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Your search keyword '"Peter Heutink"' showing total 14 results
Start Over Author "Peter Heutink" Journal annals of neurology
14 results on '"Peter Heutink"'

1. C9orf72andUNC13Aare shared risk loci for amyotrophic lateral sclerosis and frontotemporal dementia: A genome-wide meta-analysis

Author

Max Koppers, Jochen H. Weishaupt, Philip Van Damme, Aleksey Shatunov, Albert C. Ludolph, John Landers, Karen E. Morrison, Jan H. Veldink, R. Jeroen Pasterkamp, Orla Hardiman, Judith Melki, Karol Estrada, David Czell, Robert H. Brown, John C. van Swieten, Fernando Rivadeneira, Vincent Meininger, P. Nigel Leigh, Leonard H. van den Berg, Wim Robberecht, Peter M. Andersen, Vivianna M. Van Deerlin, Albert Hofman, Christopher Shaw, André G. Uitterlinden, Vincenzo Silani, Michael A. van Es, Frank P. Diekstra, Adriano Chiò, Isabella Fogh, Peter Heutink, Markus Weber, Paul I.W. de Bakker, Pamela J. Shaw, Ammar Al-Chalabi, and Bryan J. Traynor

Subjects
Genetics, nutritional and metabolic diseases, Locus (genetics), Single-nucleotide polymorphism, Genome-wide association study, Biology, medicine.disease, nervous system diseases, Neurology, C9orf72, mental disorders, Genotype, medicine, Neurology (clinical), Amyotrophic lateral sclerosis, Frontotemporal dementia, Genetic association
Abstract

OBJECTIVE Substantial clinical, pathological, and genetic overlap exists between amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). TDP-43 inclusions have been found in both ALS and FTD cases (FTD-TDP). Recently, a repeat expansion in C9orf72 was identified as the causal variant in a proportion of ALS and FTD cases. We sought to identify additional evidence for a common genetic basis for the spectrum of ALS-FTD. METHODS We used published genome-wide association studies data for 4,377 ALS patients and 13,017 controls, and 435 pathology-proven FTD-TDP cases and 1,414 controls for genotype imputation. Data were analyzed in a joint meta-analysis, by replicating topmost associated hits of one disease in the other, and by using a conservative rank products analysis, allocating equal weight to ALS and FTD-TDP sample sizes. RESULTS Meta-analysis identified 19 genome-wide significant single nucleotide polymorphisms (SNPs) in C9orf72 on chromosome 9p21.2 (lowest p = 2.6 × 10(-12) ) and 1 SNP in UNC13A on chromosome 19p13.11 (p = 1.0 × 10(-11) ) as shared susceptibility loci for ALS and FTD-TDP. Conditioning on the 9p21.2 genotype increased statistical significance at UNC13A. A third signal, on chromosome 8q24.13 at the SPG8 locus coding for strumpellin (p = 3.91 × 10(-7) ) was replicated in an independent cohort of 4,056 ALS patients and 3,958 controls (p = 0.026; combined analysis p = 1.01 × 10(-7) ). INTERPRETATION We identified common genetic variants in C9orf72, but in addition in UNC13A that are shared between ALS and FTD. UNC13A provides a novel link between ALS and FTD-TDP, and identifies changes in neurotransmitter release and synaptic function as a converging mechanism in the pathogenesis of ALS and FTD-TDP.

Published
2014

2. Angiogenin variants in Parkinson disease and amyotrophic lateral sclerosis

Author

Max Koppers, Wenhao Yu, Stefan Waibel, Rebecca D. Folkerth, Hans Scheffer, Bart P.C. van de Warrenburg, R. Jeroen Pasterkamp, Markus Weber, Helenius J. Schelhaas, John Landers, Paul I.W. de Bakker, Wim Robberecht, Bastiaan R. Bloem, Peter Heutink, Marka van Blitterswijk, Robert H. Brown, Jacobus J. van Hilten, Daniela Berg, Dagmar Verbaan, Leonard H. van den Berg, Frank P. Diekstra, Katsumi Fumoto, Patrick Lowe, Claudia Schulte, Christine Klein, Anne-Marie Wills, Jan H. Veldink, Michael A. van Es, Anneke J. van der Kooi, Hylke M. Blauw, Vincenzo Silani, Philip Van Damme, Paul W.J. van Vught, Gianni Pezzoli, Stefano Goldwurm, Rubén Fernández-Santiago, Marianne de Visser, David M. Wu, Peter M. Andersen, Ashley Lyn Leclerc, Pamela Keagle, Caroline Dahlberg, Ewout J N Groen, Wouter van Rheenen, Bart F.L. van Nuenen, Thomas Gasser, Guo-fu Hu, Albert C. Ludolph, Robin Lemmens, Nicola Ticozzi, Claudio Mariani, Edwin Cuppen, Eric A. M. Hennekam, Roel A. Ophoff, Hiroko Kishikawa, Anna Birve, Amsterdam Neuroscience, Neurology, Amsterdam Cardiovascular Sciences, Neurosurgery, Human genetics, NCA - Neurodegeneration, and Hubrecht Institute for Developmental Biology and Stem Cell Research

