Your search keyword '"Severijnen LA"' showing total 49 results

1. PRKAR1B mutation associated with a new neurodegenerative disorder with unique pathology

Author

Wong TH, Chiu WZ, Breedveld GJ, Li KW, Verkerk AJ, Hondius D, Hukema RK, Seelaar H, Frick P, Severijnen LA, Lammers GJ, Lebbink JH, van Duinen SG, Kamphorst W, Rozemuller AJ, Bakker EB, Neumann M, Willemsen R, Bonifati V, Smit AB, van Swieten J, Netherlands Brain Bank, International Parkinsonism Genetics Network, Ferreira J, Correia Guedes L, Chien HF, Barbosa ER, Merola A, Zibetti M, Lopiano L, Tassorelli C, Pacchetti C, Nappi G, Riboldazzi G, Bono G, Padovani A, Borroni B, Fincati E, Bertolasi L, Tinazzi M, Bonizzato A, Dalla Libera A, Guidi M, Marini P, Massaro F, Marconi R, Onofrj M, Thomas A, Vanacore N, Meco G, Fabbrini G, Fabrizio E, Manfredi M, Berardelli A, Stocchi F, Vacca L, De Mari M, Dell'Aquila C, Iliceto G, Lamberti P, Toni V, Trianni G, Saddi V, Cossu G, Melis M., CORTELLI, PIETRO, CAPELLARI, SABINA, Pathology, Human genetics, Neurology, NCA - neurodegeneration, Clinical Genetics, Internal Medicine, Molecular Genetics, Obstetrics & Gynecology, Molecular and Cellular Neurobiology, Neuroscience Campus Amsterdam - Neurodegeneration, AIMMS, Netherlands Institute for Neuroscience (NIN), Wong TH, Chiu WZ, Breedveld GJ, Li KW, Verkerk AJ, Hondius D, Hukema RK, Seelaar H, Frick P, Severijnen LA, Lammers GJ, Lebbink JH, van Duinen SG, Kamphorst W, Rozemuller AJ, Bakker EB, Neumann M, Willemsen R, Bonifati V, Smit AB, van Swieten J, Netherlands Brain Bank, International Parkinsonism Genetics Network, Ferreira J, Correia Guedes L, Chien HF, Barbosa ER, Merola A, Zibetti M, Lopiano L, Tassorelli C, Pacchetti C, Nappi G, Riboldazzi G, Bono G, Padovani A, Borroni B, Fincati E, Bertolasi L, Tinazzi M, Bonizzato A, Dalla Libera A, Cortelli P, Capellari S, Guidi M, Marini P, Massaro F, Marconi R, Onofrj M, Thomas A, Vanacore N, Meco G, Fabbrini G, Fabrizio E, Manfredi M, Berardelli A, Stocchi F, Vacca L, De Mari M, Dell'Aquila C, Iliceto G, Lamberti P, Toni V, Trianni G, Saddi V, Cossu G, and Melis M

Subjects

Models, Molecular, Male, Electron Microscope Tomography, Pathology, neurofilament, metabolism [Cyclic AMP-Dependent Protein Kinase Catalytic Subunits], pathology [Frontal Lobe], 0302 clinical medicine, chemistry [Cyclic AMP-Dependent Protein Kinase Catalytic Subunits], Models, Missense mutation, metabolism [alpha-Synuclein], Intermediate filament, 0303 health sciences, Parkinsonism, pathology [Neurodegenerative Diseases], Neurodegenerative Diseases, Single Nucleotide, SDG 10 - Reduced Inequalities, Middle Aged, Frontal Lobe, 3. Good health, DNA-Binding Proteins, genetics [Cyclic AMP-Dependent Protein Kinase RIbeta Subunit], metabolism [Frontal Lobe], PRKAR1B, neurodegenerative disorders, genetics [Polymorphism, Single Nucleotide], alpha-Synuclein, Female, metabolism [DNA-Binding Proteins], Frontotemporal dementia, medicine.medical_specialty, Neurofilament, Protein subunit, metabolism [Amyloid beta-Peptides], Nerve Tissue Proteins, tau Proteins, Biology, Polymorphism, Single Nucleotide, 03 medical and health sciences, medicine, Humans, ddc:610, Polymorphism, Protein kinase A, Hereditary Neurodegenerative Disorder, Genetic Association Studies, Aged, 030304 developmental biology, Family Health, intermediate filament, Cyclic AMP-Dependent Protein Kinase Catalytic Subunits, metabolism [Nerve Tissue Proteins], Amyloid beta-Peptides, protein kinase A Calpha, protein kinase A, Molecular, medicine.disease, Molecular biology, metabolism [tau Proteins], ultrastructure [Frontal Lobe], PRKAR1B protein, human, genetics [Neurodegenerative Diseases], Parkinson’s disease, Cyclic AMP-Dependent Protein Kinase RIbeta Subunit, Neurology (clinical), 030217 neurology & neurosurgery

Abstract

Inclusions of intermediate filaments are found in a number of neurodegenerative diseases. Using whole exome sequencing, linkage analysis and proteomics, Wong and Chiu et al. identify a new familial neurodegenerative disease with intermediate filament inclusions, linked to a mutation in the gene encoding the PKA type I-beta regulatory subunit, PRKAR1B.Pathological accumulation of intermediate filaments can be observed in neurodegenerative disorders, such as Alzheimer's disease, frontotemporal dementia and Parkinson's disease, and is also characteristic of neuronal intermediate filament inclusion disease. Intermediate filaments type IV include three neurofilament proteins (light, medium and heavy molecular weight neurofilament subunits) and alpha-internexin. The phosphorylation of intermediate filament proteins contributes to axonal growth, and is regulated by protein kinase A. Here we describe a family with a novel late-onset neurodegenerative disorder presenting with dementia and/or parkinsonism in 12 affected individuals. The disorder is characterized by a unique neuropathological phenotype displaying abundant neuronal inclusions by haematoxylin and eosin staining throughout the brain with immunoreactivity for intermediate filaments. Combining linkage analysis, exome sequencing and proteomics analysis, we identified a heterozygous c.149T > G (p.Leu50Arg) missense mutation in the gene encoding the protein kinase A type I-beta regulatory subunit (PRKAR1B). The pathogenicity of the mutation is supported by segregation in the family, absence in variant databases, and the specific accumulation of PRKAR1B in the inclusions in our cases associated with a specific biochemical pattern of PRKAR1B. Screening of PRKAR1B in 138 patients with Parkinson's disease and 56 patients with frontotemporal dementia did not identify additional novel pathogenic mutations. Our findings link a pathogenic PRKAR1B mutation to a novel hereditary neurodegenerative disorder and suggest an altered protein kinase A function through a reduced binding of the regulatory subunit to the A-kinase anchoring protein and the catalytic subunit of protein kinase A, which might result in subcellular dislocalization of the catalytic subunit and hyperphosphorylation of intermediate filaments.

Published

2014

2. Exome sequencing and functional analyses suggest that SIX6 is a gene involved in an altered proliferation-differentiation balance early in life and optic nerve degeneration at old age

Author

Iglesias, AI, Springelkamp, Henriët, Zondervan - van der Linde, Herma, Severijnen, LA, Amin, Najaf, Oostra, Ben, Kockx, Christel, van den Hout, MCGN, van Ijcken, Wilfred, Hofman, Bert, Uitterlinden, André, Verdijk, Rob, Klaver, Caroline, Willemsen, Rob, Duijn, Cornelia, Iglesias, AI, Springelkamp, Henriët, Zondervan - van der Linde, Herma, Severijnen, LA, Amin, Najaf, Oostra, Ben, Kockx, Christel, van den Hout, MCGN, van Ijcken, Wilfred, Hofman, Bert, Uitterlinden, André, Verdijk, Rob, Klaver, Caroline, Willemsen, Rob, and Duijn, Cornelia

Abstract

Primary open-angle glaucoma (POAG) is a hereditary neurodegenerative disease, characterized by optic nerve changes including increased excavation, notching and optic disc hemorrhages. The excavation can be described by the vertical cup-disc ratio (VCDR). Previously, genome-wide significant evidence for the association of rs10483727 in SIX1-SIX6 locus with VCDR and subsequent POAG was found. Using 1000 genomes-based imputation of four independent population-based cohorts in the Netherlands, we identified a missense variant rs33912345 (His141Asn) in SIX6 associated with VCDR (P-meta = 7.74 x 10(-7), n = 11 473) and POAG (Pmeta = 6.09 x 10(-3), n = 292). Exome sequencing analysis revealed another missense variant rs146737847 (Glu129Lys) also in SIX6 associated with VCDR (P = 5.09 x 10(-3), n = 1208). These two findings point to SIX6 as the responsible gene for the previously reported association signal. Functional characterization of SIX6 in zebrafish revealed that knockdown of six6b led to a small eye phenotype. Histological analysis showed retinal lamination, implying an apparent normal development of the eye, but an underdeveloped lens, and reduced optic nerve diameter. Expression analysis of morphants at 3 dpf showed a 5.5-fold up-regulation of cdkn2b, a cyclin-dependent kinase inhibitor, involved in cell cycle regulation and previously associated with VCDR and POAG in genome-wide association studies (GWASs). Since both six6b and cdkn2b play a key role in cell proliferation, we assessed the proliferative activity in the eye of morphants and found an alteration in the proliferative pattern of retinal cells. Our findings in humans and zebrafish suggest a functional involvement of six6b in early eye development, and open new insights into the genetic architecture of POAG.

Published

2014

3. A missense variant in the nuclear export signal of the FMR1 gene causes intellectual disability.

Author

Zeidler S, Severijnen LA, de Boer H, van der Toorn EC, Ruivenkamp CAL, Bijlsma EK, and Willemsen R

Subjects

5' Untranslated Regions genetics, Cell Line, Female, Fragile X Syndrome genetics, HEK293 Cells, Humans, Male, Phenotype, Exome Sequencing methods, Fragile X Mental Retardation Protein genetics, Intellectual Disability genetics, Mutation, Missense genetics, Nuclear Export Signals genetics

Abstract

Fragile X syndrome (FXS) is the most common monogenetic cause of intellectual disability and autism spectrum disorders. Mostly, FXS is caused by transcriptional silencing of the FMR1 gene due to a repeat expansion in the 5' UTR, and consequently lack of the protein product FMRP. However, in rare cases FXS is caused by other types of variants in the FMR1 gene. We describe a missense variant in the FMR1 gene, identified through whole-exome sequencing, in a boy with intellectual disability and behavioral problems. The variant is located in the FMRP's nuclear export signal (NES). We performed expression and localization studies of the variant in hair roots and HEK293 cells. Our results show normal expression but significant retention of the FMRP in the cells' nucleus. This finding suggests a possible FMRP reduction at its essential functional sites in the dendrites and the synaptic compartments and possible interference of other cellular processes in the nucleus. Together, this might lead to a FXS phenotype in the boy., (Copyright © 2020. Published by Elsevier B.V.)

Published

2021

4. Refining the Spectrum of Neuronal Intranuclear Inclusion Disease: A Case Report.

Author

Cupidi C, Dijkstra AA, Melhem S, Vernooij MW, Severijnen LA, Hukema RK, Rozemuller AJM, Neumann M, van Swieten JC, and Seelaar H

Subjects

Aged, Atrophy, Autopsy, Brain diagnostic imaging, Brain pathology, Cerebral Cortex pathology, Cognitive Dysfunction psychology, Diffusion Magnetic Resonance Imaging, Female, Humans, Intranuclear Inclusion Bodies pathology, Leukoaraiosis pathology, Magnetic Resonance Imaging, Muscle Weakness pathology, Myelin Sheath pathology, Nerve Fibers pathology, Neurodegenerative Diseases diagnostic imaging, Neurodegenerative Diseases psychology, Neuroglia pathology, Neurodegenerative Diseases pathology

Abstract

Neuronal intranuclear inclusion disease (NIID) is a rare heterogeneous progressive neurodegenerative disease characterized by the presence of eosinophilic hyaline intranuclear inclusions in neuronal and glial cells of the CNS, peripheral cells of the autonomic nervous system, visceral organs and skin. The clinical presentation is broadly heterogeneous and includes limb weakness, dementia, seizures, ataxia, and parkinsonism. High-intensity signal in the corticomedullary junction on brain MRI is a characteristic finding in NIID. We describe a 65-year-old patient presenting with mild cognitive impairment, evolving in dementia with behavioral disturbances and parkinsonism. Brain MRI showed mild global cortical atrophy, more pronounced in the cingulate and temporal cortex and mild leukoaraiosis, but no high-intensity signal in corticomedullary junction on diffusion weighted imaging. Neuropathological examination showed p62- and optineurin-positive neuronal intranuclear inclusions in the hippocampus and in some subcortical structures. Glial cells did not present any intranuclear inclusions, and no spongiotic changes proximal to the U-fibers or diffuse myelin pallor were disclosed in the white matter. We report on a case with pathological features of NIID showing different neuroimaging and pathological findings. We noted an absence of typical MRI abnormalities, lack of intranuclear inclusions in glial cells, and prominent involvement of hippocampal neurons, refining the clinico-pathological spectrum of the disease., (© 2019 American Association of Neuropathologists, Inc. All rights reserved.)

