Search

Your search keyword '"Smets K"' showing total 32 results
Start Over Author "Smets K" Database OAIster
32 results on '"Smets K"'

2. The External Genitalia Score (EGS): A European Multicenter Validation Study

Author

van der Straaten, S. (Saskia), Springer, A. (Alexander), Zecic, A. (Alexandra), Hebenstreit, D. (Doris), Tonnhofer, U. (Ursula), Gawlik, A. (Aneta), Baumert, M. (Malgorzata), Szeliga, K. (Kamila), Debulpaep, S. (Sara), Desloovere, A. (An), Tack, L. (Lloyd), Smets, K. (Koen), Wasniewska, M. (Malgorzata), Corica, D. (Domenico), Calafiore, M. (Mariarosa), Ljubicic, M.L. (Marie Lindhardt), Busch, A.S. (Alexander Siegfried), Juul, A. (Anders), Nordenström, A. (Anna), Sigurdsson, J. (Jon), Flück, C. (Christa), Haamberg, T. (Tanja), Graf, S. (Stefanie), Hannema, S.E. (Sabine), Wolffenbuttel, K.P. (Katja), Hiort, O. (Olaf), Ahmed, S.F. (Sayed), Cools, M.B.C.M. (Martine), van der Straaten, S. (Saskia), Springer, A. (Alexander), Zecic, A. (Alexandra), Hebenstreit, D. (Doris), Tonnhofer, U. (Ursula), Gawlik, A. (Aneta), Baumert, M. (Malgorzata), Szeliga, K. (Kamila), Debulpaep, S. (Sara), Desloovere, A. (An), Tack, L. (Lloyd), Smets, K. (Koen), Wasniewska, M. (Malgorzata), Corica, D. (Domenico), Calafiore, M. (Mariarosa), Ljubicic, M.L. (Marie Lindhardt), Busch, A.S. (Alexander Siegfried), Juul, A. (Anders), Nordenström, A. (Anna), Sigurdsson, J. (Jon), Flück, C. (Christa), Haamberg, T. (Tanja), Graf, S. (Stefanie), Hannema, S.E. (Sabine), Wolffenbuttel, K.P. (Katja), Hiort, O. (Olaf), Ahmed, S.F. (Sayed), and Cools, M.B.C.M. (Martine)

Abstract

CONTEXT: Standardized description of external genitalia is needed in the assessment of children with atypical genitalia. OBJECTIVES: To validate the External Genitalia Score (EGS), to present reference values for preterm and term babies up to 24 months and correlate obtained scores with anogenital distances (AGDs). DESIGN, SETTING: A European multicenter (n = 8) validation study was conducted from July 2016 to July 2018. PATIENTS AND METHODS: EGS is based on the external masculinization score but uses a gradual scale from female to male (range, 0-12) and terminology appropriate for both sexes. The reliability of EGS and AGDs was determined by the interclass correlation coefficient (ICC). Cross-sectional data were obtained in 686 term babies (0-24 months) and 181 preterm babies, and 111 babies with atypical genitalia. RESULTS: The ICC of EGS in typical and atypical genitalia is excellent and good, respectively. Median EGS (10th to 90th centile) in males < 28 weeks gestation is 10 (8.6-11.5); in males 28-32 weeks 11.5 (9.2-12); in males 33-36 weeks 11.5 (10.5-12) and in full-term males 12 (10.5-12). In all female babies, EGS is 0 (0-0). The mean (SD) lower/upper AGD ratio (AGDl/u) is 0.45 (0.1), with significant difference between AGDl/u in males 0.49 (0.1) and females 0.39 (0.1) and intermediate values in differences of sex development (DSDs) 0.43 (0.1). The AGDl/u correlates with EGS in males with typical genitalia and in atypical genitalia. CONCLUSIONS: EGS is a reliable and valid tool to describe external genitalia in premature and term babies up to 24 months. EGS correlates with AGDl/u in males. It facilitates standardized assessment, clinical decision-making and multicenter research.

Published
2020
Full Text
View/download PDF

3. The External Genitalia Score (EGS): A European Multicenter Validation Study

Author

Van Der Straaten, S, Springer, A, Zecic, A, Hebenstreit, D, Tonnhofer, U, Gawlik, A, Baumert, M, Szeliga, K, Debulpaep, S, Desloovere, A, Tack, L, Smets, K, Wasniewska, M, Corica, D, Calafiore, M, Ljubicic, ML, Busch, AS, Juul, A, Nordenström, A, Sigurdsson, J, Flück, CE, Haamberg, T, Graf, S, Hannema, Sabine, Wolffenbuttel, Katja, Hiort, O, Ahmed, SF, Cools, M (Martine), Van Der Straaten, S, Springer, A, Zecic, A, Hebenstreit, D, Tonnhofer, U, Gawlik, A, Baumert, M, Szeliga, K, Debulpaep, S, Desloovere, A, Tack, L, Smets, K, Wasniewska, M, Corica, D, Calafiore, M, Ljubicic, ML, Busch, AS, Juul, A, Nordenström, A, Sigurdsson, J, Flück, CE, Haamberg, T, Graf, S, Hannema, Sabine, Wolffenbuttel, Katja, Hiort, O, Ahmed, SF, and Cools, M (Martine)

Published
2020

4. Dose rationale and pharmacokinetics of dexmedetomidine in mechanically ventilated new-borns: impact of design optimisation

Author

van Dijkman, S.C., de Cock, P., Smets, K., Decaluwe, W., Smits, A, Allegaert, K.M. (Karel), van der Walle, J., Paepe, P., Della Pasqua, O. (Oscar), van Dijkman, S.C., de Cock, P., Smets, K., Decaluwe, W., Smits, A, Allegaert, K.M. (Karel), van der Walle, J., Paepe, P., and Della Pasqua, O. (Oscar)