Subjects
Male, medicine.medical_specialty, Pathology, Neurology, statistics & numerical data [Databases, Factual], Angiogenin, genetics [Ribonuclease, Pancreatic], Functional Neurogenomics Human Movement & Fatigue [DCN 2], Genome-wide association study, Genomic disorders and inherited multi-system disorders Functional Neurogenomics [IGMD 3], Disease, Gene mutation, genetics [Parkinson Disease], medicine, Humans, Multicenter Studies as Topic, Dementia, Genetic Predisposition to Disease, In patient, ddc:610, Amyotrophic lateral sclerosis, business.industry, Ribonuclease, Pancreatic, medicine.disease, genetics [Genetic Variation], United States, Europe, genetics [Amyotrophic Lateral Sclerosis], cardiovascular system, Female, Neurology (clinical), business, angiogenin
Abstract

Contains fulltext : 95644.pdf (Publisher’s version ) (Closed access) OBJECTIVE: Several studies have suggested an increased frequency of variants in the gene encoding angiogenin (ANG) in patients with amyotrophic lateral sclerosis (ALS). Interestingly, a few ALS patients carrying ANG variants also showed signs of Parkinson disease (PD). Furthermore, relatives of ALS patients have an increased risk to develop PD, and the prevalence of concomitant motor neuron disease in PD is higher than expected based on chance occurrence. We therefore investigated whether ANG variants could predispose to both ALS and PD. METHODS: We reviewed all previous studies on ANG in ALS and performed sequence experiments on additional samples, which allowed us to analyze data from 6,471 ALS patients and 7,668 controls from 15 centers (13 from Europe and 2 from the USA). We sequenced DNA samples from 3,146 PD patients from 6 centers (5 from Europe and 1 from the USA). Statistical analysis was performed using the variable threshold test, and the Mantel-Haenszel procedure was used to estimate odds ratios. RESULTS: Analysis of sequence data from 17,258 individuals demonstrated a significantly higher frequency of ANG variants in both ALS and PD patients compared to control subjects (p = 9.3 x 10(-6) for ALS and p = 4.3 x 10(-5) for PD). The odds ratio for any ANG variant in patients versus controls was 9.2 for ALS and 6.7 for PD. INTERPRETATION: The data from this multicenter study demonstrate that there is a strong association between PD, ALS, and ANG variants. ANG is a genetic link between ALS and PD. ANN NEUROL 2011;70:964-973. 01 december 2011 10 p.

Published
2011

3. Variable phenotypic expression and extensive tau pathology in two families with the noveltau mutation L315R

Author

Esther van Herpen, Dennis Dooijes, Rob Willemsen, Guido J. Breedveld, Michel Goedert, Peter Heutink, Wouter Kamphorst, Lies-Anne Serverijnen, Sonia M. Rosso, Raoul van de Graaf, R. Anthony Crowther, Danielle Majoor-Krakauer, Johan M. Kros, Hirotaka Yoshida, John C. van Swieten, and Rivka Ravid

Subjects
Adult, Male, Pathology, medicine.medical_specialty, DNA Mutational Analysis, Immunoblotting, Mutation, Missense, Penetrance, tau Proteins, Biology, medicine.disease_cause, Microtubules, Frontotemporal dementia and parkinsonism linked to chromosome 17, mental disorders, medicine, Humans, Protein Isoforms, Dementia, Missense mutation, Aged, Aged, 80 and over, Brain Chemistry, Mutation, Parkinsonism, Brain, Middle Aged, medicine.disease, Immunohistochemistry, Molecular biology, Pedigree, Chromosome 17 (human), Microscopy, Electron, Phenotype, Neurology, Female, Neurology (clinical), Frontotemporal dementia
Abstract