Published

2019

5. CXorf56, a dendritic neuronal protein, identified as a new candidate gene for X-linked intellectual disability.

Author

Verkerk AJMH, Zeidler S, Breedveld G, Overbeek L, Huigh D, Koster L, van der Linde H, de Esch C, Severijnen LA, de Vries BBA, Swagemakers SMA, Willemsen R, Hoogeboom AJM, van der Spek PJ, and Oostra BA

Subjects

Adolescent, Adult, Animals, Cells, Cultured, Codon, Terminator genetics, DNA Methylation, Female, Genetic Diseases, X-Linked pathology, Humans, Intellectual Disability pathology, Male, Mice, Mice, Inbred C57BL, Middle Aged, Neurons metabolism, Nonsense Mediated mRNA Decay, Nuclear Proteins, Genetic Diseases, X-Linked genetics, Intellectual Disability genetics, Nerve Tissue Proteins genetics

Abstract

Intellectual disability (ID) comprises a large group of heterogeneous disorders, often without a known molecular cause. X-linked ID accounts for 5-10% of male ID cases. We investigated a large, three-generation family with mild ID and behavior problems in five males and one female, with a segregation suggestive for X-linked inheritance. Linkage analysis mapped a disease locus to a 7.6 Mb candidate region on the X-chromosome (LOD score 3.3). Whole-genome sequencing identified a 2 bp insertion in exon 2 of the chromosome X open reading frame 56 gene (CXorf56), resulting in a premature stop codon. This insertion was present in all intellectually impaired individuals and carrier females. Additionally, X-inactivation status showed skewed methylation patterns favoring the inactivation of the mutated allele in the unaffected carrier females. We demonstrate that the insertion leads to nonsense-mediated decay and that CXorf56 mRNA expression is reduced in the impaired males and female. In murine brain slices and primary hippocampal neuronal cultures, CXorf56 protein was present and localized in the nucleus, cell soma, dendrites, and dendritic spines. Although no other families have been identified with pathogenic variants in CXorf56, these results suggest that CXorf56 is the causative gene in this family, and thus a novel candidate gene for X-linked ID with behavior problems.

Published

2018

6. Reversibility of neuropathology and motor deficits in an inducible mouse model for FXTAS.

Author

Hukema RK, Buijsen RA, Schonewille M, Raske C, Severijnen LA, Nieuwenhuizen-Bakker I, Verhagen RF, van Dessel L, Maas A, Charlet-Berguerand N, De Zeeuw CI, Hagerman PJ, Berman RF, and Willemsen R

Subjects

Animals, Brain metabolism, Brain pathology, Disease Models, Animal, Eye Movements genetics, Gene Expression, Genes, Reporter, Humans, Intranuclear Inclusion Bodies pathology, Mice, Mice, Transgenic, Peptides metabolism, Protein Binding, Protein Transport, Trinucleotide Repeat Expansion, Ubiquitin metabolism, Ataxia genetics, Ataxia physiopathology, Fragile X Syndrome genetics, Fragile X Syndrome physiopathology, Tremor genetics, Tremor physiopathology

Abstract

Fragile X-associated tremor/ataxia syndrome (FXTAS) is a late-onset neurodegenerative disorder affecting carriers of the fragile X-premutation, who have an expanded CGG repeat in the 5'-UTR of the FMR1 gene. FXTAS is characterized by progressive development of intention tremor, ataxia, parkinsonism and neuropsychological problems. The disease is thought to be caused by a toxic RNA gain-of-function mechanism, and the major hallmark of the disease is ubiquitin-positive intranuclear inclusions in neurons and astrocytes. We have developed a new transgenic mouse model in which we can induce expression of an expanded repeat in the brain upon doxycycline (dox) exposure (i.e. Tet-On mice). This Tet-On model makes use of the PrP-rtTA driver and allows us to study disease progression and possibilities of reversibility. In these mice, 8 weeks of dox exposure was sufficient to induce the formation of ubiquitin-positive intranuclear inclusions, which also stain positive for the RAN translation product FMRpolyG. Formation of these inclusions is reversible after stopping expression of the expanded CGG RNA at an early developmental stage. Furthermore, we observed a deficit in the compensatory eye movements of mice with inclusions, a functional phenotype that could be reduced by stopping expression of the expanded CGG RNA early in the disease development. Taken together, this study shows, for the first time, the potential of disease reversibility and suggests that early intervention might be beneficial for FXTAS patients., (© The Author 2015. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2015

7. A new inducible transgenic mouse model for C9orf72-associated GGGGCC repeat expansion supports a gain-of-function mechanism in C9orf72-associated ALS and FTD.

Author

Hukema RK, Riemslagh FW, Melhem S, van der Linde HC, Severijnen LA, Edbauer D, Maas A, Charlet-Berguerand N, Willemsen R, and van Swieten JC

Subjects

Amyotrophic Lateral Sclerosis genetics, Animals, Brain metabolism, C9orf72 Protein, Frontotemporal Dementia genetics, Humans, Inclusion Bodies metabolism, Proteins metabolism, Ubiquitin metabolism, Amyotrophic Lateral Sclerosis metabolism, DNA Repeat Expansion, Disease Models, Animal, Frontotemporal Dementia metabolism, Mice, Transgenic, Proteins genetics

Published

2014

8. FMRpolyG-positive inclusions in CNS and non-CNS organs of a fragile X premutation carrier with fragile X-associated tremor/ataxia syndrome.

Author

Buijsen RA, Sellier C, Severijnen LA, Oulad-Abdelghani M, Verhagen RF, Berman RF, Charlet-Berguerand N, Willemsen R, and Hukema RK

Subjects

Adrenal Glands metabolism, Adrenal Glands pathology, Ataxia genetics, Brain metabolism, Brain pathology, Female, Fragile X Mental Retardation Protein chemistry, Fragile X Mental Retardation Protein genetics, Fragile X Syndrome genetics, Heterozygote, Humans, Intranuclear Inclusion Bodies, Kidney metabolism, Kidney pathology, Male, Myocardium metabolism, Myocardium pathology, Thyroid Gland metabolism, Thyroid Gland pathology, Tremor genetics, Ubiquitin metabolism, Ataxia metabolism, Ataxia pathology, Fragile X Mental Retardation Protein analysis, Fragile X Syndrome metabolism, Fragile X Syndrome pathology, Tremor metabolism, Tremor pathology

Published

2014

9. Exome sequencing and functional analyses suggest that SIX6 is a gene involved in an altered proliferation-differentiation balance early in life and optic nerve degeneration at old age.

Author

Iglesias AI, Springelkamp H, van der Linde H, Severijnen LA, Amin N, Oostra B, Kockx CE, van den Hout MC, van Ijcken WF, Hofman A, Uitterlinden AG, Verdijk RM, Klaver CC, Willemsen R, and van Duijn CM

Subjects

Adolescent, Adult, Age Factors, Aged, Aged, 80 and over, Animals, Cell Proliferation, Chromosome Mapping, Exome, Eye embryology, Eye metabolism, Gene Expression Profiling, Genome-Wide Association Study, Glaucoma, Open-Angle genetics, Glaucoma, Open-Angle metabolism, Glaucoma, Open-Angle pathology, High-Throughput Nucleotide Sequencing, Homeodomain Proteins metabolism, Humans, Middle Aged, Models, Biological, Organogenesis genetics, Phenotype, Quantitative Trait Loci, Trans-Activators metabolism, Young Adult, Zebrafish, Cell Differentiation genetics, Homeodomain Proteins genetics, Nerve Degeneration genetics, Optic Nerve metabolism, Optic Nerve pathology, Trans-Activators genetics

Abstract

Primary open-angle glaucoma (POAG) is a hereditary neurodegenerative disease, characterized by optic nerve changes including increased excavation, notching and optic disc hemorrhages. The excavation can be described by the vertical cup-disc ratio (VCDR). Previously, genome-wide significant evidence for the association of rs10483727 in SIX1-SIX6 locus with VCDR and subsequent POAG was found. Using 1000 genomes-based imputation of four independent population-based cohorts in the Netherlands, we identified a missense variant rs33912345 (His141Asn) in SIX6 associated with VCDR (Pmeta = 7.74 × 10(-7), n = 11 473) and POAG (Pmeta = 6.09 × 10(-3), n = 292). Exome sequencing analysis revealed another missense variant rs146737847 (Glu129Lys) also in SIX6 associated with VCDR (P = 5.09 × 10(-3), n = 1208). These two findings point to SIX6 as the responsible gene for the previously reported association signal. Functional characterization of SIX6 in zebrafish revealed that knockdown of six6b led to a small eye phenotype. Histological analysis showed retinal lamination, implying an apparent normal development of the eye, but an underdeveloped lens, and reduced optic nerve diameter. Expression analysis of morphants at 3 dpf showed a 5.5-fold up-regulation of cdkn2b, a cyclin-dependent kinase inhibitor, involved in cell cycle regulation and previously associated with VCDR and POAG in genome-wide association studies (GWASs). Since both six6b and cdkn2b play a key role in cell proliferation, we assessed the proliferative activity in the eye of morphants and found an alteration in the proliferative pattern of retinal cells. Our findings in humans and zebrafish suggest a functional involvement of six6b in early eye development, and open new insights into the genetic architecture of POAG.

Published

2014

10. Induced expression of expanded CGG RNA causes mitochondrial dysfunction in vivo.

Author

Hukema RK, Buijsen RA, Raske C, Severijnen LA, Nieuwenhuizen-Bakker I, Minneboo M, Maas A, de Crom R, Kros JM, Hagerman PJ, Berman RF, and Willemsen R

Subjects

Animals, Anti-Bacterial Agents metabolism, Apoptosis drug effects, Ataxia genetics, Disease Models, Animal, Doxycycline metabolism, Fatty Liver pathology, Fragile X Syndrome genetics, Liver metabolism, Liver ultrastructure, Mice, Mice, Transgenic, Mitochondria drug effects, Promoter Regions, Genetic, RNA genetics, Reactive Oxygen Species, Tremor genetics, Ataxia metabolism, Fragile X Syndrome metabolism, Mitochondria metabolism, RNA metabolism, Repetitive Sequences, Nucleic Acid genetics, Tremor metabolism

Abstract

Fragile X-associated tremor/ataxia syndrome (FXTAS) is a late-onset neurodegenerative disorder affecting carriers of premutation forms of the FMR1 gene, resulting in a progressive development of tremor, ataxia and neuropsychological problems. The disease is caused by an expanded CGG repeat in the FMR1 gene, leading to an RNA gain-of-function toxicity mechanism. In order to study the pathogenesis of FXTAS, new inducible transgenic mouse models have been developed that expresses either 11CGGs or 90CGGs at the RNA level under control of a Tet-On promoter. When bred to an hnRNP-rtTA driver line, doxycycline (dox) induced expression of the transgene could be found in almost all tissues. Dox exposure resulted in loss of weight and death within 5 d for the 90CGG RNA expressing mice. Immunohistochemical examination of tissues of these mice revealed steatosis and apoptosis in the liver. Decreased expression of GPX1 and increased expression of cytochrome C is found. These effects were not seen in mice expressing a normal sized 11CGG repeat. In conclusion, we were able to show in vivo that expression of an expanded CGG-repeat rather than overexpression of a normal CGG-repeat causes pathology. In addition, we have shown that expanded CGG RNA expression can cause mitochondrial dysfunction by regulating expression levels of several markers. Although FTXAS patients do not display liver abnormalities, our findings contribute to understanding of the molecular mechanisms underlying toxicity of CGG repeat RNA expression in an animal model. In addition, the dox inducible mouse lines offer new opportunities to study therapeutic interventions for FXTAS.

