serine biosynthesis defects have to be considered in the differential diagnosis of patients with mental retardation, microcephaly, seizures, and on MRI hypomyelination and white matter attenuation.

Published
2000

19. Molecular characterization of 3-phosphoglycerate dehydrogenase deficiency - A neurometabolic disorder associated with reduced L-serine biosynthesis

Author

UCL, Klomp, LWJ, de Koning, TJ, Malingre, HEM, van Beurden, EACM, Brink, M, Opdam, FL, Duran, M., Jaeken, J., Pineda, M, Van Maldergem, L., Poll-The, BT, van den Berg, IET, Berger, R., UCL, Klomp, LWJ, de Koning, TJ, Malingre, HEM, van Beurden, EACM, Brink, M, Opdam, FL, Duran, M., Jaeken, J., Pineda, M, Van Maldergem, L., Poll-The, BT, van den Berg, IET, and Berger, R.

Abstract

3-phosphoglycerate dehydrogenase (PHGDH) deficiency is a disorder of L-serine biosynthesis that is characterized by congenital microcephaly, psychomotor retardation, and seizures. To investigate the molecular basis for this disorder, the PHGDH mRNA sequence was characterized, and six patients from four families were analyzed for sequence variations. Five patients from three different families were homozygous for a single nucleotide substitution predicted to change valine at position 490 to methionine. The sixth patient was homozygous for a valine to methionine substitution at position 425; both mutations are located in the carboxyterminal part of PHGDH. In vitro expression of these mutant proteins resulted in significant reduction of PHGDH enzyme activities. RNA-blot analysis indicated abundant expression of PHGDH in adult and fetal brain tissue. Taken together with the severe neurological impairment in our patients, the data presented in this paper suggest an important role for PHGDH activity and L-serine biosynthesis in the metabolism, development, and function of the central nervous system.

Published
2000

26. Hyperhomocyst(e)inaemia in children with chronic renal failure.

Author

Lilien, M, Duran, M, Van Hoeck, K, Poll-The, BT, and Schröder, C

Abstract

Background: Hyperhomocyst(e)inaemia has been identified as a significant risk factor for the occurrence of atherosclerosis in adults with chronic renal failure. Because of its presumed direct toxic effect on the vascular wall, long-standing hyperhomocyst(e)inaemia in children with chronic renal failure might have an important influence on their risk of future development of atherosclerosis. Hitherto no data on hyperhomocyst(e)inaemia in children with renal failure have been published. [ABSTRACT FROM PUBLISHER]

Published
1999
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28. Redefining the phenotype of alpha-methylacyl-CoA racemase (AMACR) deficiency.

Author

Klouwer FCC, Roosendaal SD, Hollak CEM, Langeveld M, Poll-The BT, Sorge AJV, Wolf NI, Knaap MSV, and Engelen M

Subjects
Humans, Male, Adult, Female, Child, Middle Aged, Aged, Child, Preschool, Young Adult, Adolescent, Racemases and Epimerases deficiency, Racemases and Epimerases genetics, Racemases and Epimerases metabolism, Phenotype
Abstract

Background: Alpha-methylacyl-CoA racemase (AMACR) deficiency is a rare peroxisomal enzyme deficiency caused by biallelic variants in the AMACR gene. This deficiency leads to the accumulation of toxic bile acid intermediates (R)-trihydroxycholestenoic acid (THCA) and (R)-dihydroxycholestenoic acid (DHCA) and pristanic acid. With less than 20 patients described in literature, the phenotype of AMACR deficiency is poorly defined and no data on the natural history are available., Results: Here we describe a cohort of 12 patients (9 adults and 3 children) with genetically confirmed AMACR deficiency (median age at diagnosis 56 years, range 3-69), followed for an average of 6 years (between 2015 and 2023). Five novel pathogenic variants are described. In 5/9 adult patients, retinitis pigmentosa was detected at a median age of 45 years (range 30-61). The median delay to diagnosis of AMACR deficiency after the diagnosis of retinitis pigmentosa was 24 years (range 0-33). All adult patients subsequently developed neurological signs and symptoms after the age of 40 years; most frequently neuropathy, ataxia and cognitive decline with prior normal cognitive functioning. One patient presented with a stroke-like episode. All adult patients showed a typical MRI pattern involving the thalami and gray matter structures of the pons and midbrain. One patient had a hepatocellular carcinoma at the time of the AMACR deficiency diagnosis and two patients suffered from gallstones. All three included children had elevated liver transaminases as single presenting sign and showed no brain MRI abnormalities., Conclusion: AMACR deficiency can be considered as an adult slowly progressive disease with a predominant neurological phenotype. The main signs comprise retinitis pigmentosa, neuropathy, ataxia and cognitive decline; stroke-like episodes may occur. Recognition of typical MRI abnormalities may facilitate prompt diagnosis. In addition, there is a risk of liver fibrosis/cirrhosis and hepatocellular carcinoma in these patients, requiring active monitoring., (© 2024. The Author(s).)

Published
2024
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29. Clinical, biochemical, and molecular characterization of mild (nonclassic) rhizomelic chondrodysplasia punctata.

