Your search keyword '"Linda Rousseau"' showing total 15 results

1. Loss of Tmem106b is unable to ameliorate frontotemporal dementia-like phenotypes in an AAV mouse model of C9ORF72-repeat induced toxicity

Author

Alexandra M. Nicholson, Xiaolai Zhou, Ralph B. Perkerson, Tammee M. Parsons, Jeannie Chew, Mieu Brooks, Mariely DeJesus-Hernandez, NiCole A. Finch, Billie J. Matchett, Aishe Kurti, Karen R. Jansen-West, Emilie Perkerson, Lillian Daughrity, Monica Castanedes-Casey, Linda Rousseau, Virginia Phillips, Fenghua Hu, Tania F. Gendron, Melissa E. Murray, Dennis W. Dickson, John D. Fryer, Leonard Petrucelli, and Rosa Rademakers

Subjects

Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Loss-of-function mutations in progranulin (GRN) and a non-coding (GGGGCC)n hexanucleotide repeat expansions in C9ORF72 are the two most common genetic causes of frontotemporal lobar degeneration with aggregates of TAR DNA binding protein 43 (FTLD-TDP). TMEM106B encodes a type II transmembrane protein with unknown function. Genetic variants in TMEM106B associated with reduced TMEM106B levels have been identified as disease modifiers in individuals with GRN mutations and C9ORF72 expansions. Recently, loss of Tmem106b has been reported to protect the FTLD-like phenotypes in Grn−/− mice. Here, we generated Tmem106b−/− mice and examined whether loss of Tmem106b could rescue FTLD-like phenotypes in an AAV mouse model of C9ORF72-repeat induced toxicity. Our results showed that neither partial nor complete loss of Tmem106b was able to rescue behavioral deficits induced by the expression of (GGGGCC)66 repeats (66R). Loss of Tmem106b also failed to ameliorate 66R-induced RNA foci, dipeptide repeat protein formation and pTDP-43 pathological burden. We further found that complete loss of Tmem106b increased astrogliosis, even in the absence of 66R, and failed to rescue 66R-induced neuronal cell loss, whereas partial loss of Tmem106b significantly rescued the neuronal cell loss but not neuroinflammation induced by 66R. Finally, we showed that overexpression of 66R did not alter expression of Tmem106b and other lysosomal genes in vivo, and subsequent analyses in vitro found that transiently knocking down C9ORF72, but not overexpression of 66R, significantly increased TMEM106B and other lysosomal proteins. In summary, reducing Tmem106b levels failed to rescue FTLD-like phenotypes in a mouse model mimicking the toxic gain-of-functions associated with overexpression of 66R. Combined with the observation that loss of C9ORF72 and not 66R overexpression was associated with increased levels of TMEM106B, this work suggests that the protective TMEM106B haplotype may exert its effect in expansion carriers by counteracting lysosomal dysfunction resulting from a loss of C9ORF72.

Published

2018

2. Neonatal AAV delivery of alpha-synuclein induces pathology in the adult mouse brain

Author

Marion Delenclos, Ayman H. Faroqi, Mei Yue, Aishe Kurti, Monica Castanedes-Casey, Linda Rousseau, Virginia Phillips, Dennis W. Dickson, John D. Fryer, and Pamela J. McLean

Subjects

Alpha-synuclein, Neonatal injection, Viral vector model, Aggregation, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Abnormal accumulation of alpha-synuclein (αsyn) is a pathological hallmark of Lewy body related disorders such as Parkinson’s disease and Dementia with Lewy body disease. During the past two decades, a myriad of animal models have been developed to mimic pathological features of synucleinopathies by over-expressing human αsyn. Although different strategies have been used, most models have little or no reliable and predictive phenotype. Novel animal models are a valuable tool for understanding neuronal pathology and to facilitate development of new therapeutics for these diseases. Here, we report the development and characterization of a novel model in which mice rapidly express wild-type αsyn via somatic brain transgenesis mediated by adeno-associated virus (AAV). At 1, 3, and 6 months of age following intracerebroventricular (ICV) injection, mice were subjected to a battery of behavioral tests followed by pathological analyses of the brains. Remarkably, significant levels of αsyn expression are detected throughout the brain as early as 1 month old, including olfactory bulb, hippocampus, thalamic regions and midbrain. Immunostaining with a phospho-αsyn (pS129) specific antibody reveals abundant pS129 expression in specific regions. Also, pathologic αsyn is detected using the disease specific antibody 5G4. However, this model did not recapitulate behavioral phenotypes characteristic of rodent models of synucleinopathies. In fact no deficits in motor function or cognition were observed at 3 or 6 months of age. Taken together, these findings show that transduction of neonatal mouse with AAV-αsyn can successfully lead to rapid, whole brain transduction of wild-type human αsyn, but increased levels of wildtype αsyn do not induce behavior changes at an early time point (6 months), despite pathological changes in several neurons populations as early as 1 month.