Published

2014

11. FBXO7 immunoreactivity in α-synuclein-containing inclusions in Parkinson disease and multiple system atrophy.

Author

Zhao T, Severijnen LA, van der Weiden M, Zheng PP, Oostra BA, Hukema RK, Willemsen R, Kros JM, and Bonifati V

Subjects

Aged, Aged, 80 and over, Brain immunology, Brain metabolism, Brain pathology, F-Box Proteins immunology, Female, HEK293 Cells, Humans, Inclusion Bodies immunology, Inclusion Bodies pathology, Male, Middle Aged, Multiple System Atrophy immunology, Multiple System Atrophy pathology, Parkinson Disease immunology, Parkinson Disease pathology, alpha-Synuclein immunology, F-Box Proteins metabolism, Inclusion Bodies metabolism, Multiple System Atrophy metabolism, Parkinson Disease metabolism, alpha-Synuclein metabolism

Abstract

Mutations in the gene encoding the F-box only protein 7 (FBXO7) cause PARK15, an autosomal recessive form of juvenile parkinsonism. Although the brain pathology in PARK15 patients remains unexplored, in vivo imaging displays severe loss of nigrostriatal dopaminergic terminals. Understanding the pathogenesis of PARK15 might therefore illuminate the mechanisms of the selective dopaminergic neuronal degeneration, which could also be important for understanding idiopathic Parkinson disease (PD). The expression of FBXO7 in the human brain remains poorly characterized, and its expression in idiopathic PD and different neurodegenerative diseases has not been investigated. Here, we studied FBXO7 protein expression in brain samples of normal controls (n = 9) and from patients with PD (n = 13), multiple system atrophy (MSA) (n = 5), Alzheimer disease (AD) (n = 5), and progressive supranuclear palsy (PSP) (n = 5) using immunohistochemistry with 2 anti-FBXO7 antibodies. We detected widespread brain FBXO7 immunoreactivity, with the highest levels in neurons of the cerebral cortex, putamen, and cerebellum. There were no major differences between normal and PD brains overall, but FBXO7 immunoreactivity was detected in large proportions of α-synuclein-positive inclusions (Lewy bodies, Lewy neurites, glial cytoplasmic inclusions), where it colocalized with α-synuclein in PD and MSA cases. By contrast, weak FBXO7 immunoreactivity was occasionally detected in tau-positive inclusions in AD and PSP. These findings suggest a role for FBXO7 in the pathogenesis of the synucleinopathies.

Published

2013

12. NPHP4 variants are associated with pleiotropic heart malformations.

Author

French VM, van de Laar IM, Wessels MW, Rohe C, Roos-Hesselink JW, Wang G, Frohn-Mulder IM, Severijnen LA, de Graaf BM, Schot R, Breedveld G, Mientjes E, van Tienhoven M, Jadot E, Jiang Z, Verkerk A, Swagemakers S, Venselaar H, Rahimi Z, Najmabadi H, Meijers-Heijboer H, de Graaff E, Helbing WA, Willemsen R, Devriendt K, Belmont JW, Oostra BA, Amack JD, and Bertoli-Avella AM

Subjects

Amino Acid Sequence, Animals, Cohort Studies, Female, Heart Defects, Congenital diagnosis, Heart Defects, Congenital pathology, Humans, Male, Molecular Sequence Data, Pedigree, Zebrafish, Genetic Pleiotropy genetics, Genetic Variation genetics, Genome-Wide Association Study methods, Heart Defects, Congenital genetics, Proteins genetics

Abstract

Rationale: Congenital heart malformations are a major cause of morbidity and mortality, especially in young children. Failure to establish normal left-right (L-R) asymmetry often results in cardiovascular malformations and other laterality defects of visceral organs., Objective: To identify genetic mutations causing cardiac laterality defects., Methods and Results: We performed a genome-wide linkage analysis in patients with cardiac laterality defects from a consanguineous family. The patients had combinations of defects that included dextrocardia, transposition of great arteries, double-outlet right ventricle, atrioventricular septal defects, and caval vein abnormalities. Sequencing of positional candidate genes identified mutations in NPHP4. We performed mutation analysis of NPHP4 in 146 unrelated patients with similar cardiac laterality defects. Forty-one percent of these patients also had laterality defects of the abdominal organs. We identified 8 additional missense variants that were absent or very rare in control subjects. To study the role of nphp4 in establishing L-R asymmetry, we used antisense morpholinos to knockdown nphp4 expression in zebrafish. Depletion of nphp4 disrupted L-R patterning as well as cardiac and gut laterality. Cardiac laterality defects were partially rescued by human NPHP4 mRNA, whereas mutant NPHP4 containing genetic variants found in patients failed to rescue. We show that nphp4 is involved in the formation of motile cilia in Kupffer's vesicle, which generate asymmetrical fluid flow necessary for normal L-R asymmetry., Conclusions: NPHP4 mutations are associated with cardiac laterality defects and heterotaxy. In zebrafish, nphp4 is essential for the development and function of Kupffer's vesicle cilia and is required for global L-R patterning.

Published

2012

13. Mutations in SLC30A10 cause parkinsonism and dystonia with hypermanganesemia, polycythemia, and chronic liver disease.

Author

Quadri M, Federico A, Zhao T, Breedveld GJ, Battisti C, Delnooz C, Severijnen LA, Di Toro Mammarella L, Mignarri A, Monti L, Sanna A, Lu P, Punzo F, Cossu G, Willemsen R, Rasi F, Oostra BA, van de Warrenburg BP, and Bonifati V

Subjects

Aged, Amino Acid Sequence, Brain metabolism, Cation Transport Proteins metabolism, Chromosome Mapping methods, Female, Frameshift Mutation genetics, Genes, Recessive, Genetic Predisposition to Disease, Hep G2 Cells, Homozygote, Humans, Immunohistochemistry methods, Liver metabolism, Male, Manganese metabolism, Manganese Poisoning metabolism, Membrane Transport Proteins metabolism, Metabolic Diseases metabolism, Middle Aged, Molecular Sequence Data, Phenotype, Sequence Alignment methods, Tumor Cells, Cultured, Zinc Transporter 8, Cation Transport Proteins genetics, Manganese Poisoning genetics, Membrane Transport Proteins genetics, Metabolic Diseases genetics, Parkinsonian Disorders genetics

Abstract

Manganese is essential for several metabolic pathways but becomes toxic in excessive amounts. Manganese levels in the body are therefore tightly regulated, but the responsible protein(s) remain incompletely known. We studied two consanguineous families with neurologic disorders including juvenile-onset dystonia, adult-onset parkinsonism, severe hypermanganesemia, polycythemia, and chronic hepatic disease, including steatosis and cirrhosis. We localized the genetic defect by homozygosity mapping and then identified two different homozygous frameshift SLC30A10 mutations, segregating with disease. SLC30A10 is highly expressed in the liver and brain, including in the basal ganglia. Its encoded protein belongs to a large family of membrane transporters, mediating the efflux of divalent cations from the cytosol. We show the localization of SLC30A10 in normal human liver and nervous system, and its depletion in liver from one affected individual. Our in silico analyses suggest that SLC30A10 possesses substrate specificity different from its closest (zinc-transporting) homologs. We also show that the expression of SLC30A10 and the levels of the encoded protein are markedly induced by manganese in vitro. The phenotype associated with SLC30A10 mutations is broad, including neurologic, hepatic, and hematologic disturbances. Intrafamilial phenotypic variability is also present. Chelation therapy can normalize the manganesemia, leading to marked clinical improvements. In conclusion, we show that SLC30A10 mutations cause a treatable recessive disease with pleomorphic phenotype, and provide compelling evidence that SLC30A10 plays a pivotal role in manganese transport. This work has broad implications for understanding of the manganese biology and pathophysiology in multiple human organs., (Copyright © 2012 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2012

14. Dopaminergic neuronal loss and dopamine-dependent locomotor defects in Fbxo7-deficient zebrafish.

Author

Zhao T, Zondervan-van der Linde H, Severijnen LA, Oostra BA, Willemsen R, and Bonifati V

Subjects

Animals, Apomorphine pharmacology, Body Patterning, Brain metabolism, Disease Models, Animal, Domperidone pharmacology, Dopamine Antagonists pharmacology, Exons, Expressed Sequence Tags, Humans, Immunohistochemistry methods, In Situ Hybridization, Introns, Locomotion, Parkinsonian Disorders metabolism, Phenotype, Protein Structure, Tertiary, RNA, Messenger metabolism, Zebrafish, Dopamine metabolism, F-Box Proteins genetics, F-Box Proteins physiology, Neurons metabolism

Abstract

Recessive mutations in the F-box only protein 7 gene (FBXO7) cause PARK15, a mendelian form of early-onset, levodopa-responsive parkinsonism with severe loss of nigrostriatal dopaminergic neurons. However, the function of the protein encoded by FBXO7, and the pathogenesis of PARK15 remain unknown. No animal models of this disease exist. Here, we report the generation of a vertebrate model of PARK15 in zebrafish. We first show that the zebrafish Fbxo7 homolog protein (zFbxo7) is expressed abundantly in the normal zebrafish brain. Next, we used two zFbxo7-specific morpholinos (targeting protein translation and mRNA splicing, respectively), to knock down the zFbxo7 expression. The injection of either of these zFbxo7-specific morpholinos in the fish embryos induced a marked decrease in the zFbxo7 protein expression, and a range of developmental defects. Furthermore, whole-mount in situ mRNA hybridization showed abnormal patterning and significant decrease in the number of diencephalic tyrosine hydroxylase-expressing neurons, corresponding to the human nigrostriatal or ventral tegmental dopaminergic neurons. Of note, the number of the dopamine transporter-expressing neurons was much more severely depleted, suggesting dopaminergic dysfunctions earlier and larger than those due to neuronal loss. Last, the zFbxo7 morphants displayed severe locomotor disturbances (bradykinesia), which were dramatically improved by the dopaminergic agonist apomorphine. The severity of these morphological and behavioral abnormalities correlated with the severity of zFbxo7 protein deficiency. Moreover, the effects of the co-injection of zFbxo7- and p53-specific morpholinos were similar to those obtained with zFbxo7-specific morpholinos alone, supporting further the contention that the observed phenotypes were specifically due to the knock down of zFbxo7. In conclusion, this novel vertebrate model reproduces pathologic and behavioral hallmarks of human parkinsonism (dopaminergic neuronal loss and dopamine-dependent bradykinesia), representing therefore a valid tool for investigating the mechanisms of selective dopaminergic neuronal death, and screening for modifier genes and therapeutic compounds.

Published

2012

15. Widespread non-central nervous system organ pathology in fragile X premutation carriers with fragile X-associated tremor/ataxia syndrome and CGG knock-in mice.