Author

Fallatah W, Schouten M, Yergeau C, Di Pietro E, Engelen M, Waterham HR, Poll-The BT, and Braverman N

Subjects
Adolescent, Adult, Child, Child, Preschool, Chondrodysplasia Punctata, Rhizomelic genetics, Female, Humans, Male, Young Adult, Chondrodysplasia Punctata, Rhizomelic diagnosis, Genetic Association Studies, Growth Charts
Abstract

Rhizomelic chondrodysplasia punctata (RCDP) is a heterogenous group of disorders due to defects in genes encoding peroxisomal proteins required for plasmalogen (PL) biosynthesis, specifically PEX7 and PEX5 receptors, or GNPAT, AGPS and FAR1 enzymes. Most patients have congenital cataract and skeletal dysplasia. In the classic form, there is profound growth restriction and psychomotor delays, with most patients not advancing past infantile developmental milestones. Disease severity correlates to erythrocyte PL levels, which are almost undetectable in severe (classic) RCDP. In milder (nonclassic) forms, residual PL levels are associated with improved growth and development. However, the clinical course of this milder group remains largely unknown as only a few cases were reported. Using as inclusion criteria the ability to communicate and walk, we identified 16 individuals from five countries, ages 5-37 years, and describe their clinical, biochemical and molecular profiles. The average age at diagnosis was 2.6 years and most had cataract, growth deficiency, joint contractures, and developmental delays. Other major symptoms were learning disability (87%), behavioral issues (56%), seizures (43%), and cardiac defects (31%). All patients had decreased C16:0 PL levels that were higher than in classic RCDP, and up to 43% of average controls. Plasma phytanic acid levels were elevated in most patients. There were several common, and four novel, PEX7, and GNPAT hypomorphic alleles in this cohort. These results can be used to support earlier diagnosis and improve management in patients with mild RCDP., (© 2020 SSIEM.)

Published
2021
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30. Postnatal Brain Growth Patterns in Pontocerebellar Hypoplasia.

Author

van Dijk T, Barth P, Baas F, Reneman L, and Poll-The BT

Subjects
Brain diagnostic imaging, Brain pathology, Cerebellum pathology, Humans, Infant, Newborn, Magnetic Resonance Imaging, Cerebellar Diseases diagnostic imaging, Cerebellar Diseases pathology, Olivopontocerebellar Atrophies diagnostic imaging, Olivopontocerebellar Atrophies pathology
Abstract

Background: Pontocerebellar hypoplasia (PCH) is a rare group of disorders mainly affecting the cerebellum and pons. Supratentorial structures are variably involved. We assessed brain growth patterns in patients with the most frequent forms of PCH, namely PCH1B (OMIM#614678) and PCH2A (OMIM#277470), since in these types of PCH, pre- and postnatal neurodegeneration is established by neuropathological profiling. To assess the influence of the different pathomechanisms on postnatal growth patterns, we included CASK- associated microcephaly and PCH (MICPCH, OMIM#300749) patients in our analyses, as MICPH mimics PCH on magnetic resonance imaging (MRI) but represents a developmental disorder including abnormal neuronal migration., Methods: A total of 66 patients were included: 9 patients with PCH1B, 18 patients with PCH2A, 6 patients with MICPCH, and 33 age- and gender-matched hospital-based controls. Segmentation of the vermis and cerebellum was performed manually, as were measurements of the thickness of the head of the caudate nucleus, the width of the anterior horn, and lateral ventricle size., Results: The cerebellum was severely hypoplastic at birth in all patients, and postnatal growth was nearly absent. In patients with PCH1B/2A, we found relative sparing of the vermis compared with the cerebellar hemispheres. In addition, PCH1B and PCH2A cases demonstrated thinning of the head of the caudate nucleus, an associated increase in anterior horn width, and an increase in lateral ventricle size. None of these features were seen in the MICPCH group., Conclusions: Our findings confirm the progressive nature including caudate nucleus atrophy in PCH1B and PCH2A. In MICPCH, the relative sparing of supratentorial structures confirms its different pathomechanism., Competing Interests: The authors declare that they have no competing interests., (Thieme. All rights reserved.)

Published
2021
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31. Endocrine and Growth Abnormalities in 4H Leukodystrophy Caused by Variants in POLR3A, POLR3B, and POLR1C.

Author

Pelletier F, Perrier S, Cayami FK, Mirchi A, Saikali S, Tran LT, Ulrick N, Guerrero K, Rampakakis E, van Spaendonk RML, Naidu S, Pohl D, Gibson WT, Demos M, Goizet C, Tejera-Martin I, Potic A, Fogel BL, Brais B, Sylvain M, Sébire G, Lourenço CM, Bonkowsky JL, Catsman-Berrevoets C, Pinto PS, Tirupathi S, Strømme P, de Grauw T, Gieruszczak-Bialek D, Krägeloh-Mann I, Mierzewska H, Philippi H, Rankin J, Atik T, Banwell B, Benko WS, Blaschek A, Bley A, Boltshauser E, Bratkovic D, Brozova K, Cimas I, Clough C, Corenblum B, Dinopoulos A, Dolan G, Faletra F, Fernandez R, Fletcher J, Garcia Garcia ME, Gasparini P, Gburek-Augustat J, Gonzalez Moron D, Hamati A, Harting I, Hertzberg C, Hill A, Hobson GM, Innes AM, Kauffman M, Kirwin SM, Kluger G, Kolditz P, Kotzaeridou U, La Piana R, Liston E, McClintock W, McEntagart M, McKenzie F, Melançon S, Misbahuddin A, Suri M, Monton FI, Moutton S, Murphy RPJ, Nickel M, Onay H, Orcesi S, Özkınay F, Patzer S, Pedro H, Pekic S, Pineda Marfa M, Pizzino A, Plecko B, Poll-The BT, Popovic V, Rating D, Rioux MF, Rodriguez Espinosa N, Ronan A, Ostergaard JR, Rossignol E, Sanchez-Carpintero R, Schossig A, Senbil N, Sønderberg Roos LK, Stevens CA, Synofzik M, Sztriha L, Tibussek D, Timmann D, Tonduti D, van de Warrenburg BP, Vázquez-López M, Venkateswaran S, Wasling P, Wassmer E, Webster RI, Wiegand G, Yoon G, Rotteveel J, Schiffmann R, van der Knaap MS, Vanderver A, Martos-Moreno GÁ, Polychronakos C, Wolf NI, and Bernard G