Abstract

Purpose There is a need for alternative analgosedatives such as dexmedetomidine in neonates. Given the ethical and practical difficulties, protocol design for clinical trials in neonates should be carefully considered before implementation. Our objective was to identify a protocol design suitable for subsequent evaluation of the dosing requirements for dexmedetomidine in mechanically ventilated neonates. Methods A published paediatric pharmacokinetic model was used to derive the dosing regimen for dexmedetomidine in a firstin-neonate study. Optimality criteria were applied to optimise the blood sampling schedule. The impact of sampling schedule optimisation on model parameter estimation was assessed by simulation and re-estimation procedures for different simulation scenarios. The optimised schedule was then implemented in a neonatal pilot study. Results Parameter estimates were more precise and similarly accurate in the optimised scenarios, as compared to empirical sampling (normalised root mean square error: 1673.1% vs. 13,229.4% and relative error: 46.4% vs. 9.1%). Most importantly, protocol deviations from the optimal design still allowed reasonable parameter estimation. Data analysis from the pilot group (n = 6) confirmed the adequacy of the optimised trial protocol. Dexmedetomidine pharmacokinetics in term neonates was scaled using allometry and maturation, but results showed a 20% higher clearance in this population compared to initial estimates obtained by extrapolation from a slightly older paediatric population. Clearance for a typical neonate, with a post-menstrual age (PMA) of 40 weeks and weight 3.4 kg, was 2.92 L/h. Extension of the study with 11 additional subjects showed a further increased clearance in pre-term subjects with lower PMA. Conclusions The use of optimal design in conjunction with simulation scenarios improved the accuracy and precision of the estimates of the parameters of interest, taking into account protocol deviations, whic

Published
2019
Full Text
View/download PDF

9. The ESRF dark-field x-ray microscope at ID06

Author

Kutsal, M., Bernard, P., Berruyer, G., Cook, P. K., Hino, R., Jakobsen, A. C., Ludwig, W., Ormstrup, Jeppe, Roth, T., Simons, Hugh, Smets, K., Sierra, J. X., Wade, J., Wattecamps, P., Yildirim, C., Poulsen, Henning Friis, Detlefs, C., Kutsal, M., Bernard, P., Berruyer, G., Cook, P. K., Hino, R., Jakobsen, A. C., Ludwig, W., Ormstrup, Jeppe, Roth, T., Simons, Hugh, Smets, K., Sierra, J. X., Wade, J., Wattecamps, P., Yildirim, C., Poulsen, Henning Friis, and Detlefs, C.

Abstract

We present an instrument for dark-field x-ray microscopy installed on beamline ID06 of the ESRF — the first of its kind. Dark-field x-ray microscopy uses full field illumination of the sample and provides three-dimensional (3D) mapping of micro-structure and lattice strain in crystalline matter. It is analogous to dark-field electron microscopy in that an objective lens magnifies diffracting features of the sample. The use of high-energy synchrotron x-rays, however, means that these features can be large and deeply embedded. 3D movies can be acquired with a time resolution of seconds to minutes. The field of view and spatial resolution can be adapted by simple reconfiguration of the x-ray objective lens, reaching spatial and angular resolution of 30-100 nm and 0.001°, respectively. The instrument furthermore allows pre-characterization of samples at larger length scales using 3DXRD or DCT, such that a region of interest (e.g. a single grain) can be selected for high-resolution studies without the need to dismount the sample. As examples of applications we show work on mapping the subgrains in plastically deformed iron and aluminum alloys, mapping domains and strain fields in ferroelectric crystals, and studies of biominerals. This ability to directly characterize complex, multi-scale phenomena in-situ is a key step towards formulating and validating multi-scale models that account for the entire heterogeneity of materials. As an outlook, we discuss future prospects for such multi-scale characterization by combining DFXM with 3DXRD/DCT, and coherent x-ray methods for coarser and finer length-scales, respectively.

Published
2019

10. A detailed clinical analysis of 13 patients with AUTS2 syndrome further delineates the phenotypic spectrum and underscores the behavioural phenotype

Author

Beunders, G., Kamp, J. van der, Vasudevan, P., Morton, J., Smets, K., Kleefstra, T., Munnik, S.A. de, Schuurs-Hoeijmakers, J.H.M., Ceulemans, B., Zollino, M., Hoffjan, S., Wieczorek, S., So, J., Mercer, L., Walker, T., Velsher, L., Parker, M.J., Magee, A.C., Elffers, B., Kooy, R.F., Yntema, H.G., Meijers-Heijboer, E.J., Sistermans, E.A., Beunders, G., Kamp, J. van der, Vasudevan, P., Morton, J., Smets, K., Kleefstra, T., Munnik, S.A. de, Schuurs-Hoeijmakers, J.H.M., Ceulemans, B., Zollino, M., Hoffjan, S., Wieczorek, S., So, J., Mercer, L., Walker, T., Velsher, L., Parker, M.J., Magee, A.C., Elffers, B., Kooy, R.F., Yntema, H.G., Meijers-Heijboer, E.J., and Sistermans, E.A.