Mutations in the tau gene cause familial frontotemporal dementia and parkinsonism linked to chromosome 17. Here, we describe two Dutch families with familial frontotemporal dementia associated with the novel missense mutation L315R in exon 11 of tau. The age at onset of disease showed a large variation within each family, ranging from 25 to 64 years. Incomplete penetrance was established in an 82-year-old mutation carrier with no signs of dementia and appeared probable in two additional subjects. The brains of two affected subjects were studied and showed extensive tau pathology in neurons (Pick-like inclusions) and astroglial cells, particularly in the frontotemporal cortex and the hippocampal formation. Sarkosyl-insoluble tau extracted from the cerebral cortex showed the presence of straight and twisted tau filaments and a pattern of pathological tau bands similar to that of Pick's disease. Upon dephosphorylation, only five of the six brain tau isoforms were observed, with the shortest isoform being undetectable. All six tau isoforms were present in soluble brain tau. Recombinant tau proteins with the L315R mutation showed a reduced ability to promote microtubule assembly.

Published
2003

4. Chromosomal translocation t(18;21)(q23;q22.1) indicates novel susceptibility loci for frontotemporal dementia with ALS

Author

Stephan Niemann, Burkhard Alber, Klaus Zang, Klaus Roemer, Thomas F. Meyer, Peter Heutink, Joern Dullinger, Johannes Prudlo, Hans-Hilger Ropers, Vera M. Kalscheuer, Thomas Martin, Albert C. Ludolph, and Helmut Sittinger

Subjects
Chromosomes, Human, Pair 21, SOD1, Chromosomal translocation, Biology, Translocation, Genetic, Superoxide Dismutase-1, mental disorders, medicine, Humans, Gene silencing, Dementia, Amyotrophic lateral sclerosis, Gene, In Situ Hybridization, Fluorescence, Genetics, Reverse Transcriptase Polymerase Chain Reaction, Superoxide Dismutase, Amyotrophic Lateral Sclerosis, Brain, nutritional and metabolic diseases, Chromosome, medicine.disease, Magnetic Resonance Imaging, nervous system diseases, Blotting, Southern, Neurology, Karyotyping, Neurology (clinical), Chromosomes, Human, Pair 18, Tomography, Emission-Computed, Frontotemporal dementia
Abstract

A chromosomal translocation t(18;21)(q23;q22) is reported in a patient with frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS). We exclude the physical involvement and silencing of the ALS-linked gene for copper/zinc superoxide dismutase (SOD1) on chromosome 21q22.1. The breakpoints are assigned to sequences flanked by the markers ATA1H06, D18S462, D21S1915, and D21S1898. These critical regions may contain susceptibility loci for FTD associated with ALS.

Published
2003

5. An English kindred with a novel recessive tauopathy and respiratory failure

Author

John Q. Trojanowski, Carl E Clarke, Peter Heutink, Alex Crowe, Virginia M.-Y. Lee, Daniel Crooks, Michael Greenstone, Patrizia Rizzu, David Nicholl, and Clinical Genetics

Subjects
Adult, Male, Pathology, medicine.medical_specialty, Molecular Sequence Data, Genes, Recessive, tau Proteins, Neuropathology, Gene mutation, Microtubules, Humans, Medicine, Age of Onset, Sibling, Base Sequence, business.industry, Brain, medicine.disease, Immunohistochemistry, Pedigree, Hypoventilation, Tauopathies, Neurology, Respiratory failure, Mutation, Female, Neurology (clinical), Tauopathy, Age of onset, medicine.symptom, Respiratory Insufficiency, business, Consanguineous Marriage
Abstract

We present the clinicopathological features of two siblings from a consanguineous marriage who presented with respiratory hypoventilation and died 10 days and 4 years later, respectively. This disorder showed extensive tau neuropathology, and both had a novel homozygous S352L tau gene mutation. This is the first description of a pathologically proved young-onset tauopathy with apparent recessive inheritance.