Subjects
Adolescent, Adult, Biological Variation, Population, Child, Child, Preschool, Cohort Studies, Cross-Sectional Studies, Endocrine System Diseases epidemiology, Endocrine System Diseases etiology, Female, Genetic Heterogeneity, Growth Disorders epidemiology, Growth Disorders etiology, Hereditary Central Nervous System Demyelinating Diseases complications, Hereditary Central Nervous System Demyelinating Diseases epidemiology, Humans, Hypogonadism epidemiology, Hypogonadism etiology, Infant, Infant, Newborn, Male, Mitochondrial Diseases complications, Mitochondrial Diseases epidemiology, Mutation, RNA Polymerase III genetics, Retrospective Studies, Young Adult, DNA-Directed RNA Polymerases genetics, Endocrine System Diseases genetics, Growth Disorders genetics, Hereditary Central Nervous System Demyelinating Diseases genetics, Mitochondrial Diseases genetics
Abstract

Context: 4H or POLR3-related leukodystrophy is an autosomal recessive disorder typically characterized by hypomyelination, hypodontia, and hypogonadotropic hypogonadism, caused by biallelic pathogenic variants in POLR3A, POLR3B, POLR1C, and POLR3K. The endocrine and growth abnormalities associated with this disorder have not been thoroughly investigated to date., Objective: To systematically characterize endocrine abnormalities of patients with 4H leukodystrophy., Design: An international cross-sectional study was performed on 150 patients with genetically confirmed 4H leukodystrophy between 2015 and 2016. Endocrine and growth abnormalities were evaluated, and neurological and other non-neurological features were reviewed. Potential genotype/phenotype associations were also investigated., Setting: This was a multicenter retrospective study using information collected from 3 predominant centers., Patients: A total of 150 patients with 4H leukodystrophy and pathogenic variants in POLR3A, POLR3B, or POLR1C were included., Main Outcome Measures: Variables used to evaluate endocrine and growth abnormalities included pubertal history, hormone levels (estradiol, testosterone, stimulated LH and FSH, stimulated GH, IGF-I, prolactin, ACTH, cortisol, TSH, and T4), and height and head circumference charts., Results: The most common endocrine abnormalities were delayed puberty (57/74; 77% overall, 64% in males, 89% in females) and short stature (57/93; 61%), when evaluated according to physician assessment. Abnormal thyroid function was reported in 22% (13/59) of patients., Conclusions: Our results confirm pubertal abnormalities and short stature are the most common endocrine features seen in 4H leukodystrophy. However, we noted that endocrine abnormalities are typically underinvestigated in this patient population. A prospective study is required to formulate evidence-based recommendations for management of the endocrine manifestations of this disorder., (© The Author(s) 2020. Published by Oxford University Press on behalf of the Endocrine Society.)

Published
2021
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34. Rhizomelic chondrodysplasia punctata morbidity and mortality, an update.

Author

Duker AL, Niiler T, Kinderman D, Schouten M, Poll-The BT, Braverman N, and Bober MB

Subjects
Child, Child, Preschool, Chondrodysplasia Punctata, Rhizomelic diagnostic imaging, Chondrodysplasia Punctata, Rhizomelic pathology, Female, Humans, Infant, Infant, Newborn, Morbidity, Pregnancy, Ultrasonography, Prenatal, Chondrodysplasia Punctata, Rhizomelic genetics, Chondrodysplasia Punctata, Rhizomelic mortality
Published
2020
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35. Optical coherence tomography shows neuroretinal thinning in myelopathy of adrenoleukodystrophy.

Author

van Ballegoij WJC, Kuijpers SC, Huffnagel IC, Weinstein HC, Poll-The BT, Engelen M, Bennebroek CAM, and Verbraak FD

Subjects
Adrenoleukodystrophy complications, Adult, Cross-Sectional Studies, Female, Humans, Image Interpretation, Computer-Assisted methods, Male, Middle Aged, Nerve Degeneration diagnostic imaging, Nerve Degeneration etiology, Neuroimaging methods, Retina pathology, Spinal Cord Diseases etiology, Adrenoleukodystrophy diagnostic imaging, Retina diagnostic imaging, Spinal Cord Diseases diagnostic imaging, Tomography, Optical Coherence methods
Abstract

Background: Progressive myelopathy is the main cause of disability in adrenoleukodystrophy (ALD). Development of therapies is hampered by a lack of quantitative outcome measures. In this study, we investigated whether myelopathy in ALD is associated with retinal neurodegeneration on optical coherence tomography (OCT), which could serve as a surrogate outcome measure., Methods: Sixty-two patients (29 men and 33 women) and 70 age-matched and sex-matched controls (33 men and 37 women) were included in this cross-sectional study. We compared retinal nerve fiber layer (RNFL), ganglion cell layer (GCL) and peripapillary retinal nerve fiber layer (pRNFL) thickness between ALD patients and controls. In addition, we correlated these OCT measurements with clinical parameters of severity of myelopathy., Results: Patients had significantly thinner RNFL (male group, p < 0.05) and pRNFL superior and temporal quadrant [both male (p < 0.005) and female (p < 0.05) groups] compared to controls. Comparing three groups (symptomatic patients, asymptomatic patients and controls), there were significant differences in RNFL thickness (total grid and peripheral ring) in the male group (p ≤ 0.002) and in pRNFL thickness (superior and temporal quadrant) in both male (p ≤ 0.02) and the female (p ≤ 0.02) groups. Neuroretinal layer thickness correlated moderately with severity of myelopathy in men (correlation coefficients between 0.29-0.55, p < 0.02), but not in women., Conclusions: These results suggest that neurodegeneration of the spinal cord in ALD is reflected in the retina of patients with ALD. Therefore, OCT could be valuable as an outcome measure for the myelopathy of ALD. Additional longitudinal studies are ongoing.

Published
2020
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36. Liver disease predominates in a mouse model for mild human Zellweger spectrum disorder.