Abstract

Item does not contain fulltext, BACKGROUND: AUTS2 syndrome is an 'intellectual disability (ID) syndrome' caused by genomic rearrangements, deletions, intragenic duplications or mutations disrupting AUTS2. So far, 50 patients with AUTS2 syndrome have been described, but clinical data are limited and almost all cases involved young children. METHODS: We present a detailed clinical description of 13 patients (including six adults) with AUTS2 syndrome who have a pathogenic mutation or deletion in AUTS2. All patients were systematically evaluated by the same clinical geneticist. RESULTS: All patients have borderline to severe ID/developmental delay, 83-100% have microcephaly and feeding difficulties. Congenital malformations are rare, but mild heart defects, contractures and genital malformations do occur. There are no major health issues in the adults; the oldest of whom is now 59 years of age. Behaviour is marked by it is a friendly outgoing social interaction. Specific features of autism (like obsessive behaviour) are seen frequently (83%), but classical autism was not diagnosed in any. A mild clinical phenotype is associated with a small in-frame 5' deletions, which are often inherited. Deletions and other mutations causing haploinsufficiency of the full-length AUTS2 transcript give a more severe phenotype and occur de novo. CONCLUSIONS: The 13 patients with AUTS2 syndrome with unique pathogenic deletions scattered around the AUTS2 locus confirm a phenotype-genotype correlation. Despite individual variations, AUTS2 syndrome emerges as a specific ID syndrome with microcephaly, feeding difficulties, dysmorphic features and a specific behavioural phenotype.

Published
2016

11. A detailed clinical analysis of 13 patients with AUTS2 syndrome further delineates the phenotypic spectrum and underscores the behavioural phenotype

Author

Beunders, G., Kamp, J. van der, Vasudevan, P., Morton, J., Smets, K., Kleefstra, T., Munnik, S.A. de, Schuurs-Hoeijmakers, J.H.M., Ceulemans, B., Zollino, M., Hoffjan, S., Wieczorek, S., So, J., Mercer, L., Walker, T., Velsher, L., Parker, M.J., Magee, A.C., Elffers, B., Kooy, R.F., Yntema, H.G., Meijers-Heijboer, E.J., Sistermans, E.A., Beunders, G., Kamp, J. van der, Vasudevan, P., Morton, J., Smets, K., Kleefstra, T., Munnik, S.A. de, Schuurs-Hoeijmakers, J.H.M., Ceulemans, B., Zollino, M., Hoffjan, S., Wieczorek, S., So, J., Mercer, L., Walker, T., Velsher, L., Parker, M.J., Magee, A.C., Elffers, B., Kooy, R.F., Yntema, H.G., Meijers-Heijboer, E.J., and Sistermans, E.A.

Abstract

Item does not contain fulltext, BACKGROUND: AUTS2 syndrome is an 'intellectual disability (ID) syndrome' caused by genomic rearrangements, deletions, intragenic duplications or mutations disrupting AUTS2. So far, 50 patients with AUTS2 syndrome have been described, but clinical data are limited and almost all cases involved young children. METHODS: We present a detailed clinical description of 13 patients (including six adults) with AUTS2 syndrome who have a pathogenic mutation or deletion in AUTS2. All patients were systematically evaluated by the same clinical geneticist. RESULTS: All patients have borderline to severe ID/developmental delay, 83-100% have microcephaly and feeding difficulties. Congenital malformations are rare, but mild heart defects, contractures and genital malformations do occur. There are no major health issues in the adults; the oldest of whom is now 59 years of age. Behaviour is marked by it is a friendly outgoing social interaction. Specific features of autism (like obsessive behaviour) are seen frequently (83%), but classical autism was not diagnosed in any. A mild clinical phenotype is associated with a small in-frame 5' deletions, which are often inherited. Deletions and other mutations causing haploinsufficiency of the full-length AUTS2 transcript give a more severe phenotype and occur de novo. CONCLUSIONS: The 13 patients with AUTS2 syndrome with unique pathogenic deletions scattered around the AUTS2 locus confirm a phenotype-genotype correlation. Despite individual variations, AUTS2 syndrome emerges as a specific ID syndrome with microcephaly, feeding difficulties, dysmorphic features and a specific behavioural phenotype.

Published
2016

12. First de novo KCND3 mutation causes severe Kv4.3 channel dysfunction leading to early onset cerebellar ataxia, intellectual disability, oral apraxia and epilepsy

Author

Smets, K., Duarri, A., Deconinck, T., Ceulemans, B., Warrenburg, B.P.C. van de, Zuchner, S., Gonzalez, M.A., Schule, R., Synofzik, M., Aa, N. van der, Jonghe, P. De, Verbeek, D.S., Baets, J., Smets, K., Duarri, A., Deconinck, T., Ceulemans, B., Warrenburg, B.P.C. van de, Zuchner, S., Gonzalez, M.A., Schule, R., Synofzik, M., Aa, N. van der, Jonghe, P. De, Verbeek, D.S., and Baets, J.

Abstract

Contains fulltext : 155287.pdf (publisher's version ) (Open Access), BACKGROUND: Identification of the first de novo mutation in potassium voltage-gated channel, shal-related subfamily, member 3 (KCND3) in a patient with complex early onset cerebellar ataxia in order to expand the genetic and phenotypic spectrum. METHODS: Whole exome sequencing in a cerebellar ataxia patient and subsequent immunocytochemistry, immunoblotting and patch clamp assays of the channel were performed. RESULTS: A de novo KCND3 mutation (c.877_885dupCGCGTCTTC; p.Arg293_Phe295dup) was found duplicating the RVF motif and thereby adding an extra positive charge to voltage-gated potassium 4.3 (Kv4.3) in the voltage-sensor domain causing a severe shift of the voltage-dependence gating to more depolarized voltages. The patient displayed a severe phenotype with early onset cerebellar ataxia complicated by intellectual disability, epilepsy, attention deficit hyperactivity disorder, strabismus, oral apraxia and joint hyperlaxity. CONCLUSIONS: We identified a de novo KCND3 mutation causing the most marked change in Kv4.3's channel properties reported so far, which correlated with a severe and unique spinocerebellar ataxia (SCA) type 19/22 disease phenotype.