Author

Hunsaker MR, Greco CM, Spath MA, Smits AP, Navarro CS, Tassone F, Kros JM, Severijnen LA, Berry-Kravis EM, Berman RF, Hagerman PJ, Willemsen R, Hagerman RJ, and Hukema RK

Subjects

Aged, Aged, 80 and over, Animals, Ataxia genetics, Disease Models, Animal, Female, Fragile X Mental Retardation Protein genetics, Gene Knock-In Techniques, Humans, Male, Mice, Mice, Mutant Strains, Organ Specificity genetics, Tremor genetics, Ataxia pathology, Fragile X Syndrome genetics, Fragile X Syndrome pathology, Genetic Carrier Screening, Tremor pathology

Abstract

Fragile X-associated tremor/ataxia syndrome (FXTAS) is an adult-onset neurodegenerative disorder generally presenting with intention tremor and gait ataxia, but with a growing list of co-morbid medical conditions including hypothyroidism, hypertension, peripheral neuropathy, and cognitive decline. The pathological hallmark of FXTAS is the presence of intranuclear inclusions in both neurons and astroglia. However, it is unknown to what extent such inclusions are present outside the central nervous system (CNS). To address this issue, we surveyed non-CNS organs in ten human cases with FXTAS and in a CGG repeat knock-in (CGG KI) mouse model known to possess neuronal and astroglial inclusions. We find inclusions in multiple tissues from FXTAS cases and CGG KI mice, including pancreas, thyroid, adrenal gland, gastrointestinal, pituitary gland, pineal gland, heart, and mitral valve, as well as throughout the associated autonomic ganglia. Inclusions were observed in the testes, epididymis, and kidney of FXTAS cases, but were not observed in mice. These observations demonstrate extensive involvement of the peripheral nervous system and systemic organs. The finding of intranuclear inclusions in non-CNS somatic organ systems, throughout the PNS, and in the enteric nervous system of both FXTAS cases as well as CGG KI mice suggests that these tissues may serve as potential sites to evaluate early intervention strategies or be used as diagnostic factors.

Published

2011

16. Loss of nuclear activity of the FBXO7 protein in patients with parkinsonian-pyramidal syndrome (PARK15).

Author

Zhao T, De Graaff E, Breedveld GJ, Loda A, Severijnen LA, Wouters CH, Verheijen FW, Dekker MC, Montagna P, Willemsen R, Oostra BA, and Bonifati V

Subjects

Aged, Aged, 80 and over, Animals, Brain cytology, Brain metabolism, Brain pathology, Cell Line, F-Box Proteins genetics, Gene Expression Regulation, HEK293 Cells, Humans, Intracellular Space metabolism, Male, Mice, Mutation, Nerve Net cytology, Neurons cytology, Neurons metabolism, Neurons pathology, Parkinsonian Disorders genetics, Protein Isoforms genetics, Protein Isoforms metabolism, Protein Transport, Cell Nucleus metabolism, F-Box Proteins metabolism, Nerve Net metabolism, Nerve Net pathology, Parkinsonian Disorders metabolism, Parkinsonian Disorders pathology

Abstract

Mutations in the F-box only protein 7 gene (FBXO7) cause PARK15, an autosomal recessive neurodegenerative disease presenting with severe levodopa-responsive parkinsonism and pyramidal disturbances. Understanding the PARK15 pathogenesis might thus provide clues on the mechanisms of maintenance of brain dopaminergic neurons, the same which are lost in Parkinson's disease. The protein(s) encoded by FBXO7 remain very poorly characterized. Here, we show that two protein isoforms are expressed from the FBXO7 gene in normal human cells. The isoform 1 is more abundant, particularly in primary skin fibroblasts. Both isoforms are undetectable in cell lines from the PARK15 patient of an Italian family; the isoform 1 is undetectable and the isoform 2 is severely decreased in the patients from a Dutch PARK15 family. In human cell lines and mouse primary neurons, the endogenous or over-expressed, wild type FBXO7 isoform 1 displays mostly a diffuse nuclear localization. An intact N-terminus is needed for the nuclear FBXO7 localization, as N-terminal modification by PARK15-linked missense mutation, or N-terminus tag leads to cytoplasmic mislocalization. Furthermore, the N-terminus of wild type FBXO7 (but not of mutant FBXO7) is able to confer nuclear localization to profilin (a cytoplasmic protein). Our data also suggest that overexpressed mutant FBXO7 proteins (T22M, R378G and R498X) have decreased stability compared to their wild type counterpart. In human brain, FBXO7 immunoreactivity was highest in the nuclei of neurons throughout the cerebral cortex, intermediate in the globus pallidum and the substantia nigra, and lowest in the hippocampus and cerebellum. In conclusion, the common cellular abnormality found in the PARK15 patients from the Dutch and Italian families is the depletion of the FBXO7 isoform 1, which normally localizes in the cell nucleus. The activity of FBXO7 in the nucleus appears therefore crucial for the maintenance of brain neurons and the pathogenesis of PARK15.

Published

2011

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

Author

van de Laar IM, Oldenburg RA, Pals G, Roos-Hesselink JW, de Graaf BM, Verhagen JM, Hoedemaekers YM, Willemsen R, Severijnen LA, Venselaar H, Vriend G, Pattynama PM, Collée M, Majoor-Krakauer D, Poldermans D, Frohn-Mulder IM, Micha D, Timmermans J, Hilhorst-Hofstee Y, Bierma-Zeinstra SM, Willems PJ, Kros JM, Oei EH, Oostra BA, Wessels MW, and Bertoli-Avella AM

Subjects

Age of Onset, Aorta, Thoracic metabolism, Aortic Aneurysm complications, Aortic Aneurysm diagnostic imaging, Chromosomes, Human, Pair 15, Family Health, Female, Humans, Immunohistochemistry methods, Male, Osteoarthritis complications, Osteoarthritis metabolism, Radiography, Signal Transduction, Syndrome, Transforming Growth Factor beta metabolism, Aortic Aneurysm genetics, Mutation, Osteoarthritis genetics, Smad3 Protein genetics

Abstract

Thoracic aortic aneurysms and dissections are a main feature of connective tissue disorders, such as Marfan syndrome and Loeys-Dietz syndrome. We delineated a new syndrome presenting with aneurysms, dissections and tortuosity throughout the arterial tree in association with mild craniofacial features and skeletal and cutaneous anomalies. In contrast with other aneurysm syndromes, most of these affected individuals presented with early-onset osteoarthritis. We mapped the genetic locus to chromosome 15q22.2-24.2 and show that the disease is caused by mutations in SMAD3. This gene encodes a member of the TGF-β pathway that is essential for TGF-β signal transmission. SMAD3 mutations lead to increased aortic expression of several key players in the TGF-β pathway, including SMAD3. Molecular diagnosis will allow early and reliable identification of cases and relatives at risk for major cardiovascular complications. Our findings endorse the TGF-β pathway as the primary pharmacological target for the development of new treatments for aortic aneurysms and osteoarthritis.

Published

2011

18. Images. Different patterns of circulatory shunting in zebrafish caldesmon morphants: a digital motion analysis.

Author

Zheng PP, Severijnen LA, Willemsen R, and Kros JM

Subjects

Animals, Cardiovascular System embryology, Collateral Circulation, Humans, Morphogenesis, Radiographic Image Enhancement instrumentation, Calmodulin-Binding Proteins, Heart embryology, Myocardial Contraction, Radiographic Image Enhancement methods, Zebrafish embryology, Zebrafish Proteins

Published

2010

19. Circulation status of subintestinal vessels is a sensitive parameter for monitoring suboptimal systemic circulation in experimental zebrafish embryos.

Author

Zheng PP, Severijnen LA, Willemsen R, and Kros JM

Subjects

Animals, Blood Circulation physiology, Digestive System blood supply, Neovascularization, Physiologic physiology, Regional Blood Flow physiology, Zebrafish embryology

Published

2009

20. Images in cardiovascular medicine. Functional cardiac phenotypes in zebrafish caldesmon morphants: a digital motion analysis.

Author

Zheng PP, Severijnen LA, Willemsen R, and Kros JM

Subjects

Animals, Cardiovascular System embryology, Heart physiology, Myocardial Contraction physiology, Radiographic Image Enhancement, Zebrafish physiology, Calmodulin-Binding Proteins physiology, Heart embryology, Phenotype, Zebrafish embryology

Published

2009

21. Reduction in fragile X related 1 protein causes cardiomyopathy and muscular dystrophy in zebrafish.

Author

Van't Padje S, Chaudhry B, Severijnen LA, van der Linde HC, Mientjes EJ, Oostra BA, and Willemsen R

Subjects

5' Untranslated Regions genetics, Animals, Base Sequence, Cause of Death, Embryonic Development, Fragile X Syndrome genetics, Fragile X Syndrome veterinary, Heart physiopathology, In Situ Hybridization, Mice, Muscle, Skeletal pathology, Muscle, Skeletal physiology, Myocardium metabolism, Protein Biosynthesis, RNA, Messenger genetics, RNA-Binding Proteins genetics, Zebrafish embryology, Zebrafish growth & development, Fish Diseases genetics, Fragile X Mental Retardation Protein genetics, Muscular Dystrophy, Animal genetics, Zebrafish genetics

Abstract

Lack of the FMR1 gene product causes fragile X syndrome, the commonest inherited cause of mental impairment. We know little of the roles that fragile X related (FXR) gene family members (FMR1, FXR2 and FXR1) play during embryonic development. Although all are expressed in the brain and testis, FXR1 is the principal member found in striated and cardiac muscle. The Fxr1 knockout mice display a striated muscle phenotype but it is not known why they die shortly after birth; however, a cardiac cause is possible. The zebrafish is an ideal model to investigate the role of fxr1 during development of the heart. We have carried out morpholino knockdown of fxr1 and have demonstrated abnormalities of striated muscle development and abnormal development of the zebrafish heart, including failure of looping and snapping of the atrium from its venous pole. In addition, we have measured cardiac function using high-speed video microscopy and demonstrated a significant reduction in cardiac function. This cardiac phenotype has not been previously described and suggests that fxr1 is essential for normal cardiac form and function.

Published

2009

22. Haemoglobin staining for in vivo portraying of functional vasculature in experimental zebrafish embryos.

Author

Zheng PP, Severijnen LA, Willemsen R, and Kros JM

Subjects

Animals, Aorta, Thoracic metabolism, Aorta, Thoracic physiology, Blood Circulation, Endothelium, Vascular metabolism, Staining and Labeling methods, Zebrafish embryology, Blood Vessels physiology, Endothelium, Vascular physiology, Hemoglobins analysis, Zebrafish physiology

Abstract

Characterization of functional vessels is required either for monitoring hemodynamics or patterning of functional vasculature in experimental models. Haemoglobin (Hb) staining is a traditionally used approach for determining the differentiation of erythroid cells. In this investigation, we tested if HB staining can be used for portraying of functional vasculature in experimental zebrafish embryos. The staining sufficiently revealed aortic arches, dorsal aorta, posterior cardinal vein, dorsal longitudinal anastomotic vessels, intersegmental vessels as well as subintestinal vessel basket. We conclude that Hb staining offers an informative and rapid method for in vivo portraying of functional vasculature in experimental zebrafish embryos. It is also suitable for large scale experiments.

Published

2009

23. Cell proliferation and migration are mutually exclusive cellular phenomena in vivo: implications for cancer therapeutic strategies.

Author

Zheng PP, Severijnen LA, van der Weiden M, Willemsen R, and Kros JM

Subjects

Animals, Cell Cycle physiology, Endothelial Cells physiology, Neoplasms blood supply, Neoplasms pathology, Neovascularization, Pathologic, Proliferating Cell Nuclear Antigen metabolism, Zebrafish, Cell Movement drug effects, Cell Proliferation drug effects, Neoplasms therapy

Published

2009

24. A crucial role of caldesmon in vascular development in vivo.

Author

Zheng PP, Severijnen LA, van der Weiden M, Willemsen R, and Kros JM

Subjects

Animals, Humans, Neovascularization, Physiologic, Zebrafish embryology, Blood Vessels embryology, Calmodulin-Binding Proteins physiology

Abstract

Aims: We explored the in vivo effects of knockdown of caldesmon on vascular development in zebrafish., Methods and Results: We investigated the effects of caldesmon knockdown on the vascular development in a zebrafish model with special attention for the trunk and head vessels including the aortic arches. We examined the developing fishes at various time points. The vascular abnormalities observed in the caldesmon morphants were morphologically and functionally characterized in detail in fixed and living embryos. The knockdown of caldesmon caused serious defects in vasculogenesis and angiogenesis in zebrafish morphants, and the vascular integrity and blood circulation were concomitantly impaired., Conclusion: The data provide the first functional assessment of the role of caldesmon in vascular development in vivo, indicating that this molecule plays a crucial role in vasculogenesis and angiogenesis in vivo. Interfering with caldesmon opens new therapeutic avenues for anti-angiogenesis in cancer and ischaemic cardiovascular disease.