Published

2017

3. In-depth clinico-pathological examination of RNA foci in a large cohort of C9ORF72 expansion carriers

Author

Anthony Lucido, Linda Rousseau, Xue Wang, Mariely DeJesus-Hernandez, Jan de Boer, Ni Cole A. Finch, Ronald C. Petersen, Aliaksei Vasilevich, Tania F. Gendron, Keith A. Josephs, Neill R. Graff-Radford, Marka van Blitterswijk, Yan W. Asmann, Jeannie Chew, Kevin F. Bieniek, Joseph E. Parisi, Leonard Petrucelli, Kevin B. Boylan, Michael G. Heckman, Dennis W. Dickson, David S. Knopman, Rachael Weesner, Meeia Parsons, Melissa E. Murray, Rosa Rademakers, Bradley F. Boeve, RS: MERLN - Cell Biology - Inspired Tissue Engineering (CBITE), and CBITE

Subjects

0301 basic medicine, Male, Cerebellum, Pathology, Cell, TOXICITY, DIPEPTIDE-REPEAT PROTEINS, Cohort Studies, 0302 clinical medicine, C9orf72, Sense (molecular biology), ALS/FTD, Neurons, DNA Repeat Expansion, Neurodegeneration, Brain, Middle Aged, Antisense RNA, medicine.anatomical_structure, Female, NEURONAL LOSS, Frontotemporal dementia, medicine.medical_specialty, C9ORF72, Chromosome 9, Biology, Pathology and Forensic Medicine, 03 medical and health sciences, Cellular and Molecular Neuroscience, medicine, Humans, RNA, Antisense, RNA, Messenger, Motor neuron disease, BAC TRANSGENIC MICE, Aged, Original Paper, Analysis of Variance, Electronic Data Processing, FRONTOTEMPORAL LOBAR DEGENERATION, HEXANUCLEOTIDE REPEAT, C9orf72 Protein, ANTISENSE TRANSCRIPTS, RNA foci, RNA, medicine.disease, Amyotrophic lateral sclerosis, 030104 developmental biology, PATHOLOGICAL FEATURES, Neurology (clinical), Human medicine, ALS, 030217 neurology & neurosurgery

Abstract

A growing body of evidence suggests that a loss of chromosome 9 open reading frame 72 (C9ORF72) expression, formation of dipeptide-repeat proteins, and generation of RNA foci contribute to disease pathogenesis in amyotrophic lateral sclerosis and frontotemporal dementia. Although the levels of C9ORF72 transcripts and dipeptide-repeat proteins have already been examined thoroughly, much remains unknown about the role of RNA foci in C9ORF72-linked diseases. As such, we performed a comprehensive RNA foci study in an extensive pathological cohort of C9ORF72 expansion carriers (n = 63). We evaluated two brain regions using a newly developed computer-automated pipeline allowing recognition of cell nuclei and RNA foci (sense and antisense) supplemented by manual counting. In the frontal cortex, the percentage of cells with sense or antisense RNA foci was 26 or 12%, respectively. In the cerebellum, 23% of granule cells contained sense RNA foci and 1% antisense RNA foci. Interestingly, the highest percentage of cells with RNA foci was observed in cerebellar Purkinje cells (~70%). In general, more cells contained sense RNA foci than antisense RNA foci; however, when antisense RNA foci were present, they were usually more abundant. We also observed that an increase in the percentage of cells with antisense RNA foci was associated with a delayed age at onset in the frontal cortex (r = 0.43, p = 0.003), whereas no other associations with clinico-pathological features were seen. Importantly, our large-scale study is the first to provide conclusive evidence that RNA foci are not the determining factor of the clinico-pathological variability observed in C9ORF72 expansion carriers and it emphasizes that the distribution of RNA foci does not follow the pattern of neurodegeneration, stressing the complex interplay between different aspects of C9ORF72-related diseases. Electronic supplementary material The online version of this article (doi:10.1007/s00401-017-1725-7) contains supplementary material, which is available to authorized users.

Published

2017

4. Loss of Tmem106b is unable to ameliorate frontotemporal dementia-like phenotypes in an AAV mouse model of C9ORF72-repeat induced toxicity

Author

Linda Rousseau, Tania F. Gendron, Xiaolai Zhou, John D. Fryer, Jeannie Chew, Virginia Phillips, Billie J. Matchett, Tammee M. Parsons, Leonard Petrucelli, Monica Castanedes-Casey, Aishe Kurti, Melissa E. Murray, Karen Jansen-West, Rosa Rademakers, Ni Cole A. Finch, Fenghua Hu, Lillian M. Daughrity, Mieu Brooks, Alexandra M. Nicholson, Dennis W. Dickson, Ralph B. Perkerson, Emilie A. Perkerson, and Mariely DeJesus-Hernandez

Subjects

0301 basic medicine, Genetic Vectors, Biology, lcsh:RC346-429, Pathology and Forensic Medicine, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Transduction, Genetic, C9orf72, Conditioning, Psychological, medicine, Animals, Humans, Interpersonal Relations, RNA, Small Interfering, Gene, lcsh:Neurology. Diseases of the nervous system, Neuroinflammation, Cell Line, Transformed, Mice, Knockout, DNA Repeat Expansion, C9orf72 Protein, Research, Tumor Suppressor Proteins, Membrane Proteins, Fear, Frontotemporal lobar degeneration, medicine.disease, Phenotype, Transmembrane protein, 3. Good health, Astrogliosis, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Gene Expression Regulation, Glycerophosphates, Exploratory Behavior, Human medicine, Neurology (clinical), Frontotemporal Lobar Degeneration, 030217 neurology & neurosurgery, Frontotemporal dementia