Published
2015

13. First de novo KCND3 mutation causes severe Kv4.3 channel dysfunction leading to early onset cerebellar ataxia, intellectual disability, oral apraxia and epilepsy

Author

Smets, K., Duarri, A., Deconinck, T., Ceulemans, B., Warrenburg, B.P.C. van de, Zuchner, S., Gonzalez, M.A., Schule, R., Synofzik, M., Aa, N. van der, Jonghe, P. De, Verbeek, D.S., Baets, J., Smets, K., Duarri, A., Deconinck, T., Ceulemans, B., Warrenburg, B.P.C. van de, Zuchner, S., Gonzalez, M.A., Schule, R., Synofzik, M., Aa, N. van der, Jonghe, P. De, Verbeek, D.S., and Baets, J.

Abstract

Contains fulltext : 155287.pdf (publisher's version ) (Open Access), BACKGROUND: Identification of the first de novo mutation in potassium voltage-gated channel, shal-related subfamily, member 3 (KCND3) in a patient with complex early onset cerebellar ataxia in order to expand the genetic and phenotypic spectrum. METHODS: Whole exome sequencing in a cerebellar ataxia patient and subsequent immunocytochemistry, immunoblotting and patch clamp assays of the channel were performed. RESULTS: A de novo KCND3 mutation (c.877_885dupCGCGTCTTC; p.Arg293_Phe295dup) was found duplicating the RVF motif and thereby adding an extra positive charge to voltage-gated potassium 4.3 (Kv4.3) in the voltage-sensor domain causing a severe shift of the voltage-dependence gating to more depolarized voltages. The patient displayed a severe phenotype with early onset cerebellar ataxia complicated by intellectual disability, epilepsy, attention deficit hyperactivity disorder, strabismus, oral apraxia and joint hyperlaxity. CONCLUSIONS: We identified a de novo KCND3 mutation causing the most marked change in Kv4.3's channel properties reported so far, which correlated with a severe and unique spinocerebellar ataxia (SCA) type 19/22 disease phenotype.

Published
2015

15. Genome-wide association analysis of genetic generalized epilepsies implicates susceptibility loci at 1q43, 2p16.1, 2q22.3 and 17q21.32

Author

Steffens, M, Leu, C, Ruppert, A-K, Zara, F, Striano, P, Robbiano, A, Capovilla, G, Tinuper, P, Gambardella, A, Bianchi, A, La Neve, A, Crichiutti, G, de Kovel, CGF, Trenite, DK-N, de Haan, G-J, Lindhout, D, Gaus, V, Schmitz, B, Janz, D, Weber, YG, Becker, F, Lerche, H, Steinhoff, BJ, Kleefuss-Lie, AA, Kunz, WS, Surges, R, Elger, CE, Muhle, H, von Spiczak, S, Ostertag, P, Helbig, I, Stephani, U, Moller, RS, Hjalgrim, H, Dibbens, LM, Bellows, S, Oliver, K, Mullen, S, Scheffer, IE, Berkovic, SF, Everett, KV, Gardiner, MR, Marini, C, Guerrini, R, Lehesjoki, A-E, Siren, A, Guipponi, M, Malafosse, A, Thomas, P, Nabbout, R, Baulac, S, Leguern, E, Guerrero, R, Serratosa, JM, Reif, PS, Rosenow, F, Moerzinger, M, Feucht, M, Zimprich, F, Kapser, C, Schankin, CJ, Suls, A, Smets, K, De Jonghe, P, Jordanova, A, Caglayan, H, Yapici, Z, Yalcin, DA, Baykan, B, Bebek, N, Ozbek, U, Gieger, C, Wichmann, H-E, Balschun, T, Ellinghaus, D, Franke, A, Meesters, C, Becker, T, Wienker, TF, Hempelmann, A, Schulz, H, Rueschendorf, F, Leber, M, Pauck, SM, Trucks, H, Toliat, MR, Nuernberg, P, Avanzini, G, Koeleman, BPC, Sander, T, Steffens, M, Leu, C, Ruppert, A-K, Zara, F, Striano, P, Robbiano, A, Capovilla, G, Tinuper, P, Gambardella, A, Bianchi, A, La Neve, A, Crichiutti, G, de Kovel, CGF, Trenite, DK-N, de Haan, G-J, Lindhout, D, Gaus, V, Schmitz, B, Janz, D, Weber, YG, Becker, F, Lerche, H, Steinhoff, BJ, Kleefuss-Lie, AA, Kunz, WS, Surges, R, Elger, CE, Muhle, H, von Spiczak, S, Ostertag, P, Helbig, I, Stephani, U, Moller, RS, Hjalgrim, H, Dibbens, LM, Bellows, S, Oliver, K, Mullen, S, Scheffer, IE, Berkovic, SF, Everett, KV, Gardiner, MR, Marini, C, Guerrini, R, Lehesjoki, A-E, Siren, A, Guipponi, M, Malafosse, A, Thomas, P, Nabbout, R, Baulac, S, Leguern, E, Guerrero, R, Serratosa, JM, Reif, PS, Rosenow, F, Moerzinger, M, Feucht, M, Zimprich, F, Kapser, C, Schankin, CJ, Suls, A, Smets, K, De Jonghe, P, Jordanova, A, Caglayan, H, Yapici, Z, Yalcin, DA, Baykan, B, Bebek, N, Ozbek, U, Gieger, C, Wichmann, H-E, Balschun, T, Ellinghaus, D, Franke, A, Meesters, C, Becker, T, Wienker, TF, Hempelmann, A, Schulz, H, Rueschendorf, F, Leber, M, Pauck, SM, Trucks, H, Toliat, MR, Nuernberg, P, Avanzini, G, Koeleman, BPC, and Sander, T