Published

2009

25. Reduction of caldesmon expression induces apoptosis and causes disassembly of the sarcomeric protein complex in cardiomyocytes in vivo.

Author

Zheng PP, Severijnen LA, Willemsen R, and Kros JM

Subjects

Animals, Calmodulin-Binding Proteins metabolism, Gene Expression, Zebrafish metabolism, Apoptosis, Calmodulin-Binding Proteins genetics, Myocytes, Cardiac metabolism, Sarcomeres metabolism

Published

2009

26. Caldesmon is essential for cardiac morphogenesis and function: in vivo study using a zebrafish model.

Author

Zheng PP, Severijnen LA, Willemsen R, and Kros JM

Subjects

Animals, Calmodulin-Binding Proteins genetics, Gene Knockdown Techniques, Models, Animal, Zebrafish genetics, Zebrafish metabolism, Zebrafish Proteins genetics, Calmodulin-Binding Proteins physiology, Heart embryology, Heart physiology, Morphogenesis genetics, Zebrafish embryology, Zebrafish Proteins metabolism

Abstract

The zebrafish homologue of caldesmon is similar to the mammalian low molecular weight caldesmon (l-CaD). In this study, we explored the effects of caldesmon knockdown on vertebrate heart development in vivo. In a zebrafish model caldesmon was knocked down resulting in defective cardiac morphogenesis, muscularization and function. The data provide the first functional assessment of the role of caldesmon in cardiac development in vivo, and indicate that caldesmon is essential for proper cardiac organogenesis and function. Because caldesmon expression remarkably influences cardiac muscularization, the findings are relevant for designing future therapeutic strategies in the regeneration of cardiac damage.

Published

2009

27. CGG-repeat length and neuropathological and molecular correlates in a mouse model for fragile X-associated tremor/ataxia syndrome.

Author

Brouwer JR, Huizer K, Severijnen LA, Hukema RK, Berman RF, Oostra BA, and Willemsen R

Subjects

Age Factors, Animals, Cerebral Cortex pathology, Disease Models, Animal, Fragile X Syndrome pathology, Intranuclear Inclusion Bodies genetics, Intranuclear Inclusion Bodies pathology, Male, Mice, RNA, Messenger metabolism, Fragile X Mental Retardation Protein genetics, Fragile X Syndrome genetics, Fragile X Syndrome metabolism, Fragile X Syndrome physiopathology, Trinucleotide Repeat Expansion

Abstract

The 5'untranslated region (UTR) of the FMR1 gene contains a CGG-repeat, which may become unstable upon transmission to the next generation. When repeat length exceeds 200, the FMR1 gene generally undergoes methylation-mediated transcriptional silencing. The subsequent absence of the gene product Fragile X Mental Retardation Protein (FMRP)causes the mental retardation seen in fragile X patients. A CGG-repeat length between 55 and 200 trinucleotides has been termed the premutation (PM). Predominantly elderly male PM carriers are at risk of developing a progressive neurodegenerative disorder: fragile X-associated tremor/ataxia syndrome (FXTAS). All PM carriers have elevated FMR1 mRNA levels, in spite of slightly decreased FMRP levels. The presence of intranuclear ubiquitin-positive inclusions in many brain regions is a neuropathological hallmark of FXTAS. Studies in humans attempting to correlate neuropathological outcomes with molecular measures are difficult because of the limited availability of tissue. Therefore, we have used the expanded CGG-repeat knock-in mouse model of FXTAS to examine the relationship between the molecular and neuropathological parameters in brain. We present Fmr1 mRNA and Fmrp levels and the presence of intranuclear inclusions at different repeat lengths. Contrary to existing hypotheses, our results suggest that inclusion formation may not depend on the elevation per se of Fmr1 transcript levels in aged CGG mice.

Published

2008

28. Elevated Fmr1 mRNA levels and reduced protein expression in a mouse model with an unmethylated Fragile X full mutation.

Author

Brouwer JR, Mientjes EJ, Bakker CE, Nieuwenhuizen IM, Severijnen LA, Van der Linde HC, Nelson DL, Oostra BA, and Willemsen R

Subjects

Alleles, Animals, Brain Chemistry, DNA Methylation, Fragile X Mental Retardation Protein analysis, Humans, Male, Mice, Knockout, Mutation, Protein Biosynthesis, RNA, Messenger analysis, RNA, Messenger metabolism, Transcription, Genetic, Disease Models, Animal, Fragile X Mental Retardation Protein genetics, Fragile X Mental Retardation Protein metabolism, Fragile X Syndrome genetics, Mice genetics, Terminal Repeat Sequences genetics

Abstract

The human FMR1 gene contains a CGG repeat in its 5' untranslated region. The repeat length in the normal population is polymorphic (5-55 CGG repeats). Lengths beyond 200 CGGs (full mutation) result in the absence of the FMR1 gene product, FMRP, through abnormal methylation and gene silencing. This causes Fragile X syndrome, the most common inherited form of mental retardation. Elderly carriers of the premutation, defined as a repeat length between 55 and 200 CGGs, can develop a progressive neurodegenerative syndrome: Fragile X-associated tremor/ataxia syndrome (FXTAS). In FXTAS, FMR1 mRNA levels are elevated and it has been hypothesised that FXTAS is caused by a pathogenic RNA gain-of-function mechanism. We have developed a knock in mouse model carrying an expanded CGG repeat (98 repeats), which shows repeat instability and displays biochemical, phenotypic and neuropathological characteristics of FXTAS. Here, we report further repeat instability, up to 230 CGGs. An expansion bias was observed, with the largest expansion being 43 CGG units and the largest contraction 80 CGG repeats. In humans, this length would be considered a full mutation and would be expected to result in gene silencing. Mice carrying long repeats ( approximately 230 CGGs) display elevated mRNA levels and decreased FMRP levels, but absence of abnormal methylation, suggesting that modelling the Fragile X full mutation in mice requires additional repeats or other genetic manipulation.

Published

2007

29. The DeltaK280 mutation in MAP tau favors exon 10 skipping in vivo.

Author

van Swieten JC, Bronner IF, Azmani A, Severijnen LA, Kamphorst W, Ravid R, Rizzu P, Willemsen R, and Heutink P

Subjects

Alzheimer Disease metabolism, Alzheimer Disease pathology, Blotting, Western methods, Brain metabolism, Brain pathology, Brain ultrastructure, Dementia pathology, Female, Humans, Immunohistochemistry methods, Microscopy, Electron, Transmission methods, Middle Aged, Molecular Weight, Neurons metabolism, Neurons pathology, Serine metabolism, Trinucleotide Repeat Expansion genetics, Dementia genetics, Exons, Lysine genetics, Mutation, tau Proteins genetics

Abstract

Tau mutations in frontotemporal dementia and parkinsonism linked to chromosome 17 (FTDP-17) are associated with changes in alternative splicing of exon 10. The DeltaK280 mutation in exon 10 is exceptional because in vitro observations suggest a dramatic effect on microtubule binding, enhanced self-aggregation, as well as a decrease of the 4R/3R ratio by the ablation of an exon splicing enhancer element. Using immunohistochemistry, Western blotting, and electron microscopy on brain material with the DeltaK280 mutation, we investigated which of these effects is most dominant in vivo. The brain showed abundant Pick bodies in several brain regions, which stained positive with 3-repeat-specific but not with 4-repeat-specific tau antibodies. Western blots of sarkosyl-insoluble tau showed exclusively three repeat (3R0N and 3R1N) tau in most regions, although some 4R1N could be detected in the frontal cortex. In addition, the sarkosyl-soluble tau fraction showed a significantly higher amount of 3-repeat tau. Because quantitative analysis of 4R and 3R mRNA transcripts showed a 4R/3R ratio of only 0.3, association between increased transcription and protein expression was observed. These observations confirm the postulated hypothesis that the DeltaK280 mutation abolishes a splice enhancer element, which overrules the decreased microtubule binding and enhanced self-aggregation.

Published

2007

30. The DNA repair-ubiquitin-associated HR23 proteins are constituents of neuronal inclusions in specific neurodegenerative disorders without hampering DNA repair.

Author

Bergink S, Severijnen LA, Wijgers N, Sugasawa K, Yousaf H, Kros JM, van Swieten J, Oostra BA, Hoeijmakers JH, Vermeulen W, and Willemsen R

Subjects

Animals, Cells, Cultured, Central Nervous System metabolism, Central Nervous System pathology, Central Nervous System physiopathology, DNA Repeat Expansion genetics, DNA-Binding Proteins genetics, Fibroblasts, Humans, Inclusion Bodies genetics, Inclusion Bodies pathology, Mice, Mice, Knockout, Neurodegenerative Diseases genetics, Neurodegenerative Diseases physiopathology, Neurofibrillary Tangles metabolism, Neurofibrillary Tangles pathology, Neurons pathology, Peptides genetics, Peptides metabolism, Peptides toxicity, Proteasome Endopeptidase Complex metabolism, tau Proteins metabolism, DNA Repair genetics, DNA-Binding Proteins metabolism, Inclusion Bodies metabolism, Neurodegenerative Diseases metabolism, Neurons metabolism, Ubiquitin metabolism

Abstract

Intracellular inclusions play a profound role in many neurodegenerative diseases. Here, we report that HR23B and HR23A, proteins that are involved in both DNA repair and shuttling proteins to the 26S proteasome for degradation, accumulate in neuronal inclusions in brain from a mouse model for FXTAS, as well as in brain material from HD, SCA3, SCA7, FTDP-17 and PD patients. Interestingly, HR23B did not significantly accumulate in tau-positive aggregates (neurofibrillary tangles) from AD patients while ubiquitin did. The sequestration of HR23 proteins in intracellular inclusions did not cause detectable accumulation of their stable binding partner in DNA repair, XPC. Surprisingly, no reduction in repair capacity was observed in primary human fibroblasts that overexpressed GFP-polyQ, a polypeptide that induces HR23B-positive inclusions in these transfected cells. This illustrates that impairment of the ubiquitin-proteasome system (UPS) by expanded glutamine repeats, including the sequestration of HR23B, is not affecting NER.

Published

2006

31. Expression profiling suggests underexpression of the GABA(A) receptor subunit delta in the fragile X knockout mouse model.

Author

Gantois I, Vandesompele J, Speleman F, Reyniers E, D'Hooge R, Severijnen LA, Willemsen R, Tassone F, and Kooy RF

Subjects

Animals, Disease Models, Animal, Fragile X Mental Retardation Protein genetics, Gene Expression Profiling, Humans, Immunohistochemistry, Male, Mice, Mice, Knockout, Reverse Transcriptase Polymerase Chain Reaction, Sequence Homology, Nucleic Acid, Brain physiology, Fragile X Syndrome genetics, Oligonucleotide Array Sequence Analysis, Receptors, GABA metabolism

Abstract

It is still unclear why absence of the fragile X protein (FMRP) leads to mental retardation and specific behavioral problems. In neurons, the protein transports specific mRNAs towards the actively translating ribosomes near the synapses. To unravel the mechanism leading to the disorder, we performed global gene expression analysis by means of the differential display method using the fragile X mouse model. To verify differential expression, we used microarray technology and real-time PCR. Three differentially expressed cDNAs showed consistent underexpression in the fragile X knockout mouse, including a GABA(A) receptor subunit delta, a Rho guanine exchange factor 12 and an EST BU563433. In addition, we identified 5 genes that showed differential expression dependent on the sample of RNA analysis. We consider their differential expression as provisional. It is possible that these differentially expressed genes play an important role in the cognitive and behavioral problems observed in the fragile X syndrome.