Abstract

Loss-of-function mutations in progranulin (GRN) and a non-coding (GGGGCC)n hexanucleotide repeat expansions in C9ORF72 are the two most common genetic causes of frontotemporal lobar degeneration with aggregates of TAR DNA binding protein 43 (FTLD-TDP). TMEM106B encodes a type II transmembrane protein with unknown function. Genetic variants in TMEM106B associated with reduced TMEM106B levels have been identified as disease modifiers in individuals with GRN mutations and C9ORF72 expansions. Recently, loss of Tmem106b has been reported to protect the FTLD-like phenotypes in Grn−/− mice. Here, we generated Tmem106b−/− mice and examined whether loss of Tmem106b could rescue FTLD-like phenotypes in an AAV mouse model of C9ORF72-repeat induced toxicity. Our results showed that neither partial nor complete loss of Tmem106b was able to rescue behavioral deficits induced by the expression of (GGGGCC)66 repeats (66R). Loss of Tmem106b also failed to ameliorate 66R-induced RNA foci, dipeptide repeat protein formation and pTDP-43 pathological burden. We further found that complete loss of Tmem106b increased astrogliosis, even in the absence of 66R, and failed to rescue 66R-induced neuronal cell loss, whereas partial loss of Tmem106b significantly rescued the neuronal cell loss but not neuroinflammation induced by 66R. Finally, we showed that overexpression of 66R did not alter expression of Tmem106b and other lysosomal genes in vivo, and subsequent analyses in vitro found that transiently knocking down C9ORF72, but not overexpression of 66R, significantly increased TMEM106B and other lysosomal proteins. In summary, reducing Tmem106b levels failed to rescue FTLD-like phenotypes in a mouse model mimicking the toxic gain-of-functions associated with overexpression of 66R. Combined with the observation that loss of C9ORF72 and not 66R overexpression was associated with increased levels of TMEM106B, this work suggests that the protective TMEM106B haplotype may exert its effect in expansion carriers by counteracting lysosomal dysfunction resulting from a loss of C9ORF72. Electronic supplementary material The online version of this article (10.1186/s40478-018-0545-x) contains supplementary material, which is available to authorized users.

Published

2018

5. C9ORF72 repeat expansions in mice cause TDP-43 pathology, neuronal loss, and behavioral deficits

Author

Mercedes Prudencio, Aishe Kurti, Jeannette N. Stankowski, Dennis W. Dickson, Linda Rousseau, Emilie A. Perkerson, Yong Jie Zhang, Tania F. Gendron, Ena C. Whitelaw, Dieter Edbauer, Peter O. Bauer, Karen Overstreet, Lillian M. Daughrity, Leonard Petrucelli, Pamela Desaro, Karen Jansen-West, Kevin F. Bieniek, John D. Fryer, Melissa E. Murray, Amelia Johnston, Rosa Rademakers, Monica Castanedes-Casey, Chris W. Lee, Hiroki Sasaguri, Caroline Stetler, Jeannie Chew, and Kevin B. Boylan

Subjects

Pathology, medicine.medical_specialty, Multidisciplinary, Neurodegeneration, Cerebellar Purkinje cell, Biology, medicine.disease, Astrogliosis, C9orf72 Protein, C9orf72, medicine, Amyotrophic lateral sclerosis, Trinucleotide repeat expansion, Engineering sciences. Technology, Frontotemporal dementia

Abstract

The major genetic cause of frontotemporal dementia and amyotrophic lateral sclerosis is a G(4)C(2) repeat expansion in C9ORF72. Efforts to combat neurodegeneration associated with "c9FTD/ALS" are hindered by a lack of animal models recapitulating disease features. We developed a mouse model to mimic both neuropathological and clinical c9FTD/ALS phenotypes. We expressed (G(4)C(2))(66) throughout the murine central nervous system by means of somatic brain transgenesis mediated by adeno-associated virus. Brains of 6-month-old mice contained nuclear RNA foci, inclusions of poly(Gly-Pro), poly(Gly-Ala), and poly(Gly-Arg) dipeptide repeat proteins, as well as TDP-43 pathology. These mouse brains also exhibited cortical neuron and cerebellar Purkinje cell loss, astrogliosis, and decreased weight. (G(4)C(2))(66) mice also developed behavioral abnormalities similar to clinical symptoms of c9FTD/ALS patients, including hyperactivity, anxiety, antisocial behavior, and motor deficits.

Published

2015

6. Neonatal AAV delivery of alpha-synuclein induces pathology in the adult mouse brain

Author

Pamela J. McLean, Aishe Kurti, Marion Delenclos, Ayman H. Faroqi, Mei Yue, Linda Rousseau, Dennis W. Dickson, Monica Castanedes-Casey, John D. Fryer, and Virginia Phillips

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Genetic Vectors, Hippocampus, Motor Activity, Biology, lcsh:RC346-429, Pathology and Forensic Medicine, Alpha-synuclein, Neonatal injection, Aggregation, 03 medical and health sciences, Cellular and Molecular Neuroscience, chemistry.chemical_compound, 0302 clinical medicine, Memory, medicine, Animals, Humans, Learning, Dementia, Gliosis, lcsh:Neurology. Diseases of the nervous system, Synucleinopathies, Lewy body, Research, Brain, Neurodegenerative Diseases, Dependovirus, medicine.disease, 3. Good health, Olfactory bulb, Mice, Inbred C57BL, Disease Models, Animal, HEK293 Cells, 030104 developmental biology, Animals, Newborn, chemistry, Astrocytes, Microglia, Neurology (clinical), Viral vector model, medicine.symptom, Neuroscience, 030217 neurology & neurosurgery, Immunostaining