Abstract

Genetic generalized epilepsies (GGEs) have a lifetime prevalence of 0.3% and account for 20-30% of all epilepsies. Despite their high heritability of 80%, the genetic factors predisposing to GGEs remain elusive. To identify susceptibility variants shared across common GGE syndromes, we carried out a two-stage genome-wide association study (GWAS) including 3020 patients with GGEs and 3954 controls of European ancestry. To dissect out syndrome-related variants, we also explored two distinct GGE subgroups comprising 1434 patients with genetic absence epilepsies (GAEs) and 1134 patients with juvenile myoclonic epilepsy (JME). Joint Stage-1 and 2 analyses revealed genome-wide significant associations for GGEs at 2p16.1 (rs13026414, P(meta) = 2.5 × 10(-9), OR[T] = 0.81) and 17q21.32 (rs72823592, P(meta) = 9.3 × 10(-9), OR[A] = 0.77). The search for syndrome-related susceptibility alleles identified significant associations for GAEs at 2q22.3 (rs10496964, P(meta) = 9.1 × 10(-9), OR[T] = 0.68) and at 1q43 for JME (rs12059546, P(meta) = 4.1 × 10(-8), OR[G] = 1.42). Suggestive evidence for an association with GGEs was found in the region 2q24.3 (rs11890028, P(meta) = 4.0 × 10(-6)) nearby the SCN1A gene, which is currently the gene with the largest number of known epilepsy-related mutations. The associated regions harbor high-ranking candidate genes: CHRM3 at 1q43, VRK2 at 2p16.1, ZEB2 at 2q22.3, SCN1A at 2q24.3 and PNPO at 17q21.32. Further replication efforts are necessary to elucidate whether these positional candidate genes contribute to the heritability of the common GGE syndromes.

Published
2012

20. Mutations in SACS cause atypical and late-onset forms of ARSACS

Author

UCL - Cliniques universitaires Saint-Luc, UCL - SSS/IONS - Institute of NeuroScience, UCL - SSS/DDUV - Institut de Duve, UCL - SSS/IONS/NEUR - Clinical Neuroscience, UCL - (SLuc) Service de neurologie, Baets, J., Van den Bergh, Peter, Deconinck, T., Smets, K., Goossens, D., Dahan, Karin, Schmedding, E., Santens, P., Rasic, V. Milic, Van Damme, Patricia, Robberecht, Wim, De Meirleir, L., Michielsens, B., Del-Favero, J., Jordanova, A., De Jonghe, P., UCL - Cliniques universitaires Saint-Luc, UCL - SSS/IONS - Institute of NeuroScience, UCL - SSS/DDUV - Institut de Duve, UCL - SSS/IONS/NEUR - Clinical Neuroscience, UCL - (SLuc) Service de neurologie, Baets, J., Van den Bergh, Peter, Deconinck, T., Smets, K., Goossens, D., Dahan, Karin, Schmedding, E., Santens, P., Rasic, V. Milic, Van Damme, Patricia, Robberecht, Wim, De Meirleir, L., Michielsens, B., Del-Favero, J., Jordanova, A., and De Jonghe, P.

Abstract

Background: Autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS) is a complex neurodegenerative disorder caused by mutations in SACS. The phenotype consists of a childhood-onset triad of cerebellar ataxia, peripheral neuropathy, and pyramidal tract signs. Objective: To provide more insight into the prevalence of SACS mutations and the variability of the associated phenotype. Methods: Mutation screening of SACS by direct sequencing and multiplex amplicon quantification for detection of intragenic copy number variations in a cohort of 85 index patients with phenotypes suggestive for ARSACS. Additional short tandem repeat (STR) marker analysis was performed for haplotype sharing. Results: In 11 families, 18 new SACS mutations were found (12.9% of total cohort). Five patients displayed onset ages in adulthood, a feature not known to be associated with ARSACS. The remaining index patients displayed a classic early onset phenotype. Initial phenotypic presentation was atypical in several patients, obscuring the clinical diagnosis. A founder mutation in SACS was identified in 3 Belgian families. In one isolated patient, an intragenic SACS deletion of exons 3-5 was detected. Partial SACS deletions were not previously described. Conclusions: In this study, we enlarge the ARSACS phenotype and the underlying genetic spectrum of SACS mutations. Patients with ARSACS are more common than previously known and risk underdiagnosis due to late onset age and unusual presentation. Neurology (R) 2010; 75: 1181-1188

Published
2010

21. REEP1 mutation spectrum and genotype/phenotype correlation in hereditary spastic paraplegia type 31.

Author

Beetz, C., Schule, R., Deconinck, T., Tran-Viet, K.N., Zhu, H., Kremer, H.P.H., Frints, S.G., Zelst-Stams, W.A.G. van, Byrne, P., Otto, S., Nygren, A.O., Baets, J., Smets, K., Ceulemans, B., Dan, B., Nagan, N., Kassubek, J., Klimpe, S., Klopstock, T., Stolze, H., Smeets, H.J.M., Schrander-Stumpel, C.T.R.M., Hutchinson, M., Warrenburg, B.P.C. van de, Braastad, C., Deufel, T., Pericak-Vance, M., Schols, L., Jonghe, P. de, Zuchner, S., Beetz, C., Schule, R., Deconinck, T., Tran-Viet, K.N., Zhu, H., Kremer, H.P.H., Frints, S.G., Zelst-Stams, W.A.G. van, Byrne, P., Otto, S., Nygren, A.O., Baets, J., Smets, K., Ceulemans, B., Dan, B., Nagan, N., Kassubek, J., Klimpe, S., Klopstock, T., Stolze, H., Smeets, H.J.M., Schrander-Stumpel, C.T.R.M., Hutchinson, M., Warrenburg, B.P.C. van de, Braastad, C., Deufel, T., Pericak-Vance, M., Schols, L., Jonghe, P. de, and Zuchner, S.