Published

2006

32. Hereditary Pick's disease with the G272V tau mutation shows predominant three-repeat tau pathology.

Author

Bronner IF, ter Meulen BC, Azmani A, Severijnen LA, Willemsen R, Kamphorst W, Ravid R, Heutink P, and van Swieten JC

Subjects

Blotting, Western, Chromosomes, Human, Pair 17 genetics, DNA Mutational Analysis, Female, Frontal Lobe ultrastructure, Haplotypes, Humans, Male, Middle Aged, Nerve Tissue Proteins metabolism, Pedigree, Pick Disease of the Brain metabolism, Pick Disease of the Brain pathology, tau Proteins metabolism, Mutation, Nerve Tissue Proteins genetics, Pick Disease of the Brain genetics, tau Proteins genetics

Abstract

Frontotemporal dementia and parkinsonism linked to chromosome 17 have been associated with mutations in the microtubule associated protein tau (MAPT or tau) gene. This disorder is characterized by a large spectrum of neuronal and glial tau lesions in different brain regions. Pick bodies were found in a family with hereditary Pick's disease with the G272V mutation and in several families with other tau mutations in exons 9 and 11-13. The biochemical composition of Pick bodies varies between these mutations. Until recently, no detailed biochemical characterization of G272V brain material was done owing to unavailability of fresh frozen brain material. We now report a detailed study using the immunohistochemistry, western blots and electron microscopy of two brains with the G272V mutation that recently became available. Both brains showed severe neuronal loss in the temporal cortex, whereas in the frontal cortex the loss was less; and abundant Pick bodies in the dentate gyrus of the hippocampus, and caudate nucleus. The Pick bodies consisted exclusively of three-repeat (3R) isoforms, as was demonstrated by isoform-specific antibodies and supported by western blot analysis of sarkosyl-insoluble tau. These observations confirm that this family diagnosed with hereditary Pick disease meets all the criteria for this condition, including the presence of Pick bodies that are unphosphorylated at Ser262 and contain twisted filaments with long periodicity consisting only of 3R tau.

Published

2005

33. Characterisation of Fmrp in zebrafish: evolutionary dynamics of the fmr1 gene.

Author

van 't Padje S, Engels B, Blonden L, Severijnen LA, Verheijen F, Oostra BA, and Willemsen R

Subjects

Amino Acid Sequence, Animals, Base Sequence, Blotting, Western, Brain Chemistry genetics, COS Cells, Chlorocebus aethiops, Conserved Sequence, Embryo, Nonmammalian, Fragile X Mental Retardation Protein, Fragile X Syndrome, Immunohistochemistry, Models, Animal, Molecular Sequence Data, Nerve Tissue Proteins chemistry, Nuclear Localization Signals genetics, Protein Structure, Tertiary, RNA-Binding Proteins chemistry, Sequence Homology, Amino Acid, Sequence Homology, Nucleic Acid, Transfection, Zebrafish embryology, Evolution, Molecular, Gene Expression Regulation, Developmental, Nerve Tissue Proteins genetics, RNA-Binding Proteins genetics, Zebrafish genetics

Abstract

Fragile X syndrome is the most common inherited form of mental retardation. It is caused by the lack of the Fragile X Mental Retardation Protein (FMRP), which is encoded by the FMR1 gene. Although Fmr1 knockout mice display some characteristics also found in fragile X patients, it is a complex animal model to study brain abnormalities, especially during early embryonic development. Interestingly, the ortholog of the FMR1 gene has been identified not only in mouse, but also in zebrafish (Danio rerio). In this study, an amino acid sequence comparison of FMRP orthologs was performed to determine the similar regions of FMRP between several species, including human, mouse, frog, fruitfly and zebrafish. Further characterisation of Fmrp has been performed in both adults and embryos of zebrafish using immunohistochemistry and western blotting with specific antibodies raised against zebrafish Fmrp. We have demonstrated a strong Fmrp expression in neurons of the brain and only a very weak expression in the testis. In brain tissue, a different distribution of the isoforms of Fmrp, compared to human and mouse brain tissue, was shown using western blot analysis. Due to the high similarity between zebrafish Fmrp and human FMRP and their similar expression pattern, the zebrafish has great potential as a complementary animal model to study the pathogenesis of the fragile X syndrome, especially during embryonic development.

Published

2005

34. Two members of the Fxr gene family, Fmr1 and Fxr1, are differentially expressed in Xenopus tropicalis.

Author

Blonden L, van 't Padje S, Severijnen LA, Destree O, Oostra BA, and Willemsen R

Subjects

Amino Acid Sequence, Animals, Fragile X Mental Retardation Protein chemistry, Fragile X Mental Retardation Protein genetics, Gene Expression Regulation, Developmental, Humans, In Situ Hybridization, Models, Animal, Molecular Sequence Data, RNA-Binding Proteins chemistry, RNA-Binding Proteins metabolism, Sequence Homology, Amino Acid, Xenopus Proteins chemistry, Xenopus Proteins genetics, Fragile X Mental Retardation Protein metabolism, Fragile X Syndrome genetics, Intellectual Disability genetics, RNA-Binding Proteins genetics, Xenopus genetics, Xenopus Proteins metabolism

Abstract

The Fxr gene family is composed of three members, FMR1, FXR1 and FXR2. The FMR1 gene is involved in the fragile X syndrome, whereas for the other two members, no human disorder has been identified yet. An appropriate animal model to study in vivo gene function is essential to unravel the cellular function of the gene products FMRP, FXR1P and FXR2P, respectively. In Xenopus tropicalis both Fmr1 and Fxr1 were identified; however, unexpectedly Fxr2 was not. Here we describe the characterization of both Fmrp and Fxr1p in Xenopus tropicalis. Fmrp is expressed ubiquitously throughout the embryo during embryonic development, whereas Fxr1p shows a more tissue-specific expression particularly during late embryonic development. In adult frogs both proteins are highly expressed in most neurons of the central nervous system and in all spermatogenic cells in the testis. In addition, Fxr1p is also highly expressed in striated muscle tissue. Western blotting experiments revealed only one prominent isoform for both proteins using different tissue homogenates from adult frogs. Thus, for in vivo gene function studies, this relative simple animal model may serve as a highly advantageous and complementary model.

Published

2005

35. Transport kinetics of FMRP containing the I304N mutation of severe fragile X syndrome in neurites of living rat PC12 cells.

Author

Schrier M, Severijnen LA, Reis S, Rife M, van't Padje S, van Cappellen G, Oostra BA, and Willemsen R

Subjects

Amino Acid Substitution genetics, Animals, Axonal Transport genetics, Cytoplasmic Granules genetics, Cytoplasmic Granules metabolism, Fragile X Mental Retardation Protein, Fragile X Syndrome genetics, Fragile X Syndrome physiopathology, Green Fluorescent Proteins, Kinetics, Luminescent Proteins genetics, Luminescent Proteins metabolism, Macromolecular Substances, Microtubules genetics, Microtubules metabolism, Myelin P0 Protein metabolism, Nerve Tissue Proteins genetics, Neurites ultrastructure, PC12 Cells, Protein Transport genetics, RNA-Binding Proteins genetics, Rats, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Fragile X Syndrome metabolism, Mutation genetics, Nerve Tissue Proteins metabolism, Neurites metabolism, RNA-Binding Proteins metabolism

Abstract

Lack of fragile X mental retardation protein (FMRP) causes the fragile X syndrome, a common form of inherited mental retardation. The syndrome usually results from the expansion of a CGG repeat in the FMR1 gene with consequent transcriptional silencing of FMR1. However, one missense mutation (Ile304Asn) was reported in the second KH domain of the protein involved in RNA binding. The protein containing this mutation showed an impaired function, leading to an extremely severe phenotype. In the present report, we have studied the role of FMRP I304N in living PC12 cells to better understand the (dys) function of this mutant FMRP. We have generated an FMR1 I304N-EGFP stably transfected PC12 cell line with an inducible expression system (Tet-On) for regulated expression of the FMRP I304N-EGFP fusion protein. After Dox-induction, FMRP I304N-EGFP was localized in the neurites of PC12 cells; however, no granules were formed as has been recently demonstrated for the normal FMRP. Time-lapse microscopy in combination with bleaching technology illustrated that although FMRP I304N-EGFP does not form visible granules, the transport into the neurites is microtubule dependent. Immunoprecipitation with antibodies against GFP demonstrates that FMRP I304N-EGFP coprecipitate with both the 60S ribosomal protein P0 and FXR1P, suggesting that the mutant FMRP is still able to form complexes, however, with different characteristics compared to normal FMRP.

Published

2004

36. Characterization of Fxr1 in Danio rerio; a simple vertebrate model to study costamere development.

Author

Engels B, van 't Padje S, Blonden L, Severijnen LA, Oostra BA, and Willemsen R

Subjects

Amino Acid Sequence, Animals, Base Sequence, Blotting, Western, Cryoultramicrotomy, DNA Primers, Immunohistochemistry, Molecular Sequence Data, RNA-Binding Proteins metabolism, Sequence Alignment, Sequence Analysis, DNA, Zebrafish genetics, Gene Expression Profiling, Models, Animal, Zebrafish metabolism

Abstract

The X-linked FMR1 gene, which is involved in the fragile X syndrome, forms a small gene family with its two autosomal homologs, FXR1 and FXR2. Mouse models for the FXR genes have been generated and proved to be valuable in elucidating the function of these genes, particularly in adult mice. Unfortunately, Fxr1 knockout mice die shortly after birth, necessitating an animal model that allows the study of the role of Fxr1p, the gene product of Fxr1, in early embryonic development. For gene function studies during early embryonic development the use of zebrafish as a model organism is highly advantageous. In this paper the suitability of the zebrafish as a model organism to study Fxr1p function during early development is explored. As a first step, we present here the initial characterization of Fxr1p in zebrafish. Fxr1p is present in all the cells from zebrafish embryos from the 2/4-cell stage onward; however, during late development a more tissue-specific distribution is found, with the highest expression in developing muscle. In adult zebrafish, Fxr1p is localized at the myoseptum and in costamere-like granules in skeletal muscle. In the testis, Fxr1p is localized in immature spermatogenic cells and in brain tissue Fxr1p displays a predominantly nuclear staining in neurons throughout the brain. Finally, the different tissue-specific isoforms of Fxr1p are characterized. Since the functional domains and the expression pattern of Fxr1p in zebrafish are comparable to those in higher vertebrates such as mouse and human, we conclude that the zebrafish is a highly suitable model for functional studies of Fxr1p.

Published

2004

37. Proteomic analysis of exosomes isolated from human malignant pleural effusions.

Author

Bard MP, Hegmans JP, Hemmes A, Luider TM, Willemsen R, Severijnen LA, van Meerbeeck JP, Burgers SA, Hoogsteden HC, and Lambrecht BN

Subjects

Aged, Breast Neoplasms pathology, Carcinoma secondary, Complement System Proteins analysis, Endosomes metabolism, Endosomes ultrastructure, Female, Humans, Immunoglobulins immunology, Lung Neoplasms pathology, Lung Neoplasms secondary, Male, Mesothelioma metabolism, Mesothelioma pathology, Microscopy, Electron, Middle Aged, Neoplasm Proteins analysis, Ovarian Neoplasms pathology, Pleural Effusion, Malignant pathology, Predictive Value of Tests, Secretory Vesicles pathology, Secretory Vesicles ultrastructure, Serpins analysis, Sorting Nexins, Thrombospondins analysis, Ultracentrifugation methods, Biomarkers, Tumor analysis, Carrier Proteins analysis, Eye Proteins, Lung Neoplasms metabolism, Nerve Growth Factors, Pleural Effusion, Malignant metabolism, Proteins analysis, Proteomics, Secretory Vesicles metabolism, Vesicular Transport Proteins analysis

Abstract

Exosomes are membrane vesicles from endosomal origin secreted by various cells such as hematopoietic, epithelial, and tumor cells. Exosomes secreted by tumor cells contain specific antigens potentially useful for immunotherapeutic purposes. Our aim was to determine if exosomes are present in human cancerous pleural effusions and to identify their proteomic content. Exosomes were purified by sucrose gradient ultracentrifugation, and electron microscopy was used to check both concentration and purity of exosomes. Proteins were separated by one-dimensional sodium dodecyl sulfate-polyacrylamide gel electrophoresis, and protein bands were identified by matrix-assisted laser desorption ionization time-of-flight mass spectrometry and Western blotting. Exosomes were present in pleural fluid obtained from patients suffering from mesothelioma (n = 4), lung cancer (n = 2), breast cancer (n = 2), and ovarian cancer (n = 1). As previously reported by others, antigen-presenting molecules, cytoskeletal proteins, and signal transduction-involved proteins were present. Proteins not previously reported were identified (SNX25, BTG1, PEDF, thrombospondin 2). Different types of immunoglobulins and complement factors were abundantly present in the sucrose fractions containing exosomes. Exosome-directed specificity of these immunoglobulins was not observed. In conclusion, sucrose gradient ultracentrifugation allows isolation of exosomes from malignant pleural effusions. However, pleural fluid proteins and especially immunoglobulins are coisolated and may hamper the use of exosomes isolated from malignant effusion for immunotherapy programs.