Author

Berendse K, Boek M, Gijbels M, Van der Wel NN, Klouwer FC, van den Bergh-Weerman MA, Shinde AB, Ofman R, Poll-The BT, Houten SM, Baes M, Wanders RJA, and Waterham HR

Subjects
ATPases Associated with Diverse Cellular Activities genetics, Alleles, Animals, Disease Models, Animal, Female, Fibroblasts, Humans, Liver pathology, Liver Diseases pathology, Male, Membrane Proteins genetics, Mice, Mice, Inbred C57BL, Mice, Knockout, Mitochondria metabolism, Peroxisomes, Phenotype, ATPases Associated with Diverse Cellular Activities metabolism, Liver metabolism, Liver Diseases etiology, Liver Diseases metabolism, Zellweger Syndrome complications
Abstract

Zellweger spectrum disorders (ZSDs) are autosomal recessive diseases caused by defective peroxisome assembly. They constitute a clinical continuum from severe early lethal to relatively milder presentations in adulthood. Liver disease is a prevalent symptom in ZSD patients. The underlying pathogenesis for the liver disease, however, is not fully understood. We report a hypomorphic ZSD mouse model, which is homozygous for Pex1-c.2531G>A (p.G844D), the equivalent of the most common pathogenic variant found in ZSD, and which predominantly presents with liver disease. After introducing the Pex1-G844D allele by knock-in, we characterized homozygous Pex1-G844D mice for survival, biochemical parameters, including peroxisomal and mitochondrial functions, organ histology, and developmental parameters. The first 20 post-natal days (P20) were critical for survival of homozygous Pex1-G844D mice (~20% survival rate). Lethality was likely due to a combination of cholestatic liver problems, liver dysfunction and caloric deficit, probably as a consequence of defective bile acid biosynthesis. Survival beyond P20 was nearly 100%, but surviving mice showed a marked delay in growth. Surviving mice showed similar hepatic problems as described for mild ZSD patients, including hepatomegaly, bile duct proliferation, liver fibrosis and mitochondrial alterations. Biochemical analyses of various tissues showed the absence of functional peroxisomes accompanied with aberrant levels of peroxisomal metabolites predominantly in the liver, while other tissues were relatively spared. ur findings show that homozygous Pex1-G844D mice have a predominant liver disease phenotype, mimicking the hepatic pathology of ZSD patients, and thus constitute a good model to study pathogenesis and treatment of liver disease in ZSD patients., (Copyright © 2019 The Authors. Published by Elsevier B.V. All rights reserved.)

Published
2019
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37. Hepatic symptoms and histology in 13 patients with a Zellweger spectrum disorder.

Author

Berendse K, Koot BGP, Klouwer FCC, Engelen M, Roels F, Lacle MM, Nikkels PGJ, Verheij J, and Poll-The BT

Subjects
Adolescent, Adult, Carcinoma, Hepatocellular pathology, Child, Child, Preschool, Disease Progression, Female, Humans, Infant, Liver Cirrhosis pathology, Liver Neoplasms pathology, Male, Middle Aged, Netherlands, Peroxisomes genetics, Zellweger Syndrome genetics, Carcinoma, Hepatocellular etiology, Liver pathology, Liver Cirrhosis etiology, Liver Neoplasms etiology, Zellweger Syndrome complications
Abstract

Patients with a Zellweger spectrum disorder (ZSD) have a defect in the assembly or maintenance of peroxisomes, leading to a multisystem disease with variable outcome. Liver disease is an important feature in patients with severe and milder phenotypes and a frequent cause of death. However, the course and histology of liver disease in ZSD patients are ill-defined. We reviewed the hepatic symptoms and histological findings of 13 patients with a ZSD in which one or several liver biopsies have been performed (patient age 0.2-39 years). All patients had at least some histological liver abnormalities, ranging from minor fibrosis to cirrhosis. Five patients demonstrated significant disease progression with liver failure and early death. In others, liver-related symptoms were absent, although some still silently developed cirrhosis. Patients with peroxisomal mosaicism had a better prognosis. In addition, we show that patients are at risk to develop a hepatocellular carcinoma (HCC), as one patient developed a HCC at the age of 36 years and one patient a precancerous lesion at the age of 18 years. Thus, regular examination to detect fibrosis or cirrhosis should be included in the standard care of ZSD patients. In case of advanced fibrosis/cirrhosis expert consultation and HCC screening should be initiated. This study further delineates the spectrum and significance of liver involvement in ZSDs., (© 2019 SSIEM.)

Published
2019
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39. The cholic acid extension study in Zellweger spectrum disorders: Results and implications for therapy.

Author

Klouwer FCC, Koot BGP, Berendse K, Kemper EM, Ferdinandusse S, Koelfat KVK, Lenicek M, Vaz FM, Engelen M, Jansen PLM, Wanders RJA, Waterham HR, Schaap FG, and Poll-The BT

Subjects
Administration, Oral, Adolescent, Adult, Bile Acids and Salts metabolism, Biomarkers blood, Child, Child, Preschool, Cholic Acid blood, Female, Humans, Liver metabolism, Liver Diseases drug therapy, Liver Diseases metabolism, Male, Peroxisomes metabolism, Young Adult, Zellweger Syndrome blood, Zellweger Syndrome metabolism, Cholic Acid therapeutic use, Zellweger Syndrome drug therapy
Abstract

Introduction: Currently, no therapies are available for Zellweger spectrum disorders (ZSDs), a group of genetic metabolic disorders characterised by a deficiency of functional peroxisomes. In a previous study, we showed that oral cholic acid (CA) treatment can suppress bile acid synthesis in ZSD patients and, thereby, decrease plasma levels of toxic C 27 -bile acid intermediates, one of the biochemical abnormalities in these patients. However, no effect on clinically relevant outcome measures could be observed after 9 months of CA treatment. It was noted that, in patients with advanced liver disease, caution is needed because of possible hepatotoxicity., Methods: An extension study of the previously conducted pretest-posttest design study was conducted including 17 patients with a ZSD. All patients received oral CA for an additional period of 12 months, encompassing a total of 21 months of treatment. Multiple clinically relevant parameters and markers for bile acid synthesis were assessed after 15 and 21 months of treatment., Results: Bile acid synthesis was still suppressed after 21 months of CA treatment, accompanied with reduced levels of C 27 -bile acid intermediates in plasma. These levels significantly increased again after discontinuation of CA. No significant changes were found in liver tests, liver elasticity, coagulation parameters, fat-soluble vitamin levels or body weight., Conclusions: Although CA treatment did lead to reduced levels of toxic C 27 -bile acid intermediates in ZSD patients without severe liver fibrosis or cirrhosis, no improvement of clinically relevant parameters was observed after 21 months of treatment. We discuss the implications for CA therapy in ZSD based on these results., (© 2018 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.)