Abstract

Contains fulltext : 71291.pdf (publisher's version ) (Closed access), Mutations in the receptor expression enhancing protein 1 (REEP1) have recently been reported to cause autosomal dominant hereditary spastic paraplegia (HSP) type SPG31. In a large collaborative effort, we screened a sample of 535 unrelated HSP patients for REEP1 mutations and copy number variations. We identified 13 novel and 2 known REEP1 mutations in 16 familial and sporadic patients by direct sequencing analysis. Twelve out of 16 mutations were small insertions, deletions or splice site mutations. These changes would result in shifts of the open-reading-frame followed by premature termination of translation and haploinsufficiency. Interestingly, we identified two disease associated variations in the 3'-UTR of REEP1 that fell into highly conserved micro RNA binding sites. Copy number variation analysis in a subset of 133 HSP index patients revealed a large duplication of REEP1 that involved exons 2-7 in an Irish family. Clinically most SPG31 patients present with a pure spastic paraplegia; rare complicating features were restricted to symptoms or signs of peripheral nerve involvement. Interestingly, the distribution of age at onset suggested a bimodal pattern with the appearance of initial symptoms of disease either before the age of 20 years or after the age of 30 years. The overall mutation rate in our clinically heterogeneous sample was 3.0%; however, in the sub-sample of pure HSP REEP1 mutations accounted for 8.2% of all patients. These results firmly establish REEP1 as a relatively frequent autosomal dominant HSP gene for which genetic testing is warranted. We also establish haploinsufficiency as the main molecular genetic mechanism in SPG31, which should initiate and guide functional studies on REEP1 with a focus on loss-of-function mechanisms. Our results should be valid as a reference for mutation frequency, spectrum of REEP1 mutations, and clinical phenotypes associated with SPG31.

Published
2008

22. REEP1 mutation spectrum and genotype/phenotype correlation in hereditary spastic paraplegia type 31.

Author

Beetz, C., Schule, R., Deconinck, T., Tran-Viet, K.N., Zhu, H., Kremer, H.P.H., Frints, S.G., Zelst-Stams, W.A.G. van, Byrne, P., Otto, S., Nygren, A.O., Baets, J., Smets, K., Ceulemans, B., Dan, B., Nagan, N., Kassubek, J., Klimpe, S., Klopstock, T., Stolze, H., Smeets, H.J.M., Schrander-Stumpel, C.T.R.M., Hutchinson, M., Warrenburg, B.P.C. van de, Braastad, C., Deufel, T., Pericak-Vance, M., Schols, L., Jonghe, P. de, Zuchner, S., Beetz, C., Schule, R., Deconinck, T., Tran-Viet, K.N., Zhu, H., Kremer, H.P.H., Frints, S.G., Zelst-Stams, W.A.G. van, Byrne, P., Otto, S., Nygren, A.O., Baets, J., Smets, K., Ceulemans, B., Dan, B., Nagan, N., Kassubek, J., Klimpe, S., Klopstock, T., Stolze, H., Smeets, H.J.M., Schrander-Stumpel, C.T.R.M., Hutchinson, M., Warrenburg, B.P.C. van de, Braastad, C., Deufel, T., Pericak-Vance, M., Schols, L., Jonghe, P. de, and Zuchner, S.

Abstract

Contains fulltext : 71291.pdf (publisher's version ) (Closed access), Mutations in the receptor expression enhancing protein 1 (REEP1) have recently been reported to cause autosomal dominant hereditary spastic paraplegia (HSP) type SPG31. In a large collaborative effort, we screened a sample of 535 unrelated HSP patients for REEP1 mutations and copy number variations. We identified 13 novel and 2 known REEP1 mutations in 16 familial and sporadic patients by direct sequencing analysis. Twelve out of 16 mutations were small insertions, deletions or splice site mutations. These changes would result in shifts of the open-reading-frame followed by premature termination of translation and haploinsufficiency. Interestingly, we identified two disease associated variations in the 3'-UTR of REEP1 that fell into highly conserved micro RNA binding sites. Copy number variation analysis in a subset of 133 HSP index patients revealed a large duplication of REEP1 that involved exons 2-7 in an Irish family. Clinically most SPG31 patients present with a pure spastic paraplegia; rare complicating features were restricted to symptoms or signs of peripheral nerve involvement. Interestingly, the distribution of age at onset suggested a bimodal pattern with the appearance of initial symptoms of disease either before the age of 20 years or after the age of 30 years. The overall mutation rate in our clinically heterogeneous sample was 3.0%; however, in the sub-sample of pure HSP REEP1 mutations accounted for 8.2% of all patients. These results firmly establish REEP1 as a relatively frequent autosomal dominant HSP gene for which genetic testing is warranted. We also establish haploinsufficiency as the main molecular genetic mechanism in SPG31, which should initiate and guide functional studies on REEP1 with a focus on loss-of-function mechanisms. Our results should be valid as a reference for mutation frequency, spectrum of REEP1 mutations, and clinical phenotypes associated with SPG31.