Published

2004

38. DJ-1 colocalizes with tau inclusions: a link between parkinsonism and dementia.

Author

Rizzu P, Hinkle DA, Zhukareva V, Bonifati V, Severijnen LA, Martinez D, Ravid R, Kamphorst W, Eberwine JH, Lee VM, Trojanowski JQ, and Heutink P

Subjects

Aged, Aged, 80 and over, Animals, Brain metabolism, COS Cells, Chlorocebus aethiops, Dementia metabolism, HeLa Cells, Humans, Immunoblotting, Immunohistochemistry, Inclusion Bodies ultrastructure, Intracellular Signaling Peptides and Proteins, Middle Aged, Neurofibrillary Tangles metabolism, Neurofibrillary Tangles pathology, Oncogene Proteins genetics, Parkinsonian Disorders metabolism, Protein Deglycase DJ-1, Transfection, Brain pathology, Dementia pathology, Inclusion Bodies metabolism, Oncogene Proteins metabolism, Parkinsonian Disorders pathology, tau Proteins metabolism

Abstract

Two novel mutations recently have been identified in the DJ-1 gene that cause a new form of autosomal recessive, early-onset parkinsonism. Because the pathological role of this protein is unknown, we examined the issue here and report the colocalization of DJ-1 protein within a subset of pathological tau inclusions in a diverse group of neurodegenerative disorders known as tauopathies. Our study extends the view that different neurodegenerative diseases may have similar pathological mechanisms, and that these processes likely include DJ-1.

Published

2004

39. NUFIP1 (nuclear FMRP interacting protein 1) is a nucleocytoplasmic shuttling protein associated with active synaptoneurosomes.

Author

Bardoni B, Willemsen R, Weiler IJ, Schenck A, Severijnen LA, Hindelang C, Lalli E, and Mandel JL

Subjects

Active Transport, Cell Nucleus genetics, Animals, Animals, Newborn, Brain metabolism, Brain ultrastructure, Cell Compartmentation genetics, Cell Nucleus ultrastructure, Fragile X Mental Retardation Protein, Fragile X Syndrome genetics, HeLa Cells, Humans, Karyopherins genetics, Karyopherins metabolism, Male, Mice, Microscopy, Electron, Nerve Tissue Proteins metabolism, Nuclear Matrix genetics, Nuclear Matrix metabolism, Nuclear Matrix ultrastructure, Nuclear Proteins genetics, Presynaptic Terminals metabolism, Presynaptic Terminals ultrastructure, Protein Biosynthesis genetics, RNA biosynthesis, RNA genetics, RNA-Binding Proteins genetics, Rats, Ribosomes genetics, Ribosomes metabolism, Ribosomes ultrastructure, Signal Transduction genetics, Synaptosomes, Testis metabolism, Testis ultrastructure, Exportin 1 Protein, Cell Nucleus metabolism, Fragile X Syndrome metabolism, Nuclear Proteins metabolism, Organelles metabolism, RNA-Binding Proteins metabolism, Receptors, Cytoplasmic and Nuclear

Abstract

Fragile X syndrome, the most common cause of inherited mental retardation, is caused by the absence of FMRP (Fragile X Mental Retardation Protein). FMRP is an RNA binding protein reported to be involved in translational control, notably at postsynaptic sites of protein synthesis as a part of a multiprotein/mRNA complex. One of the FMRP interactors, NUFIP1, is an RNA binding protein with an expression profile matching that of FMRP. We now show that in the nucleus NUFIP1 is localized in the nuclear matrix in RNA-containing structures lying in the proximity of, but not overlapping with, sites of nascent RNA. NUFIP1 is also present in the cytoplasm, where it is associated with ribosomes, similarly to FMRP. In neurons NUFIP1 can be detected in functional synaptoneurosomes, colocalizing with ribosomes. Consistent with its subcellular localization in both nucleus and cytoplasm, we show that NUFIP1 contains a functional CRM1-dependent nuclear export signal and is able to shuttle between these two cellular compartments. These findings suggest the involvement of NUFIP1 in the export and localization of mRNA and, in association with FMRP, in the regulation of local protein synthesis near synapses.

Published

2003

40. FMRP expression studies in blood and hair roots in a fragile X family with methylation mosaics.

Author

de Vries BB, Severijnen LA, Jacobs A, Olmer R, Halley DJ, Oostra BA, and Willemsen R

Subjects

Blotting, Southern, Child, Child, Preschool, DNA genetics, DNA metabolism, Family Health, Fragile X Mental Retardation Protein, Fragile X Syndrome metabolism, Fragile X Syndrome psychology, Humans, Intelligence, Male, Mutation, Nerve Tissue Proteins blood, Nerve Tissue Proteins metabolism, Pedigree, DNA Methylation, Fragile X Syndrome genetics, Hair metabolism, Lymphocytes metabolism, Nerve Tissue Proteins genetics, RNA-Binding Proteins

Published

2003

41. Morphological changes in muscle tissue of patients with infantile Pompe's disease receiving enzyme replacement therapy.

Author

Winkel LP, Kamphoven JH, van den Hout HJ, Severijnen LA, van Doorn PA, Reuser AJ, and van der Ploeg AT

Subjects

Animals, Dose-Response Relationship, Drug, Endothelium, Vascular metabolism, Endothelium, Vascular pathology, Endothelium, Vascular ultrastructure, Female, Glycogen metabolism, Glycogen Storage Disease Type II metabolism, Humans, Infant, Lysosomes metabolism, Lysosomes pathology, Lysosomes ultrastructure, Male, Microscopy, Electron, Muscle Fibers, Skeletal metabolism, Muscle Fibers, Skeletal pathology, Muscle Fibers, Skeletal ultrastructure, Muscle, Skeletal enzymology, Myocytes, Smooth Muscle metabolism, Myocytes, Smooth Muscle pathology, Myocytes, Smooth Muscle ultrastructure, Peripheral Nerves metabolism, Peripheral Nerves pathology, Rabbits, Recombinant Fusion Proteins pharmacology, Recombinant Fusion Proteins therapeutic use, Schwann Cells metabolism, Schwann Cells pathology, Treatment Outcome, alpha-Glucosidases deficiency, Glycogen Storage Disease Type II drug therapy, Glycogen Storage Disease Type II pathology, Muscle, Skeletal drug effects, Muscle, Skeletal pathology, alpha-Glucosidases pharmacology, alpha-Glucosidases therapeutic use

Abstract

Pompe's disease (glycogen storage disease type II) is an autosomal recessive myopathy caused by lysosomal alpha-glucosidase deficiency. Enzyme replacement therapy (ERT) is currently under development for this disease. We evaluated the morphological changes in muscle tissue of four children with infantile Pompe's disease who received recombinant human alpha-glucosidase from rabbit milk for 72 weeks. The patients were 2.5-8 months of age at entry. Prior to treatment, all patients showed lysosomal glycogen storage in skeletal and smooth muscle cells, vascular endothelium, Schwann cells, and perineurium. The first response to treatment was noticed in vascular endothelium and in peripheral nerves after 12 weeks of treatment at an enzyme dose of 15-20 mg/kg. Increasing the dose to 40 mg/kg led, after 72 weeks of treatment, to a reduction of glycogen storage and substantial improvement of muscle architecture in the least affected patient. Not all patients responded equally well, possibly due to differences in degree of glycogen storage and concomitant muscle pathology at the start of treatment. We conclude that intravenous administration of recombinant human alpha-glucosidase from rabbit milk can improve muscle morphology in classic infantile Pompe's disease when treatment is started before irreversible damage has occurred.

Published

2003

42. Predictive testing for cognitive functioning in female carriers of the fragile X syndrome using hair root analysis.

Author

Willemsen R, Smits A, Severijnen LA, Jansen M, Jacobs A, De Bruyn E, and Oostra B

Subjects

Case-Control Studies, Cognition Disorders complications, Cognition Disorders diagnosis, Female, Fragile X Mental Retardation Protein, Fragile X Syndrome diagnosis, Fragile X Syndrome physiopathology, Humans, Intelligence Tests, Predictive Value of Tests, Prognosis, Trinucleotide Repeats genetics, Cognition Disorders genetics, Cognition Disorders physiopathology, Fragile X Syndrome complications, Fragile X Syndrome genetics, Hair Follicle metabolism, Heterozygote, Nerve Tissue Proteins genetics, RNA-Binding Proteins

Published

2003

43. The FMR1 CGG repeat mouse displays ubiquitin-positive intranuclear neuronal inclusions; implications for the cerebellar tremor/ataxia syndrome.

Author

Willemsen R, Hoogeveen-Westerveld M, Reis S, Holstege J, Severijnen LA, Nieuwenhuizen IM, Schrier M, van Unen L, Tassone F, Hoogeveen AT, Hagerman PJ, Mientjes EJ, and Oostra BA

Subjects

Animals, Cell Nucleus pathology, Fragile X Mental Retardation Protein, Humans, Immunohistochemistry, Mice, Mice, Transgenic, Neurons pathology, Cell Nucleus metabolism, Cerebellar Ataxia genetics, Nerve Tissue Proteins genetics, Neurons metabolism, RNA-Binding Proteins, Trinucleotide Repeat Expansion, Ubiquitin metabolism

Abstract

Recent studies have reported that alleles in the premutation range in the FMR1 gene in males result in increased FMR1 mRNA levels and at the same time mildly reduced FMR1 protein levels. Some elderly males with premutations exhibit an unique neurodegenerative syndrome characterized by progressive intention tremor and ataxia. We describe neurohistological, biochemical and molecular studies of the brains of mice with an expanded CGG repeat and report elevated Fmr1 mRNA levels and intranuclear inclusions with ubiquitin, Hsp40 and the 20S catalytic core complex of the proteasome as constituents. An increase was observed of both the number and the size of the inclusions during the course of life, which correlates with the progressive character of the cerebellar tremor/ataxia syndrome in humans. The observations in expanded-repeat mice support a direct role of the Fmr1 gene, by either CGG expansion per se or by mRNA level, in the formation of the inclusions and suggest a correlation between the presence of intranuclear inclusions in distinct regions of the brain and the clinical features in symptomatic premutation carriers. This mouse model will facilitate the possibilities to perform studies at the molecular level from onset of symptoms until the final stage of the disease.