Abstract

Abnormal accumulation of alpha-synuclein (αsyn) is a pathological hallmark of Lewy body related disorders such as Parkinson’s disease and Dementia with Lewy body disease. During the past two decades, a myriad of animal models have been developed to mimic pathological features of synucleinopathies by over-expressing human αsyn. Although different strategies have been used, most models have little or no reliable and predictive phenotype. Novel animal models are a valuable tool for understanding neuronal pathology and to facilitate development of new therapeutics for these diseases. Here, we report the development and characterization of a novel model in which mice rapidly express wild-type αsyn via somatic brain transgenesis mediated by adeno-associated virus (AAV). At 1, 3, and 6 months of age following intracerebroventricular (ICV) injection, mice were subjected to a battery of behavioral tests followed by pathological analyses of the brains. Remarkably, significant levels of αsyn expression are detected throughout the brain as early as 1 month old, including olfactory bulb, hippocampus, thalamic regions and midbrain. Immunostaining with a phospho-αsyn (pS129) specific antibody reveals abundant pS129 expression in specific regions. Also, pathologic αsyn is detected using the disease specific antibody 5G4. However, this model did not recapitulate behavioral phenotypes characteristic of rodent models of synucleinopathies. In fact no deficits in motor function or cognition were observed at 3 or 6 months of age. Taken together, these findings show that transduction of neonatal mouse with AAV-αsyn can successfully lead to rapid, whole brain transduction of wild-type human αsyn, but increased levels of wildtype αsyn do not induce behavior changes at an early time point (6 months), despite pathological changes in several neurons populations as early as 1 month. Electronic supplementary material The online version of this article (doi:10.1186/s40478-017-0455-3) contains supplementary material, which is available to authorized users.

Published

2017

7. Poly(GP) proteins are a useful pharmacodynamic marker for C9ORF72-associated amyotrophic lateral sclerosis

Author

Timothy M. Miller, Jon B. Toledo, Jennifer Farren, Jeffrey D. Rothstein, John Q. Trojanowski, Luc Pregent, Michael G. Heckman, Alessandro Prelle, Aliesha D. O’Raw, Beth K. Rush, Bryan J. Traynor, Laura Braun, Matthew D. Disney, Yari Carlomagno, Veronique V. Belzil, Antonia Ratti, Lilia J. Tabassian, Monica Castanedes-Casey, Dennis W. Dickson, Michael Tierney, John C. van Swieten, Adam L. Boxer, Jeannie Chew, Lauren Elman, Murray Grossman, Emilie A. Perkerson, Mercedes Prudencio, Ana M. Caputo, Frank Rigo, Lillian M. Daughrity, Casey Cook, Otto Pedraza, James D. Berry, David Lacomis, Christina Fournier, Jennifer Jockel-Balsarotti, Leonard Petrucelli, Giovanna Antognetti, Marka van Blitterswijk, Lindsey R. Hayes, Robert H. Brown, Joanne Wuu, Kevin B. Boylan, Jimei Tong, Edythe Wiggs, Amelia Robertson, Linda Rousseau, Karen Jansen-West, Mary Kay Floeter, Yuping Song, John D. Fryer, Tania D Gendron, Robert Bowser, Barbara Poletti, Jennifer D. McBride, Shafeeq Ladha, Federica Solca, Alexander McCampbell, Leo McCluskey, Bruce L. Miller, Weixing Yang, Rosa Rademakers, Virginia Phillips, Chris W. Lee, Mei Yue, Denitza Raitcheva, Carla Palmucci, Jonathan D. Glass, Nancy N. Diehl, Vincenzo Silani, Jeannette N. Stankowski, Pamela Desaro, Cinzia Tiloca, Claudia Morelli, Abhishek Datta, William T. Hu, Yong Jie Zhang, Michael Benatar, Christine Ambrose, and Neurology

Subjects

0301 basic medicine, Oligonucleotides, Neurodegenerative, medicine.disease_cause, Medical and Health Sciences, Mice, 0302 clinical medicine, C9orf72, Leukocytes, Longitudinal Studies, Amyotrophic lateral sclerosis, Dinucleotide Repeats, Neurons, Mutation, Brain, General Medicine, Middle Aged, Biological Sciences, Prognosis, Editorial, Neurological, Adult, Mononuclear, Induced Pluripotent Stem Cells, Clinical Trials and Supportive Activities, Peripheral blood mononuclear cell, Article, Cell Line, 03 medical and health sciences, Rare Diseases, Clinical Research, medicine, Extracellular, Acquired Cognitive Impairment, Genetics, Animals, Humans, Antisense, Biology, Aged, C9orf72 Protein, Oligonucleotide, business.industry, Amyotrophic Lateral Sclerosis, Neurosciences, RNA, Oligonucleotides, Antisense, medicine.disease, Molecular biology, Brain Disorders, 030104 developmental biology, Cancer research, Leukocytes, Mononuclear, Dementia, Human medicine, ALS, Trinucleotide repeat expansion, business, 030217 neurology & neurosurgery, Biomarkers