Published
2019
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40. Disease progression in women with X-linked adrenoleukodystrophy is slow.

Author

Huffnagel IC, Dijkgraaf MGW, Janssens GE, van Weeghel M, van Geel BM, Poll-The BT, Kemp S, and Engelen M

Subjects
Adrenoleukodystrophy blood, Adult, Biomarkers blood, Computational Biology, Cross-Sectional Studies, Disease Progression, Female, Humans, Logistic Models, Middle Aged, Spinal Cord Diseases pathology, Adrenoleukodystrophy pathology
Abstract

Background: Over 80% of women with X-linked adrenoleukodystrophy (ALD) develop spinal cord disease in adulthood for which treatment is supportive only. For future clinical trials quantitative data on disease progression rates are essential. Moreover, diagnosis can be challenging in ALD women, as the most important diagnostic biomarker is normal in 15-20%. Better biomarkers are needed. The purpose of this single centre cross-sectional follow-up study in women with ALD was to assess whether Expanded Disability Status Scale (EDSS), AMC Linear Disability Scale (ALDS) and Short Form (36) Health Survey (SF-36) can detect disease progression and to model the effect of age and duration of symptoms on the rate of progression. Moreover, we performed a pilot study to assess if a semi-targeted lipidomics approach can identify possible new diagnostic biomarkers., Results: In this study 46 women (baseline clinical data published by our group previously) were invited for a follow-up visit. Newly identified women at our center were also recruited. We analysed 65 baseline and 34 follow-up assessments. Median time between baseline and follow-up was 7.8 years (range 6.4-8.7). Mean age at baseline was 49.2 ± 14.2 years, at follow-up 55.4 ± 10.1. EDSS increased significantly (+ 0.08 points/year), but the other outcome measures did not. Increasing age and duration of symptoms were associated with more disability. For the pilot study we analysed plasma of 20 ALD women and 10 controls with ultra-high performance liquid chromatography coupled to high-resolution mass spectrometry, which identified 100 potential biomarker ratios with strong differentiating properties and non-overlapping data distributions between ALD women and controls., Conclusions: Progression of spinal cord disease can be detected with EDSS, but not with ALDS or SF-36 after a follow-up period of almost 8 years. Moreover, age and the duration of symptoms seem positively associated with the rate of progression. Although a significant progression was measurable, it was below the rate generally conceived as clinically relevant. Therefore, EDSS, ALDS and SF-36 are not suitable as primary outcome measures in clinical trials for spinal cord disease in ALD women. In addition, a semi-targeted lipidomics approach can identify possible new diagnostic biomarkers for women with ALD.

Published
2019
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41. Biallelic loss of function variants in COASY cause prenatal onset pontocerebellar hypoplasia, microcephaly, and arthrogryposis.

Author

van Dijk T, Ferdinandusse S, Ruiter JPN, Alders M, Mathijssen IB, Parboosingh JS, Innes AM, Meijers-Heijboer H, Poll-The BT, Bernier FP, Wanders RJA, Lamont RE, and Baas F

Subjects
Aborted Fetus abnormalities, Arthrogryposis pathology, Cells, Cultured, Cerebellar Diseases pathology, Humans, Infant, Newborn, Male, Microcephaly pathology, Syndrome, Transferases metabolism, Arthrogryposis genetics, Cerebellar Diseases genetics, Loss of Function Mutation, Microcephaly genetics, Transferases genetics
Abstract

Pontocerebellar hypoplasia (PCH) is a heterogeneous neurodegenerative disorder with a prenatal onset. Using whole-exome sequencing, we identified variants in the gene Coenzyme A (CoA) synthase (COASY) gene, an enzyme essential in CoA synthesis, in four individuals from two families with PCH, prenatal onset microcephaly, and arthrogryposis. In family 1, compound heterozygous variants were identified in COASY: c.[1549&#95;1550delAG]; [1486-3 C>G]. In family 2, all three affected siblings were homozygous for the c.1486-3 C>G variant. In both families, the variants segregated with the phenotype. RNA analysis showed that the c.1486-3 C>G variant leads to skipping of exon 7 with partial retention of intron 7, disturbing the reading frame and resulting in a premature stop codon (p.(Ala496Ilefs*20)). No CoA synthase protein was detected in patient cells by immunoblot analysis and CoA synthase activity was virtually absent. Partial CoA synthase defects were previously described as a cause of COASY Protein-Associated Neurodegeneration (CoPAN), a type of Neurodegeneration and Brain Iron Accumulation (NBIA). Here we demonstrate that near complete loss of function variants in COASY are associated with lethal PCH and arthrogryposis.

Published
2018
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42. A SEPSECS mutation in a 23-year-old woman with microcephaly and progressive cerebellar ataxia.