Published

2003

44. Transport of fragile X mental retardation protein via granules in neurites of PC12 cells.

Author

De Diego Otero Y, Severijnen LA, van Cappellen G, Schrier M, Oostra B, and Willemsen R

Subjects

Animals, Anti-Bacterial Agents pharmacology, Antineoplastic Agents pharmacology, Cytochalasin D pharmacology, Cytoplasmic Granules chemistry, Doxycycline pharmacology, Fragile X Mental Retardation Protein, Fragile X Syndrome metabolism, Gene Expression Regulation, Green Fluorescent Proteins, Humans, Indicators and Reagents metabolism, Intellectual Disability, Luminescent Proteins genetics, Luminescent Proteins metabolism, Microscopy, Confocal, Nerve Tissue Proteins genetics, Nocodazole pharmacology, Nucleic Acid Synthesis Inhibitors pharmacology, PC12 Cells, Protein Transport, RNA, Messenger metabolism, RNA-Binding Proteins metabolism, Rats, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Time Factors, Cytoplasmic Granules metabolism, Nerve Tissue Proteins metabolism, Neurites metabolism

Abstract

Lack of fragile X mental retardation protein (FMRP) causes fragile X syndrome, a common form of inherited mental retardation. FMRP is an RNA binding protein thought to be involved in translation efficiency and/or trafficking of certain mRNAs. Recently, a subset of mRNAs to which FMRP binds with high affinity has been identified. These FMRP-associated mRNAs contain an intramolecular G-quartet structure. In neurons, dendritic mRNAs are involved in local synthesis of proteins in response to synaptic activity, and this represents a mechanism for synaptic plasticity. To determine the role of FMRP in dendritic mRNA transport, we have generated a stably FMR1-enhanced green fluorescent protein (EGFP)-transfected PC12 cell line with an inducible expression system (Tet-On) for regulated expression of the FMRP-GFP fusion protein. After doxycycline induction, FMRP-GFP was localized in granules in the neurites of PC12 cells. By using time-lapse microscopy, the trafficking of FMRP-GFP granules into the neurites of living PC12 cells was demonstrated. Motile FMRP-GFP granules displayed two types of movements: oscillatory (bidirectional) and unidirectional anterograde. The average velocity of the granules was 0.19 micro m/s with a maximum speed of 0.71 micro m/s. In addition, we showed that the movement of FMRP-GFP labeled granules into the neurites was microtubule dependent. Colocalization studies further showed that the FMRP-GFP labeled granules also contained RNA, ribosomal subunits, kinesin heavy chain, and FXR1P molecules. This report is the first example of trafficking of RNA-containing granules with FMRP as a core constituent in living PC12 cells.

Published

2002

45. Timing of the absence of FMR1 expression in full mutation chorionic villi.

Author

Willemsen R, Bontekoe CJ, Severijnen LA, and Oostra BA

Subjects

Alleles, Dosage Compensation, Genetic, Embryonic and Fetal Development genetics, Female, Fragile X Mental Retardation Protein, Fragile X Syndrome diagnosis, Gene Expression, Gestational Age, Humans, Immunohistochemistry, Male, Pregnancy, Prenatal Diagnosis, X Chromosome genetics, Chorionic Villi metabolism, Fragile X Syndrome embryology, Fragile X Syndrome genetics, Mutation, Nerve Tissue Proteins genetics, RNA-Binding Proteins

Abstract

Fragile X syndrome is caused by the expansion of the CGG repeat in the 5' untranslated region of the FMR1 gene. This expansion leads to methylation of the FMR1 promoter region thereby blocking FMR1 protein (FMRP) expression. Prenatal diagnosis can be performed on chorionic villi samples (CVS) by Southern blot analysis. Alternatively, for males, an immunohistochemical method has been introduced for CVS. In this study, we have used this immunocytochemical method for CVS in full mutation male fetuses at different times of gestational age, varying from 10.0-12.5 weeks, and in two cases of full mutation female fetuses (>13 weeks). FMRP expression studies in CVS from full mutation male fetuses (10.0-12.5 weeks) illustrate the timing of the disappearance of FMRP expression in these CVS. Until approximately 10 weeks of gestation, FMRP is expressed normally in full mutation male CVS, whereas FMRP is completely absent at 12.5 weeks of gestation. FMRP expression in full mutation female CVS (>13 weeks) is completely absent in a number of villi, whereas other villi show normal FMRP expression. Unlabelled villi can only be present in the absence of the expression of the full mutation FMR1 gene on one X-chromosome together with the X-inactivation of the normal X allele. FMRP positive villi can be explained by an active normal X allele. The presence of both positive and negative villi indicates that X-inactivation in human CVS is a random process. No villi are found with a mixture of both FMRP-expressing and non-FMRP-expressing cells. This indicates that X-inactivation occurs very early in development, before the villi start to proliferate, and that X-inactivation in villi is a clonal process. In addition, our results indicate that the timing of both X-inactivation and full mutation FMR1 allele inactivation is different, i.e. X-inactivation occurs earlier in development than inactivation of the full mutation.

Published

2002

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

Author

Rosso SM, van Herpen E, Deelen W, Kamphorst W, Severijnen LA, Willemsen R, Ravid R, Niermeijer MF, Dooijes D, Smith MJ, Goedert M, Heutink P, and van Swieten JC

Subjects

Adult, DNA genetics, Exons genetics, Humans, Male, Microscopy, Electron, Microtubules drug effects, Microtubules physiology, Recombinant Proteins pharmacology, Ultrasonography, tau Proteins pharmacology, Alzheimer Disease genetics, Alzheimer Disease pathology, Inclusion Bodies diagnostic imaging, Mutation, Missense physiology, Pick Disease of the Brain pathology, tau Proteins genetics

Abstract

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

47. Fluticasone propionate aqueous nasal spray reduces inflammatory cells in unchallenged allergic nasal mucosa: effects of single allergen challenge.

Author

Holm A, Dijkstra M, Kleinjan A, Severijnen LA, Boks S, Mulder P, and Fokkens W

Subjects

Administration, Intranasal, Adolescent, Adult, Androstadienes administration & dosage, CD4-Positive T-Lymphocytes drug effects, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes drug effects, CD8-Positive T-Lymphocytes immunology, Double-Blind Method, Female, Fluticasone, Humans, Immunohistochemistry, Male, Middle Aged, Rhinitis, Allergic, Seasonal immunology, Androstadienes therapeutic use, Anti-Allergic Agents therapeutic use, Nasal Mucosa drug effects, Rhinitis, Allergic, Seasonal drug therapy

Abstract

Background: Topical corticosteroid therapy reduces symptoms and nasal mucosal inflammatory cells in patients with allergic rhinitis. Usually patients are advised to start their medication (1 week) before the beginning of the pollen season. The effect of pretreatment with a topical corticosteroid on unchallenged nasal mucosa is not well documented., Objectives: The purpose of this study was to investigate, in a double-blind, placebo-controlled study, the effect of 6 weeks' pretreatment with 200 microg twice daily fluticasone propionate on nasal symptoms and inflammatory cell numbers after nasal allergen provocation in patients with seasonal allergic rhinitis., Methods: Nineteen patients with grass pollen-induced allergic rhinitis were treated for a 6-week period out of the grass pollen season. After completing the treatment period, patients were challenged with grass pollen. Nasal mucosal biopsy specimens were taken 5 times in every patient. In nasal mucosa changes in numbers of T cells, B cells, mast cells, eosinophils, macrophages, and Langerhans' cells were investigated., Results: After 4 weeks of treatment but before allergen provocation, significantly fewer epithelial Langerhans' cells, macrophages, mast cells, T cells, and eosinophils were found in the fluticasone propionate group compared with those found in the placebo group. In the lamina propria significantly fewer Langerhans' cells and eosinophils were found in the fluticasone propionate group. Cell influx in nasal mucosa after allergen provocation was significantly inhibited in the fluticasone propionate group compared with that in the placebo group for epithelial Langerhans' cells, mast cells, macrophages, and T cells and for lamina propria eosinophils, mast cells, Langerhans' cells, macrophages, and T cells., Conclusions: Fluticasone propionate is effective in reducing early- and late-phase nasal symptoms. Topical corticosteroid treatment reduces inflammatory cells in unchallenged nasal mucosa.

Published

2001

48. Increase in IL-8, IL-10, IL-13, and RANTES mRNA levels (in situ hybridization) in the nasal mucosa after nasal allergen provocation.

Author

KleinJan A, Dijkstra MD, Boks SS, Severijnen LA, Mulder PG, and Fokkens WJ

Subjects

Adult, Biopsy, Cell Count, Chemokine CCL5 biosynthesis, Eosinophilia genetics, Eosinophilia metabolism, Eosinophils, Female, Humans, In Situ Hybridization, Interferon-gamma genetics, Interleukin-10 biosynthesis, Interleukin-13 biosynthesis, Interleukin-8 biosynthesis, Interleukins genetics, Male, Middle Aged, Nasal Mucosa pathology, Poaceae, Rhinitis, Allergic, Seasonal genetics, Rhinitis, Allergic, Seasonal pathology, Seasons, Tumor Necrosis Factor-alpha genetics, Allergens, Chemokine CCL5 genetics, Eosinophilia etiology, Interleukin-10 genetics, Interleukin-13 genetics, Interleukin-8 genetics, Nasal Mucosa metabolism, Nasal Provocation Tests, Pollen immunology, RNA, Messenger biosynthesis, Rhinitis, Allergic, Seasonal metabolism

Abstract

Background: Allergic inflammation is regulated by the local production and release of several cytokines., Objectives: This study was designed to assess the changes in mRNA cytokine-positive cells after allergen provocation and to compare these cytokines with tissue eosinophilia as a marker of allergic inflammation., Methods: A grass pollen allergen provocation study was conducted in autumn, out of the hay fever season. Nasal mucosal biopsy specimens were taken before provocation and 1 hour, 24 hours, and 1 week after allergen provocation. Eosinophils and mRNA-positive cells (in situ hybridization for IL-2, IL-3, IL-4, IL-5, IL-6, IL-8, IL-10, IL-13, IFN-gamma, RANTES, and TNF-alpha) were assessed in the biopsy specimens., Results: After allergen provocation, an increase in cell number was found for eosinophils and cells expressing mRNA for the chemokines IL-8 and RANTES and for the TH2 cytokines IL-10 and IL-13. Significant correlations were found between eosinophils and RANTES and eosinophils and IFN-gamma in the early phase and between eosinophils and IL-5 and eosinophils and RANTES in the late phase. The increase in eosinophils and IL-10 and IL-13 mRNA-positive cells could still be observed 1 week after allergen provocation., Conclusions: Nasal allergen provocation induced significant tissue eosinophilia and a significant increase in IL-8, IL-13, and RANTES mRNA-positive cells. A significant increase in eosinophils and IL-10 and IL-13 mRNA-positive cells compared with baseline can still be observed 1 week after a single allergen provocation.

Published

1999

49. The long-term effects of capsaicin aqueous spray on the nasal mucosa.

Author

Blom HM, Severijnen LA, Van Rijswijk JB, Mulder PG, Van Wijk RG, and Fokkens WJ

Subjects

Administration, Intranasal, Adolescent, Adult, Antigens, CD analysis, Biopsy, Capsaicin pharmacology, Cell Count drug effects, Chymases, Double-Blind Method, Epithelial Cells chemistry, Epithelial Cells cytology, Epithelial Cells drug effects, Female, Humans, Immunoglobulin E analysis, Immunohistochemistry, Male, Middle Aged, Nasal Mucosa cytology, Nasal Mucosa pathology, Neurofilament Proteins analysis, Rhinitis drug therapy, Rhinitis pathology, Serine Endopeptidases analysis, Synaptophysin analysis, Time Factors, Treatment Outcome, Tryptases, Capsaicin therapeutic use, Nasal Mucosa drug effects

Abstract

Background: Capsaicin has been shown previously to reduce nasal complaints in patients with a non-allergic non-infectious perennial rhinitis. Proposed pathophysiological mechanisms for non-allergic non-infectious perennial rhinitis include a chronic inflammatory disorder of an antigenic or neurogenic nature as well as the possibility of a functional neuronal disorder. We hypothesized that the beneficial effect of capsaicin might be the result of a down-regulation of inflammation (by a reduction of inflammatory cells) or through modulation of neural tissue density., Methods: Patients were treated with either a placebo or capsaicin spray solution delivering 0.15 mg of capsaicin per nostril once every second or third day for a total of seven treatments. Both sides were treated each visit. Biopsies were taken before and 2 weeks, 3 months and 9 months after the treatment period. Immunohistochemical staining of the biopsy specimen was performed to ascertain the effect of treatment on immunocompetent cell densities (quantitative) and neural tissue densities (semi-quantitative) in the nasal mucosa., Results: Nasal complaints were significantly reduced in the capsaicin-treated group. The number of CD1+, CD25+, CD3+, CD68+, BMK13+, IgE+, tryptase+, and chymase+ cells did not significantly differ between capsaicin and placebo group. No significant differences between both groups were found in pan-neurogenic staining of nasal mucosa using neurofilament and synaptophysine., Conclusion: Capsaicin aqueous nasal spray has previously been shown to reduce nasal complaints without affecting cellular homeostasis or overall neurogenic staining up to 9 months after treatment. Immunocompetent cells are not involved in non-allergic non-infectious perennial rhinitis.

Published

1998