Published
2003

6. A novel tau mutation, S320F, causes a tauopathy with inclusions similar to those in Pick's disease

Author

Dennis Dooijes, Wout H. Deelen, Lies-Anne Severijnen, Michel Goedert, Martinus F. Niermeijer, Peter Heutink, Rob Willemsen, John C. van Swieten, Esther van Herpen, Michael J. Smith, Rivka Ravid, Sonia M. Rosso, Wouter Kamphorst, Neurology, and Clinical Genetics

Subjects
Adult, Male, Proband, Pathology, medicine.medical_specialty, Elucidation of hereditary disorders and their molecular diagnosis, Tau protein, Mutation, Missense, tau Proteins, Microtubules, Frontotemporal dementia and parkinsonism linked to chromosome 17, Pick Disease of the Brain, Alzheimer Disease, mental disorders, medicine, Humans, Missense mutation, Ultrasonography, Inclusion Bodies, Genetics, biology, DNA, Exons, medicine.disease, Recombinant Proteins, Microscopy, Electron, Neurology, Mutation (genetic algorithm), biology.protein, Pick's disease, Neurology (clinical), Tauopathy, Alzheimer's disease, Opheldering van erfelijke ziekten en hun moleculaire diagnostiek
Abstract

Item does not contain fulltext Mutations in the tau gene cause familial frontotemporal dementia and parkinsonism linked to chromosome 17. In this article, we describe a novel missense mutation, S320F, in the tau gene in a family with presenile dementia. To our knowledge, it is the first mutation to be described in exon 11 of tau. The proband died at age 53 years, after a disease duration of 15 years, and autopsy revealed a neuropathological picture similar to Pick's disease. Recombinant tau protein with the S320F mutation showed a greatly reduced ability to promote microtubule assembly.

Published
2002

7. Phenotypic variation in hereditary frontotemporal dementia with tau mutations

Author

J. C. van Swieten, Marijke Joosse, Wouter Kamphorst, Maria Grazia Spillantini, Martinus F. Niermeijer, I. de Koning, Sonia M. Rosso, Peter Heutink, Rivka Ravid, Patrizia Rizzu, M. Stevens, Neurology, and Clinical Genetics

Subjects
Temporal cortex, Pathology, medicine.medical_specialty, biology, Parkinsonism, Tau protein, Hippocampus, medicine.disease, Frontotemporal dementia and parkinsonism linked to chromosome 17, Neurology, Frontal lobe, biology.protein, medicine, Neurology (clinical), Senile plaques, Psychology, Frontotemporal dementia
Abstract

Several mutations in the tau gene have been found in families with hereditary frontotemporal dementia and parkinsonism linked to chromosome 17q21-22 (FTDP-17). This study is the first attempt to correlate genotype and phenotype in six families with FTDP-17 with mutations in the tau gene (DK280, G272V, P301L, and R406W). We have investigated tau pathology in 1 P301L and 1 R406W patient. The R406W family showed a significantly higher age at onset (59.2 6 5.5 years) and longer duration of illness (12.7 6 1.5 years) than the families with the other mutations. The six families showed considerable variation in clinical presentation, but none of them had early parkinsonism. Mutism developed significantly later in the R406W family than in the other families. Frontotemporal atrophy on neuroimaging in the R406W family was less severe than in the P301L and DK280 families. The P301L brain contained many pretangles in the frontal and temporal cortex, and the dentate gyrus of hippocampus, showing three tau bands (64, 68, and 72 kd) of extracted tau from the frontal cortex. The presence of many neurofibrillary tangles, many diffuse and classic neuritic plaques in the temporal and parietal cortex, and the hippocampus of the same P301L brain correlated with the presence of four sarkosyl-insoluble (60, 64, 68, and 72 kd) tau bands. The coexistence of characteristic P301L and Alzheimer pathology in the same brain needs further explanation. The R406W brain showed abundant neurofibrillary tangles in several brain regions, and four tau bands (60, 64, 68, and 72 kd) of extracted tau from these regions. The slower progression of the disease in the R406W family might be explained by the microtubule-binding properties of the mutant protein.