Published
2008

23. REEP1 mutation spectrum and genotype/phenotype correlation in hereditary spastic paraplegia type 31.

Author

Beetz, C., Schule, R., Deconinck, T., Tran-Viet, K.N., Zhu, H., Kremer, H.P.H., Frints, S.G., Zelst-Stams, W.A.G. van, Byrne, P., Otto, S., Nygren, A.O., Baets, J., Smets, K., Ceulemans, B., Dan, B., Nagan, N., Kassubek, J., Klimpe, S., Klopstock, T., Stolze, H., Smeets, H.J.M., Schrander-Stumpel, C.T.R.M., Hutchinson, M., Warrenburg, B.P.C. van de, Braastad, C., Deufel, T., Pericak-Vance, M., Schols, L., Jonghe, P. de, Zuchner, S., Beetz, C., Schule, R., Deconinck, T., Tran-Viet, K.N., Zhu, H., Kremer, H.P.H., Frints, S.G., Zelst-Stams, W.A.G. van, Byrne, P., Otto, S., Nygren, A.O., Baets, J., Smets, K., Ceulemans, B., Dan, B., Nagan, N., Kassubek, J., Klimpe, S., Klopstock, T., Stolze, H., Smeets, H.J.M., Schrander-Stumpel, C.T.R.M., Hutchinson, M., Warrenburg, B.P.C. van de, Braastad, C., Deufel, T., Pericak-Vance, M., Schols, L., Jonghe, P. de, and Zuchner, S.

Abstract

Contains fulltext : 71291.pdf (publisher's version ) (Closed access), Mutations in the receptor expression enhancing protein 1 (REEP1) have recently been reported to cause autosomal dominant hereditary spastic paraplegia (HSP) type SPG31. In a large collaborative effort, we screened a sample of 535 unrelated HSP patients for REEP1 mutations and copy number variations. We identified 13 novel and 2 known REEP1 mutations in 16 familial and sporadic patients by direct sequencing analysis. Twelve out of 16 mutations were small insertions, deletions or splice site mutations. These changes would result in shifts of the open-reading-frame followed by premature termination of translation and haploinsufficiency. Interestingly, we identified two disease associated variations in the 3'-UTR of REEP1 that fell into highly conserved micro RNA binding sites. Copy number variation analysis in a subset of 133 HSP index patients revealed a large duplication of REEP1 that involved exons 2-7 in an Irish family. Clinically most SPG31 patients present with a pure spastic paraplegia; rare complicating features were restricted to symptoms or signs of peripheral nerve involvement. Interestingly, the distribution of age at onset suggested a bimodal pattern with the appearance of initial symptoms of disease either before the age of 20 years or after the age of 30 years. The overall mutation rate in our clinically heterogeneous sample was 3.0%; however, in the sub-sample of pure HSP REEP1 mutations accounted for 8.2% of all patients. These results firmly establish REEP1 as a relatively frequent autosomal dominant HSP gene for which genetic testing is warranted. We also establish haploinsufficiency as the main molecular genetic mechanism in SPG31, which should initiate and guide functional studies on REEP1 with a focus on loss-of-function mechanisms. Our results should be valid as a reference for mutation frequency, spectrum of REEP1 mutations, and clinical phenotypes associated with SPG31.

Published
2008

24. Integrale bosreservaten en xylobionten

Author

Smets, K., Vandekerkhove, K., Crèvecoeur, L., Smets, K., Vandekerkhove, K., and Crèvecoeur, L.

Abstract

In integrale bosreservaten waar processen van opbouw en afbraak uitermate belangrijk zijn, speelt dood hout een cruciale rol. De afbraak is een complex verhaal waarbij een hele resem organismen elkaar opvolgen. Net als gieren die pas na de leeuwen en hyena’s een kadaver in de savanne kunnen benaderen, spelen zich op dode bomen gelijkaardige taferelen af, zij het op iets kleinere schaal, en dit zowel met zwammen als met xylobionte kevers (keversoorten die hout nodig hebben voor een fase van hun ontwikkeling). De laatste jaren werden er door het Koninklijk Belgisch Instituut voor Natuurwetenschappen en door Luc Crèvecoeur, met ondersteuning van het INBO, enkele gerichte studies uitgevoerd om een beeld te krijgen van de aanwezige xylobiontenfauna in de Vlaamse integrale bosreservaten (Versteirt et al.,2000; De Bakker et al., 2002; Heirbaut et al., 2002; Crèvecoeur et al., 2004; Crèvecoeur & Vandekerkhove, 2005). Hiervoor werden zware staande boomlijken van Eik en Beuk bemonsterd met een uitgebreide vallenset. In sommige bossen werd ook actief gezocht naar xylobionte kevers, gebruik makende van een zeef om houtmolm te zeven, klopscherm en handvangsten.

Published
2006

25. Meningoencephalitis caused by Streptococcus pneumoniae: a diagnostic and therapeutic challenge. Diagnosis with diffusion-weighted MRI leading to treatment with corticosteroids.

Author

Jorens, P.G., Parizel, P.M., Demey, H.E., Smets, K., Jadoul, K., Verbeek, M.M., Wevers, R.A., Cras, P., Jorens, P.G., Parizel, P.M., Demey, H.E., Smets, K., Jadoul, K., Verbeek, M.M., Wevers, R.A., and Cras, P.

Abstract

Contains fulltext : 48791.pdf (publisher's version ) (Closed access), Streptococcus pneumoniae is a common cause of bacterial meningitis but only rarely causes other infections such as brain abscess, encephalitis, encephalomyelitis or meningoencephalitis. We report on three adult patients with meningoencephalitis caused by S. pneumoniae. In all three, CT and MRI revealed widespread brain lesions, suggesting extensive parenchymal injury. Diffusion-weighted MRI showed lesions with restricted diffusion, reflecting local areas of ischaemia with cytotoxic oedema secondary to an immunologically mediated necrotising vasculitis and thrombosis. High levels of markers of neuronal, glial and myelin damage were found in the cerebrospinal fluid. According to the literature, brain parenchyma lesions in adults with pneumococcal meningoencephalitis are often associated with death or severe neurological deficit. Our patients were treated with pulse doses of glucocorticoids: this resulted in dramatic clinical improvement and an excellent final neurological recovery.

Published
2005

26. Meningoencephalitis caused by Streptococcus pneumoniae: a diagnostic and therapeutic challenge. Diagnosis with diffusion-weighted MRI leading to treatment with corticosteroids.