Abstract

There is no effective treatment for amyotrophic lateral sclerosis (ALS), a devastating motor neuron disease. However, discovery of a G(4)C(2) repeat expansion in the C9ORF72 gene as the most common genetic cause of ALS has opened up new avenues for therapeutic intervention for this form of ALS. G(4)C(2) repeat expansion RNAs and proteins of repeating dipeptides synthesized from these transcripts are believed to play a key role in C9ORF72-associated ALS (c9ALS). Therapeutics that target G(4)C(2) RNA, such as antisense oligonucleotides (ASOs) and small molecules, are thus being actively investigated. A limitation in moving such treatments from bench to bedside is a lack of pharmacodynamic markers for use in clinical trials. We explored whether poly(GP) proteins translated from G(4)C(2) RNA could serve such a purpose. Poly(GP) proteins were detected in cerebrospinal fluid (CSF) and in peripheral blood mononuclear cells from c9ALS patients and, notably, from asymptomatic C9ORF72 mutation carriers. Moreover, CSF poly(GP) proteins remained relatively constant over time, boding well for their use in gauging biochemical responses to potential treatments. Treating c9ALS patient cells or a mouse model of c9ALS with ASOs that target G(4)C(2) RNA resulted in decreased intracellular and extracellular poly(GP) proteins. This decrease paralleled reductions in G(4)C(2) RNA and downstream G(4)C(2) RNA-mediated events. These findings indicate that tracking poly(GP) proteins in CSF could provide a means to assess target engagement of G(4)C(2) RNA-based therapies in symptomatic C9ORF72 repeat expansion carriers and presymptomatic individuals who are expected to benefit from early therapeutic intervention.

Published

2017

8. Severe amygdala dysfunction in a MAPT transgenic mouse model of frontotemporal dementia

Author

Linda Rousseau, Leonard Petrucelli, Monica Castanedes-Casey, Nawsheen Shukoor, Dennis W. Dickson, John D. Fryer, Kristyn Scheffel, Casey Cook, Michael S. Penuliar, Judy Dunmore, Jimei Tong, Virginia Phillips, Melissa E. Murray, and Aishe Kurti

Subjects

Genetically modified mouse, Aging, Elevated plus maze, Mice, Transgenic, tau Proteins, Severity of Illness Index, Amygdala, Article, Mice, Memory, Conditioning, Psychological, medicine, Animals, Humans, Learning, Fear conditioning, Language, Behavior, Animal, General Neuroscience, Parkinsonism, Neurodegeneration, Fear, medicine.disease, Disease Models, Animal, medicine.anatomical_structure, Frontotemporal Dementia, Mutation, Nerve Degeneration, Exploratory Behavior, Neurology (clinical), Tauopathy, Geriatrics and Gerontology, Psychology, Neuroscience, Developmental Biology, Frontotemporal dementia

Abstract

Frontotemporal dementia with Parkinsonism-linked to chromosome 17 (FTDP-17) is a neurodegenerative tauopathy caused by mutations in the tau gene (MAPT). Individuals with FTDP-17 have deficits in learning, memory and language, in addition to personality and behavioral changes that are often characterized by a lack of social inhibition. Several transgenic mouse models expressing tau mutations have been tested extensively for memory or motor impairments, though reports of amygdala-dependent behaviors are lacking. To this end, we tested the rTg4510 mouse model on a behavioral battery that included amygdala-dependent tasks of exploration. As expected, rTg4510 mice exhibit profound impairments in hippocampal-dependent learning and memory tests, including contextual fear conditioning. However, rTg4510 mice also display an abnormal hyper-exploratory phenotype in the open field assay, elevated plus maze, light-dark exploration, and cued fear conditioning, indicative of amygdala dysfunction. Furthermore, significant tau burden is detected in the amygdala of both rTg4510 mice and human FTDP-17 patients, suggesting that the rTg4510 mouse model recapitulates the behavioral disturbances and neurodegeneration of the amygdala characteristic of FTDP-17.

Published

2014

9. Neuronal sensitivity to TDP-43 overexpression is dependent on timing of induction

Author

Xin Yu, Baoli Yang, Simon D'Alton, Joshua Knight, Ian M. Farnham, Rachel M. Bailey, Yong Jie Zhang, John Howard, Monica Castanedes-Casey, Matthew R. Sarkisian, Brittany Scott, Jada Lewis, Linda Rousseau, Ashley Cannon, Dennis W. Dickson, Wen-Lang Lin, Leonard Petrucelli, Michael Jurasic, and Charles A. Wuertzer

Subjects

Genetically modified mouse, Pathology, medicine.medical_specialty, Mice, 129 Strain, Time Factors, TDP-43, Transgene, Neurodevelopment, Clinical Neurology, Apoptosis, Mice, Transgenic, Biology, Mitochondrion, Frontotemporal lobar degeneration, Pathology and Forensic Medicine, 03 medical and health sciences, Cellular and Molecular Neuroscience, Mice, 0302 clinical medicine, Ubiquitin, mental disorders, medicine, Transgenic mice, Animals, Humans, 030304 developmental biology, Neurons, 0303 health sciences, Original Paper, Neurodegeneration, nutritional and metabolic diseases, medicine.disease, Amyotrophic lateral sclerosis, Cell biology, nervous system diseases, Mitochondria, DNA-Binding Proteins, Disease Models, Animal, Gene Expression Regulation, TDP-43 Proteinopathies, Knockout mouse, Forebrain, biology.protein, Neurology (clinical), 030217 neurology & neurosurgery