Published
1999

8. Hereditary Frontotemporal Dementia Is Linked to Chromosome 17q21-q22: A Genetic and Clinicopathological Study of Three Dutch Families

Author

Aad Tibben, Ben A. Oostra, Johan M. Kros, J. C. van Swieten, Martinus F. Niermeijer, C M van Duijn, Peter Heutink, Egbert Bakker, M. Stevens, Patrizia Rizzu, Clinical Genetics, Neurology, Pathology, Psychiatry, and Epidemiology

Subjects
Temporal cortex, Pathology, medicine.medical_specialty, Genetic Linkage, Middle Aged, medicine.disease, Temporal Lobe, Frontotemporal dementia and parkinsonism linked to chromosome 17, Frontal Lobe, Pedigree, Central nervous system disease, Degenerative disease, Atrophy, Neurology, Genetic linkage, Chromosomal region, medicine, Humans, Dementia, Neurology (clinical), Psychology, Frontotemporal dementia, Chromosomes, Human, Pair 17, Netherlands
Abstract

Hereditary frontotemporal dementia (HFTD) is a rare autosomal dominant form of presenile dementia characterized by behavioral changes and reduced speech. Three multigeneration kindreds with this condition, in the Netherlands, were investigated for clinicopathological comparison and linkage analysis. Frontotemporal atrophy on computed tomographic scanning and/or magnetic resonance imaging was usually present. Single-photon emission computed tomography (SPECT) showed frontal hypoperfusion in the early phase of the disease. Brain tissue showed moderate to severe atrophy of frontal and temporal cortex with neuronal loss, gliosis, and spongiosis. Pick bodies were lacking in all cases of the 3 families. The mean age of onset varied significantly between families. We report here evidence for linkage to chromosome 17q21-q22 with a maximum lod score of 4.70 at theta = 0.05 with the marker D17S932. Recombination analysis positions the gene for HFTD in a region of approximately 5 cM between markers D17S946 and D17S791. Three other neurodegenerative disorders with a strong clinical and pathological resemblance have recently been mapped to the same chromosomal region, suggesting that a group of clinically related neurodegenerative disorders may originate from mutations in the same gene.

Published
1997

9. FTDP-17: an early-onset phenotype with parkinsonism and epileptic seizures caused by a novel mutation

Author

Michael B. Collatz, Marijke Joosse, Hartmut Baier, Sven N. Reske, Johannes Schwarz, Peter Heutink, Markus Palmbach, Anne D. Sperfeld, Alexander Storch, Klaus Tatsch, Albert C. Ludolph, and Clinical Genetics

Subjects
Adult, Male, Nonsense mutation, Tau protein, Mutation, Missense, tau Proteins, medicine.disease_cause, Epilepsy, medicine, Missense mutation, Dementia, Humans, Age of Onset, Child, Aged, Genetics, Tomography, Emission-Computed, Single-Photon, Mutation, biology, Parkinsonism, Infant, Newborn, Brain, Chromosome Mapping, Electroencephalography, Parkinson Disease, Middle Aged, medicine.disease, Magnetic Resonance Imaging, Temporal Lobe, Frontal Lobe, Pedigree, Phenotype, Neurology, Amino Acid Substitution, Child, Preschool, biology.protein, Disease Progression, Female, Neurology (clinical), Psychology, Neuroscience, Microtubule-Associated Proteins, Frontotemporal dementia, Chromosomes, Human, Pair 17
Abstract

Recently, mutations in the tau gene on chromosome 17 were found causative for autosomal dominantly inherited frontotemporal dementia and parkinsonism (FTDP-17). We describe a family carrying a missense mutation at nucleotide 1137 C --> T, resulting in the amino acid substitution P301S. Methods of investigations include clinical, electrophysiological, and imaging techniques. This kindred presents with a novel phenotype characterized by an early onset of rapidly progressive frontotemporal dementia and parkinsonism in combination with epileptic seizures. We define the dopaminergic deficits as being predominantly presynaptic by the use of single-photon emission computed tomography with a dopamine transporter ligand. The association of this early-onset phenotype with P301S mutation is not entirely consistent with current criteria for the diagnosis of frontotemporal dementias and may encourage the search for tau mutations in diseases similar but not identical to FTDP-17. Also, the change from proline to serine suggests that this mutation might contribute to tau hyperphosphorylation.

Published
1999

14. Early-onset Parkinson's disease caused by a compound heterozygous DJ-1 mutation.

Author

Stephen Hague, Ekaterina Rogaeva, Dena Hernandez, Cindy Gulick, Amanda Singleton, Melissa Hanson, Janel Johnson, Roberto Weiser, Marisol Gallardo, Bernard Ravina, Katrina Gwinn-Hardy, Anthony Crawley, Peter H. St. George-Hyslop, Anthony E. Lang, Peter Heutink, Vincenzo Bonifati, John Hardy, and Andrew Singleton

Published
2003

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