Author

Jorens, P.G., Parizel, P.M., Demey, H.E., Smets, K., Jadoul, K., Verbeek, M.M., Wevers, R.A., Cras, P., Jorens, P.G., Parizel, P.M., Demey, H.E., Smets, K., Jadoul, K., Verbeek, M.M., Wevers, R.A., and Cras, P.

Abstract

Contains fulltext : 48791.pdf (publisher's version ) (Closed access), Streptococcus pneumoniae is a common cause of bacterial meningitis but only rarely causes other infections such as brain abscess, encephalitis, encephalomyelitis or meningoencephalitis. We report on three adult patients with meningoencephalitis caused by S. pneumoniae. In all three, CT and MRI revealed widespread brain lesions, suggesting extensive parenchymal injury. Diffusion-weighted MRI showed lesions with restricted diffusion, reflecting local areas of ischaemia with cytotoxic oedema secondary to an immunologically mediated necrotising vasculitis and thrombosis. High levels of markers of neuronal, glial and myelin damage were found in the cerebrospinal fluid. According to the literature, brain parenchyma lesions in adults with pneumococcal meningoencephalitis are often associated with death or severe neurological deficit. Our patients were treated with pulse doses of glucocorticoids: this resulted in dramatic clinical improvement and an excellent final neurological recovery.

Published
2005

27. Meningoencephalitis caused by Streptococcus pneumoniae: a diagnostic and therapeutic challenge. Diagnosis with diffusion-weighted MRI leading to treatment with corticosteroids.

Author

Jorens, P.G., Parizel, P.M., Demey, H.E., Smets, K., Jadoul, K., Verbeek, M.M., Wevers, R.A., Cras, P., Jorens, P.G., Parizel, P.M., Demey, H.E., Smets, K., Jadoul, K., Verbeek, M.M., Wevers, R.A., and Cras, P.

Abstract

Contains fulltext : 48791.pdf (publisher's version ) (Closed access), Streptococcus pneumoniae is a common cause of bacterial meningitis but only rarely causes other infections such as brain abscess, encephalitis, encephalomyelitis or meningoencephalitis. We report on three adult patients with meningoencephalitis caused by S. pneumoniae. In all three, CT and MRI revealed widespread brain lesions, suggesting extensive parenchymal injury. Diffusion-weighted MRI showed lesions with restricted diffusion, reflecting local areas of ischaemia with cytotoxic oedema secondary to an immunologically mediated necrotising vasculitis and thrombosis. High levels of markers of neuronal, glial and myelin damage were found in the cerebrospinal fluid. According to the literature, brain parenchyma lesions in adults with pneumococcal meningoencephalitis are often associated with death or severe neurological deficit. Our patients were treated with pulse doses of glucocorticoids: this resulted in dramatic clinical improvement and an excellent final neurological recovery.

Published
2005

28. The EPIBEL study: Outcomes to discharge from hospital for extremely preterm infants in Belgium

Author

UCL - MD/GYPE - Département de gynécologie, d'obstétrique et de pédiatrie, UCL - (SLuc) Service de néonatologie, Vanhaesebrouck, P, Allegaert, K, Bottu, J, Debauche, Christian, Devlieger, H, Docx, M, Francois, A, Haumont, D, Lombet, J, Rigo, J, Smets, K, Vanherreweghe, I, Van Overmeire, B, Van Reempts, P, Annual Ross Conference, UCL - MD/GYPE - Département de gynécologie, d'obstétrique et de pédiatrie, UCL - (SLuc) Service de néonatologie, Vanhaesebrouck, P, Allegaert, K, Bottu, J, Debauche, Christian, Devlieger, H, Docx, M, Francois, A, Haumont, D, Lombet, J, Rigo, J, Smets, K, Vanherreweghe, I, Van Overmeire, B, Van Reempts, P, and Annual Ross Conference

Abstract

Objective. To determine mortality and morbidity at discharge from the hospital of a large population-based cohort of infants who were born at less than or equal to26 weeks' gestation. Methods. Perinatal data were collected on extremely preterm infants who were alive at the onset of labor and born between January 1, 1999, and December 31, 2000, in all 19 Belgian perinatal centers. Results. A total of 525 infants were recorded. Life-supporting care was provided to 322 liveborn infants, 303 of whom were admitted for intensive care. The overall survival rate of liveborn infants was 54%. Of the infants who were alive at the age of 7 days, 82% survived to discharge. Vaginal delivery, shorter gestation, air leak, longer ventilator dependence, and higher initial oxygen need all were independently associated with death; gender, plurality, and surfactant therapy were not. Among the 175 survivors, 63% had 1 or more of the 3 major adverse outcome variables at the time of discharge (serious neuromorbidity, chronic lung disease at 36 weeks' postmenstrual age, or treated retinopathy of prematurity). The chance of survival free from serious neonatal morbidity at the time of hospital discharge was <15%(21 of 158) for the admitted infants with a gestation <26 weeks. Conclusions. If for the time being prolongation of pregnancy is unsuccessful, then outcome perspectives should be discussed and treatment options including nonintervention explicitly be made available to parents of infants of <26 weeks' gestation within the limits of medical feasibility and appropriateness.

Published
2004

29. Handleiding voor de Ouderbegeleider

Author

Bonnet, M., Schuengel, C., Baartman, H.E.M., Smets, K., Bonnet, M., Schuengel, C., Baartman, H.E.M., and Smets, K.

Published
2004

31. Handleiding voor de Ouderbegeleider

Author

Bonnet, M., Schuengel, C., Baartman, H.E.M., Smets, K., Bonnet, M., Schuengel, C., Baartman, H.E.M., and Smets, K.

Published
2004

Catalog

Books, media, physical & digital resources
See catalog results