Abstract

Ubiquitin-immunoreactive neuronal inclusions composed of TAR DNA binding protein of 43 kDa (TDP-43) are a major pathological feature of frontotemporal lobar degeneration (FTLD-TDP). In vivo studies with TDP-43 knockout mice have suggested that TDP-43 plays a critical, although undefined role in development. In the current report, we generated transgenic mice that conditionally express wild-type human TDP-43 (hTDP-43) in the forebrain and established a paradigm to examine the sensitivity of neurons to TDP-43 overexpression at different developmental stages. Continuous TDP-43 expression during early neuronal development produced a complex phenotype, including aggregation of phospho-TDP-43, increased ubiquitin immunoreactivity, mitochondrial abnormalities, neurodegeneration and early lethality. In contrast, later induction of hTDP-43 in the forebrain of weaned mice prevented early death and mitochondrial abnormalities while yielding salient features of FTLD-TDP, including progressive neurodegeneration and ubiquitinated, phospho-TDP-43 neuronal cytoplasmic inclusions. These results suggest that neurons in the developing forebrain are extremely sensitive to TDP-43 overexpression and that timing of TDP-43 overexpression in transgenic mice must be considered when distinguishing normal roles of TDP-43, particularly as they relate to development, from its pathogenic role in FTLD-TDP and other TDP-43 proteinopathies. Finally, our adult induction of hTDP-43 strategy provides a mouse model that develops critical pathological features that are directly relevant for human TDP-43 proteinopathies. Electronic supplementary material The online version of this article (doi:10.1007/s00401-012-0979-3) contains supplementary material, which is available to authorized users.

Published

2012

10. Tau deposition drives neuropathological, inflammatory and behavioral abnormalities independently of neuronal loss in a novel mouse model

Author

Casey Cook, Mitsuru Shinohara, Leonard Petrucelli, Wen Lang Lin, Guojun Bu, Mei Yue, Dennis W. Dickson, Yari Carlomagno, Silvia S. Kang, Linda Rousseau, Emilie A. Perkerson, Monica Castanedes-Casey, Virginia Phillips, Karen Jansen-West, Aishe Kurti, and John D. Fryer

Subjects

Transgene, Tau protein, Mice, Transgenic, tau Proteins, Biology, Silver stain, Mice, Genetics, medicine, Animals, Humans, Molecular Biology, Genetics (clinical), Neuroinflammation, Ultrasonography, Neurons, Behavior, Animal, Cell Death, Brain, Neurofibrillary tangle, Neurofibrillary Tangles, General Medicine, Articles, medicine.disease, Phenotype, Disease Models, Animal, Gliosis, Tauopathies, biology.protein, Tauopathy, medicine.symptom, Neuroscience

Abstract

Aberrant tau protein accumulation drives neurofibrillary tangle (NFT) formation in several neurodegenerative diseases. Currently, efforts to elucidate pathogenic mechanisms and assess the efficacy of therapeutic targets are limited by constraints of existing models of tauopathy. In order to generate a more versatile mouse model of tauopathy, somatic brain transgenesis was utilized to deliver adeno-associated virus serotype 1 (AAV1) encoding human mutant P301L-tau compared with GFP control. At 6 months of age, we observed widespread human tau expression with concomitant accumulation of hyperphosphorylated and abnormally folded proteinase K resistant tau. However, no overt neuronal loss was observed, though significant abnormalities were noted in the postsynaptic scaffolding protein PSD95. Neurofibrillary pathology was also detected with Gallyas silver stain and Thioflavin-S, and electron microscopy revealed the deposition of closely packed filaments. In addition to classic markers of tauopathy, significant neuroinflammation and extensive gliosis were detected in AAV1-Tau(P301L) mice. This model also recapitulates the behavioral phenotype characteristic of mouse models of tauopathy, including abnormalities in exploration, anxiety, and learning and memory. These findings indicate that biochemical and neuropathological hallmarks of tauopathies are accurately conserved and are independent of cell death in this novel AAV-based model of tauopathy, which offers exceptional versatility and speed in comparison with existing transgenic models. Therefore, we anticipate this approach will facilitate the identification and validation of genetic modifiers of disease, as well as accelerate preclinical assessment of potential therapeutic targets.

Published

2015

11. Neurodegeneration. C9ORF72 repeat expansions in mice cause TDP-43 pathology, neuronal loss, and behavioral deficits

Author

Jeannie, Chew, Tania F, Gendron, Mercedes, Prudencio, Hiroki, Sasaguri, Yong-Jie, Zhang, Monica, Castanedes-Casey, Chris W, Lee, Karen, Jansen-West, Aishe, Kurti, Melissa E, Murray, Kevin F, Bieniek, Peter O, Bauer, Ena C, Whitelaw, Linda, Rousseau, Jeannette N, Stankowski, Caroline, Stetler, Lillian M, Daughrity, Emilie A, Perkerson, Pamela, Desaro, Amelia, Johnston, Karen, Overstreet, Dieter, Edbauer, Rosa, Rademakers, Kevin B, Boylan, Dennis W, Dickson, John D, Fryer, and Leonard, Petrucelli