Author

van Dijk T, Vermeij JD, van Koningsbruggen S, Lakeman P, Baas F, and Poll-The BT

Subjects
Brain diagnostic imaging, Cerebellar Diseases genetics, Cognitive Dysfunction etiology, Female, Homozygote, Humans, Magnetic Resonance Imaging, Mutation, Missense, Exome Sequencing, Young Adult, Amino Acyl-tRNA Synthetases genetics, Brain pathology, Cerebellar Ataxia etiology, Cerebellar Diseases physiopathology, Microcephaly etiology
Abstract

Mutations in the SEPSECS gene are associated with pontocerebellar hypoplasia type 2D. Pontocerebellar hypoplasia (PCH) is a heterogeneous group of rare autosomal recessive neurodegenerative disorders, mainly affecting pons and cerebellum. Patients have severe motor and cognitive impairments and often die during infancy. Here, we report a 23-year-old woman with slowly progressive cerebellar ataxia and cognitive impairment, in whom a homozygous missense mutation in the SEPSECS gene (c.1321G>A; p.Gly441Arg) was identified with whole exome sequencing. Our findings underline that defects in selenoprotein synthesis can also result in milder cerebellar atrophy presenting at a later age.

Published
2018
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43. What's new in pontocerebellar hypoplasia? An update on genes and subtypes.

Author

van Dijk T, Baas F, Barth PG, and Poll-The BT

Subjects
Cerebellar Diseases genetics, Humans, Neurology, Phenotype, Cerebellar Diseases diagnosis
Abstract

Background: Pontocerebellar hypoplasia (PCH) describes a rare, heterogeneous group of neurodegenerative disorders mainly with a prenatal onset. Patients have severe hypoplasia or atrophy of cerebellum and pons, with variable involvement of supratentorial structures, motor and cognitive impairments. Based on distinct clinical features and genetic causes, current classification comprises 11 types of PCH., Main Text: In this review we describe the clinical, neuroradiological and genetic characteristics of the different PCH subtypes, summarize the differential diagnosis and reflect on potential disease mechanisms in PCH. Seventeen PCH-related genes are now listed in the OMIM database, most of them have a function in RNA processing or translation. It is unknown why defects in these apparently ubiquitous processes result in a brain-specific phenotype., Conclusions: Many new PCH related genes and phenotypes have been described due to the appliance of next generation sequencing techniques. By including such a broad range of phenotypes, including non-degenerative and postnatal onset disorders, the current classification gives rise to confusion. Despite the discovery of new pathways involved in PCH, treatment is still symptomatic. However, correct diagnosis of PCH is important to provide suitable care and counseling regarding prognosis, and offer appropriate (prenatal) genetic testing to families.

Published
2018
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44. Incidence and outcome of acquired demyelinating syndromes in Dutch children: update of a nationwide and prospective study.

Author

de Mol CL, Wong YYM, van Pelt ED, Ketelslegers IA, Bakker DP, Boon M, Braun KPJ, van Dijk KGJ, Eikelenboom MJ, Engelen M, Geleijns K, Haaxma CA, Niermeijer JMF, Niks EH, Peeters EAJ, Peeters-Scholte CMPCD, Poll-The BT, Portier RP, de Rijk-van Andel JF, Samijn JPA, Schippers HM, Snoeck IN, Stroink H, Vermeulen RJ, Verrips A, Visscher F, Vles JSH, Willemsen MAAP, Catsman-Berrevoets CE, Hintzen RQ, and Neuteboom RF

Subjects
Adolescent, Central Nervous System Diseases therapy, Child, Child, Preschool, Demyelinating Diseases therapy, Female, Follow-Up Studies, Humans, Incidence, Male, Netherlands epidemiology, Prospective Studies, Central Nervous System Diseases epidemiology, Demyelinating Diseases epidemiology
Abstract

Introduction: Acquired demyelinating syndromes (ADS) are immune-mediated demyelinating disorders of the central nervous system in children. A nationwide, multicentre and prospective cohort study was initiated in the Netherlands in 2006, with a reported ADS incidence of 0.66/100,000 per year and MS incidence of 0.15/100,000 per year in the period between 2007 and 2010. In this study, we provide an update on the incidence and the long-term follow-up of ADS in the Netherlands., Methods: Children < 18 years with a first attack of demyelination were included consecutively from January 2006 to December 2016. Diagnoses were based on the International Paediatric MS study group consensus criteria. Outcome data were collected by neurological and neuropsychological assessments, and telephone call assessments., Results: Between 2011 and 2016, 55/165 of the ADS patients were diagnosed with MS (33%). This resulted in an increased ADS and MS incidence of 0.80/100,000 per year and 0.26/100,000 per year, respectively. Since 2006 a total of 243 ADS patients have been included. During follow-up (median 55 months, IQR 28-84), 137 patients were diagnosed with monophasic disease (56%), 89 with MS (37%) and 17 with multiphasic disease other than MS (7%). At least one form of residual deficit including cognitive impairment was observed in 69% of all ADS patients, even in monophasic ADS. An Expanded Disability Status Scale score of ≥ 5.5 was reached in 3/89 MS patients (3%)., Conclusion: The reported incidence of ADS in Dutch children has increased since 2010. Residual deficits are common in this group, even in monophasic patients. Therefore, long-term follow-up in ADS patients is warranted.

Published
2018
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45. Brain atrophy following hemiplegic migraine attacks.

Author

Pelzer N, Hoogeveen ES, Ferrari MD, Poll-The BT, Kruit MC, and Terwindt GM

Subjects
Adolescent, Atrophy etiology, Atrophy pathology, Calcium Channels genetics, Child, Child, Preschool, Female, Humans, Migraine with Aura complications, Migraine with Aura genetics, Mutation, Young Adult, Brain pathology, Brain Diseases etiology, Brain Diseases pathology, Migraine with Aura pathology
Abstract

Background Patients with hemiplegic migraine (HM) may sometimes develop progressive neurological deterioration of which the pathophysiology is unknown. Patient We report a 16-year clinical and neuroradiological follow-up of a patient carrying a de novo p.Ser218Leu CACNA1A HM mutation who had nine severe HM attacks associated with seizures and decreased consciousness between the ages of 3 and 12 years. Results Repeated ictal and postictal neuroimaging revealed cytotoxic oedema during severe HM attacks in the symptomatic hemisphere, which later showed atrophic changes. In addition, progressive cerebellar atrophy was observed. Brain atrophy halted after cessation of severe attacks, possibly due to prophylactic treatment with flunarizine and sodium valproate. Conclusion Severe HM attacks may result in brain atrophy and prophylactic treatment of these attacks might be needed in an early stage of disease to prevent permanent brain damage.