Subjects

N-glycylalanine, genetics [DNA-Binding Proteins], metabolism [Purkinje Cells], Purkinje Cells, Mice, genetics [Antisocial Personality Disorder], Animals, Humans, pathology [Amyotrophic Lateral Sclerosis], genetics [Frontotemporal Dementia], RNA, Nuclear, Cerebral Cortex, C9orf72 Protein, metabolism [Cerebral Cortex], Amyotrophic Lateral Sclerosis, pathology [Antisocial Personality Disorder], metabolism [Dipeptides], Gene Transfer Techniques, Proteins, Antisocial Personality Disorder, Dipeptides, Dependovirus, genetics [Proteins], pathology [Purkinje Cells], DNA-Binding Proteins, genetics [Amyotrophic Lateral Sclerosis], Disease Models, Animal, HEK293 Cells, metabolism [RNA, Nuclear], Frontotemporal Dementia, ddc:320, pathology [Frontotemporal Dementia], pathology [Cerebral Cortex], glycylproline, C9orf72 protein, human

Abstract

The major genetic cause of frontotemporal dementia and amyotrophic lateral sclerosis is a G4C2 repeat expansion in C9ORF72. Efforts to combat neurodegeneration associated with "c9FTD/ALS" are hindered by a lack of animal models recapitulating disease features. We developed a mouse model to mimic both neuropathological and clinical c9FTD/ALS phenotypes. We expressed (G4C2)66 throughout the murine central nervous system by means of somatic brain transgenesis mediated by adeno-associated virus. Brains of 6-month-old mice contained nuclear RNA foci, inclusions of poly(Gly-Pro), poly(Gly-Ala), and poly(Gly-Arg) dipeptide repeat proteins, as well as TDP-43 pathology. These mouse brains also exhibited cortical neuron and cerebellar Purkinje cell loss, astrogliosis, and decreased weight. (G4C2)66 mice also developed behavioral abnormalities similar to clinical symptoms of c9FTD/ALS patients, including hyperactivity, anxiety, antisocial behavior, and motor deficits.

Published

2015

12. Cerebellar c9RAN proteins associate with clinical and neuropathological characteristics of C9ORF72 repeat expansion carriers

Author

John A. Lucas, Keith A. Josephs, Clotilde Lagier-Tourenne, Jie Jiang, Tania F. Gendron, Amelia Robertson, Neill R. Graff-Radford, Monica Castanedes-Casey, Colleen S. Thomas, Marka van Blitterswijk, Beth K. Rush, Pamela Desaro, Joseph E. Parisi, Kevin B. Boylan, Julia E. Crook, David S. Knopman, Karen Overstreet, Dennis W. Dickson, Linda Rousseau, Ronald C. Petersen, Lillian M. Daughrity, Kevin F. Bieniek, Melissa E. Murray, Don W. Cleveland, Leonard Petrucelli, Rosa Rademakers, Bradley F. Boeve, Otto Pedraza, and Dieter Edbauer

Subjects

Male, Pathology, Cerebellum, complications [Motor Neuron Disease], Messenger, Hippocampus, Dipeptide repeat proteins, metabolism [Hippocampus], genetics [Cognition Disorders], pathology [Frontal Lobe], Cohort Studies, Cognition, C9orf72, complications [Frontotemporal Dementia], 80 and over, pathology [Cerebellum], Amyotrophic lateral sclerosis, genetics [Frontotemporal Dementia], Aged, 80 and over, DNA Repeat Expansion, pathology [Motor Cortex], Motor Cortex, Frontotemporal lobar degeneration, metabolism [Cerebellum], Middle Aged, 3. Good health, Frontal Lobe, metabolism [Motor Neuron Disease], genetics [Amyotrophic Lateral Sclerosis], metabolism [Frontal Lobe], medicine.anatomical_structure, Frontotemporal Dementia, metabolism [Frontotemporal Dementia], complications [Amyotrophic Lateral Sclerosis], Female, genetics [Motor Neuron Disease], Frontotemporal dementia, metabolism [Motor Cortex], medicine.medical_specialty, complications [Cognition Disorders], Heterozygote, pathology [Motor Neuron Disease], Neuropathological diagnosis, Clinical Sciences, Clinical Neurology, Chromosome 9, and over, metabolism [RNA, Messenger], Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, metabolism [Cognition Disorders], medicine, Humans, ddc:610, RNA, Messenger, Motor Neuron Disease, pathology [Amyotrophic Lateral Sclerosis], Aged, c9RAN proteins, Original Paper, Neurology & Neurosurgery, C9orf72 Protein, business.industry, C9ORF72 repeat expansion, metabolism [Amyotrophic Lateral Sclerosis], Amyotrophic Lateral Sclerosis, Neurosciences, Proteins, Repeat-associated non-ATG translation, medicine.disease, genetics [Proteins], pathology [Hippocampus], Protein Biosynthesis, pathology [Frontotemporal Dementia], RNA, pathology [Cognition Disorders], Neurology (clinical), Human medicine, C9orf72 protein, human, Trinucleotide repeat expansion, business, Cognition Disorders