Published
2018
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46. Clinical, Biomarker, and Molecular Delineations and Genotype-Phenotype Correlations of Ataxia With Oculomotor Apraxia Type 1.

Author

Renaud M, Moreira MC, Ben Monga B, Rodriguez D, Debs R, Charles P, Chaouch M, Ferrat F, Laurencin C, Vercueil L, Mallaret M, M'Zahem A, Pacha LA, Tazir M, Tilikete C, Ollagnon E, Ochsner F, Kuntzer T, Jung HH, Beis JM, Netter JC, Djamshidian A, Bower M, Bottani A, Walsh R, Murphy S, Reiley T, Bieth É, Roelens F, Poll-The BT, Lourenço CM, Jardim LB, Straussberg R, Landrieu P, Roze E, Thobois S, Pouget J, Guissart C, Goizet C, Dürr A, Tranchant C, Koenig M, and Anheim M

Subjects
Adolescent, Adult, Apraxias complications, Apraxias diagnostic imaging, Apraxias genetics, Ataxia complications, Ataxia diagnostic imaging, Cogan Syndrome complications, Cogan Syndrome diagnostic imaging, Disability Evaluation, Female, Humans, International Cooperation, Male, Middle Aged, Retrospective Studies, TRPC Cation Channels genetics, Young Adult, alpha-Fetoproteins metabolism, Apraxias congenital, Ataxia genetics, Cogan Syndrome genetics, DNA-Binding Proteins genetics, Genetic Association Studies, Mutation genetics, Nuclear Proteins genetics
Abstract

Importance: Ataxia with oculomotor apraxia type 1 (AOA1) is an autosomal recessive cerebellar ataxia due to mutations in the aprataxin gene (APTX) that is characterized by early-onset cerebellar ataxia, oculomotor apraxia, axonal motor neuropathy, and eventual decrease of albumin serum levels., Objectives: To improve the clinical, biomarker, and molecular delineation of AOA1 and provide genotype-phenotype correlations., Design, Setting, and Participants: This retrospective analysis included the clinical, biological (especially regarding biomarkers of the disease), electrophysiologic, imaging, and molecular data of all patients consecutively diagnosed with AOA1 in a single genetics laboratory from January 1, 2002, through December 31, 2014. Data were analyzed from January 1, 2015, through January 31, 2016., Main Outcomes and Measures: The clinical, biological, and molecular spectrum of AOA1 and genotype-phenotype correlations., Results: The diagnosis of AOA1 was confirmed in 80 patients (46 men [58%] and 34 women [42%]; mean [SD] age at onset, 7.7 [7.4] years) from 51 families, including 57 new (with 8 new mutations) and 23 previously described patients. Elevated levels of α-fetoprotein (AFP) were found in 33 patients (41%); hypoalbuminemia, in 50 (63%). Median AFP level was higher in patients with AOA1 (6.0 ng/mL; range, 1.1-17.0 ng/mL) than in patients without ataxia (3.4 ng/mL; range, 0.8-17.2 ng/mL; P < .01). Decreased albumin levels (ρ = -0.532) and elevated AFP levels (ρ = 0.637) were correlated with disease duration. The p.Trp279* mutation, initially reported as restricted to the Portuguese founder haplotype, was discovered in 53 patients with AOA1 (66%) with broad white racial origins. Oculomotor apraxia was found in 49 patients (61%); polyneuropathy, in 74 (93%); and cerebellar atrophy, in 78 (98%). Oculomotor apraxia correlated with the severity of ataxia and mutation type, being more frequent with deletion or truncating mutations (83%) than with presence of at least 1 missense variant (17%; P < .01). Mean (SD) age at onset was higher for patients with at least 1 missense mutation (17.7 [11.4] vs 5.2 [2.6] years; P < .001)., Conclusions and Relevance: The AFP level, slightly elevated in a substantial fraction of patients, may constitute a new biomarker for AOA1. Oculomotor apraxia may be an optional finding in AOA1 and correlates with more severe disease. The p.Trp279* mutation is the most frequent APTX mutation in the white population. APTX missense mutations may be associated with a milder phenotype.

Published
2018
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47. Development and validation of a severity scoring system for Zellweger spectrum disorders.

Author

Klouwer FCC, Meester-Delver A, Vaz FM, Waterham HR, Hennekam RCM, and Poll-The BT

Subjects
Adolescent, Adult, Child, Child, Preschool, Disease Management, Female, Genetic Association Studies, Humans, Male, Mutation, Phenotype, Reproducibility of Results, Retrospective Studies, Severity of Illness Index, Young Adult, Zellweger Syndrome genetics, Zellweger Syndrome diagnosis
Abstract

The lack of a validated severity scoring system for individuals with Zellweger spectrum disorders (ZSD) hampers optimal patient care and reliable research. Here, we describe the development of such severity score and its validation in a large, well-characterized cohort of ZSD individuals. We developed a severity scoring system based on the 14 organs that typically can be affected in ZSD. A standardized and validated method was used to classify additional care needs in individuals with neurodevelopmental disabilities (Capacity Profile [CAP]). Thirty ZSD patients of varying ages were scored by the severity score and the CAP. The median score was 9 (range 6-19) with a median scoring age of 16.0 years (range 2-36 years). The ZSD severity score was significantly correlated with all 5 domains of the CAP, most significantly with the sensory domain (r = 0.8971, P = <.0001). No correlation was found between age and severity score. Multiple peroxisomal biochemical parameters were significantly correlated with the severity score. The presently reported severity score for ZSD is a suitable tool to assess phenotypic severity in a ZSD patient at any age. This severity score can be used for objective phenotype descriptions, genotype-phenotype correlation studies, the identification of prognostic features in ZSD patients and for classification and stratification of patients in clinical trials., (© 2017 The Authors. Clinical Genetics published by John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2018
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48. Coagulopathy in Zellweger spectrum disorders: a role for vitamin K.

Author

Zeynelabidin S, Klouwer FCC, Meijers JCM, Suijker MH, Engelen M, Poll-The BT, and van Ommen CH

Subjects
Administration, Intravenous, Administration, Oral, Adolescent, Biomarkers blood, Blood Coagulation Disorders blood, Blood Coagulation Disorders diagnosis, Blood Coagulation Disorders epidemiology, Child, Female, Hemorrhage blood, Hemorrhage diagnosis, Hemorrhage epidemiology, Humans, Incidence, Male, Netherlands epidemiology, Pilot Projects, Proof of Concept Study, Prospective Studies, Protein Precursors blood, Prothrombin, Retrospective Studies, Severity of Illness Index, Treatment Outcome, Vitamin K Deficiency blood, Vitamin K Deficiency diagnosis, Vitamin K Deficiency epidemiology, Young Adult, Zellweger Syndrome blood, Zellweger Syndrome diagnosis, Zellweger Syndrome epidemiology, Blood Coagulation drug effects, Blood Coagulation Disorders drug therapy, Dietary Supplements, Hemorrhage drug therapy, Vitamin K administration & dosage, Vitamin K Deficiency drug therapy, Zellweger Syndrome drug therapy
Abstract

Introduction: Zellweger spectrum disorders (ZSDs) are caused by an impairment of peroxisome biogenesis, resulting in multiple metabolic abnormalities. This leads to a range of symptoms, including hepatic dysfunction and coagulopathy. This study evaluated the incidence and severity of coagulopathy and the effect of vitamin K supplementation orally and IV in ZSD., Methods: Data were retrospectively retrieved from the medical records of 30 ZSD patients to study coagulopathy and the effect of vitamin K orally on proteins induced by vitamin K absence (PIVKA-II) levels. Five patients from the cohort with a prolonged prothrombin time, low factor VII, and elevated PIVKA-II levels received 10 mg of vitamin K IV. Laboratory results, including thrombin generation, at baseline and 72 h after vitamin K administration were examined., Results: In the retrospective cohort, four patients (13.3%) experienced intracranial bleedings and 14 (46.7%) reported minor bleeding. No thrombotic events occurred. PIVKA-II levels decreased 38% after start of vitamin K therapy orally. In the five patients with a coagulopathy, despite treatment with oral administration of vitamin K, vitamin K IV caused an additional decrease (23%) of PIVKA-II levels and increased thrombin generation., Conclusion: Bleeding complications frequently occur in ZSD patients due to liver disease and vitamin K deficiency. Vitamin K deficiency is partly corrected by vitamin K supplementation orally, and vitamin K administered IV additionally improves vitamin K status, as shown by further decrease of PIVKA-II and improved thrombin generation.

Published
2018
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49. Relevance of neuroimaging for neurocognitive and behavioral outcome after pediatric traumatic brain injury.

Author

Königs M, Pouwels PJ, Ernest van Heurn LW, Bakx R, Jeroen Vermeulen R, Goslings JC, Carel Goslings J, Poll-The BT, van der Wees M, Catsman-Berrevoets CE, and Oosterlaan J

Subjects
Adolescent, Brain Injuries, Traumatic complications, Brain Injuries, Traumatic therapy, Child, Child Behavior Disorders diagnostic imaging, Child Behavior Disorders etiology, Cross-Sectional Studies, Diffusion Tensor Imaging, Female, Follow-Up Studies, Humans, Learning Disabilities diagnostic imaging, Learning Disabilities etiology, Magnetic Resonance Imaging, Male, Mental Disorders diagnostic imaging, Mental Disorders etiology, Neuroimaging, Prognosis, Tomography, X-Ray Computed, White Matter diagnostic imaging, White Matter injuries, Adolescent Behavior, Brain diagnostic imaging, Brain Injuries, Traumatic diagnostic imaging, Brain Injuries, Traumatic psychology, Child Behavior, Cognition
Abstract

This study aims to (1) investigate the neuropathology of mild to severe pediatric TBI and (2) elucidate the predictive value of conventional and innovative neuroimaging for functional outcome. Children aged 8-14 years with trauma control (TC) injury (n = 27) were compared to children with mild TBI and risk factors for complicated TBI (mild RF+ , n = 20) or moderate/severe TBI (n = 17) at 2.8 years post-injury. Neuroimaging measures included: acute computed tomography (CT), volumetric analysis on post-acute conventional T1-weighted magnetic resonance imaging (MRI) and post-acute diffusion tensor imaging (DTI, analyzed using tract-based spatial statistics and voxel-wise regression). Functional outcome was measured using Common Data Elements for neurocognitive and behavioral functioning. The results show that intracranial pathology on acute CT-scans was more prevalent after moderate/severe TBI (65%) than after mild RF+ TBI (35%; p = .035), while both groups had decreased white matter volume on conventional MRI (ps ≤ .029, ds ≥ -0.74). The moderate/severe TBI group further showed decreased fractional anisotropy (FA) in a widespread cluster affecting all white matter tracts, in which regional associations with neurocognitive functioning were observed (FSIQ, Digit Span and RAVLT Encoding) that consistently involved the corpus callosum. FA had superior predictive value for functional outcome (i.e. intelligence, attention and working memory, encoding in verbal memory and internalizing problems) relative to acute CT-scanning (i.e. internalizing problems) and conventional MRI (no predictive value). We conclude that children with mild RF+ TBI and moderate/severe TBI are at risk of persistent white matter abnormality. Furthermore, DTI has superior predictive value for neurocognitive out-come relative to conventional neuroimaging.

Published
2018
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