Abstract

Clinical and neuropathological characteristics associated with G4C2 repeat expansions in chromosome 9 open reading frame 72 (C9ORF72), the most common genetic cause of amyotrophic lateral sclerosis (ALS) and frontotemporal dementia, are highly variable. To gain insight on the molecular basis for the heterogeneity among C9ORF72 mutation carriers, we evaluated associations between features of disease and levels of two abundantly expressed “c9RAN proteins” produced by repeat-associated non-ATG (RAN) translation of the expanded repeat. For these studies, we took a departure from traditional immunohistochemical approaches and instead employed immunoassays to quantitatively measure poly(GP) and poly(GA) levels in cerebellum, frontal cortex, motor cortex, and/or hippocampus from 55 C9ORF72 mutation carriers [12 patients with ALS, 24 with frontotemporal lobar degeneration (FTLD) and 19 with FTLD with motor neuron disease (FTLD-MND)]. We additionally investigated associations between levels of poly(GP) or poly(GA) and cognitive impairment in 15 C9ORF72 ALS patients for whom neuropsychological data were available. Among the neuroanatomical regions investigated, poly(GP) levels were highest in the cerebellum. In this same region, associations between poly(GP) and both neuropathological and clinical features were detected. Specifically, cerebellar poly(GP) levels were significantly lower in patients with ALS compared to patients with FTLD or FTLD-MND. Furthermore, cerebellar poly(GP) associated with cognitive score in our cohort of 15 patients. In the cerebellum, poly(GA) levels similarly trended lower in the ALS subgroup compared to FTLD or FTLD-MND subgroups, but no association between cerebellar poly(GA) and cognitive score was detected. Both cerebellar poly(GP) and poly(GA) associated with C9ORF72 variant 3 mRNA expression, but not variant 1 expression, repeat size, disease onset, or survival after onset. Overall, these data indicate that cerebellar abnormalities, as evidenced by poly(GP) accumulation, associate with neuropathological and clinical phenotypes, in particular cognitive impairment, of C9ORF72 mutation carriers. Electronic supplementary material The online version of this article (doi:10.1007/s00401-015-1474-4) contains supplementary material, which is available to authorized users.

Published

2015

13. LRRK2 phosphorylates novel tau epitopes and promotes tauopathy

Author

Ruth E. Watkinson, Sarah Miles, Linda Rousseau, Rachel M. Bailey, Benoit I. Giasson, Matthew J. Farrer, Jason P. Covy, Joshua Knight, Heather L. Melrose, Jada Lewis, and Dennis W. Dickson

Subjects

Male, Transgene, Clinical Neurology, Mice, Transgenic, tau Proteins, Biology, Protein Serine-Threonine Kinases, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2, Epitope, Pathology and Forensic Medicine, 03 medical and health sciences, Cellular and Molecular Neuroscience, Epitopes, Mice, 0302 clinical medicine, medicine, Animals, Humans, Phosphorylation, 030304 developmental biology, Aged, Aged, 80 and over, 0303 health sciences, Original Paper, Kinase, HEK 293 cells, Brain, Middle Aged, medicine.disease, Molecular biology, LRRK2, In vitro, 3. Good health, nervous system diseases, HEK293 Cells, Tauopathies, Female, Neurology (clinical), Tauopathy, 030217 neurology & neurosurgery

Abstract

Mutations in the gene encoding leucine-rich repeat kinase 2 (LRRK2) are the most frequent cause of familial Parkinson’s disease (PD). The neuropathology of LRRK2-related PD is heterogeneous and can include aberrant tau phosphorylation or neurofibrillary tau pathology. Recently, LRRK2 has been shown to phosphorylate tau in vitro; however, the major epitopes phosphorylated by LRRK2 and the physiological or pathogenic consequences of these modifications in vivo are unknown. Using mass spectrometry, we identified multiple sites on recombinant tau that are phosphorylated by LRRK2 in vitro, including pT149 and pT153, which are phospho-epitopes that to date have been largely unexplored. Importantly, we demonstrate that expression of transgenic LRRK2 in a mouse model of tauopathy increased the aggregation of insoluble tau and its phosphorylation at T149, T153, T205, and S199/S202/T205 epitopes. These findings indicate that tau can be a LRRK2 substrate and that this interaction can enhance salient features of human disease. Electronic supplementary material The online version of this article (doi:10.1007/s00401-013-1188-4) contains supplementary material, which is available to authorized users.

Published

2013

14. TMEM106B p.T185S regulates TMEM106B protein levels: implications for frontotemporal dementia

Author

Roberta Ghidoni, Luisa Benussi, Nilufer Ertekin-Taner, Dennis W. Dickson, Giuliano Binetti, Elizabeth Finger, Ralph B. Perkerson, Matt Baker, Aleksandra Wojtas, Ian R. A. Mackenzie, Linda Rousseau, Nicole A. Finch, Alexandra M. Nicholson, Rosa Rademakers, Bradley F. Boeve, Monica Castanedes-Casey, Neill R. Graff-Radford, and Ging-Yuek Robin Hsiung

Subjects

Gene isoform, Linkage disequilibrium, TAR DNA-Binding Protein 43, Biology, medicine.disease_cause, Biochemistry, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, mental disorders, medicine, Gene, 030304 developmental biology, Genetics, 0303 health sciences, Mutation, nutritional and metabolic diseases, Frontotemporal lobar degeneration, medicine.disease, Molecular biology, Transmembrane protein, 3. Good health, nervous system diseases, Chemistry, Human medicine, 030217 neurology & neurosurgery, Frontotemporal dementia

Abstract

Frontotemporal lobar degeneration (FTLD) is the second leading cause of dementia in individuals under age 65. In many patients, the predominant pathology includes neuronal cytoplasmic or intranuclear inclusions of ubiquitinated TAR DNA binding protein 43 (FTLD-TDP). Recently, a genome-wide association study identified the first FTLD-TDP genetic risk factor, in which variants in and around the TMEM106B gene (top SNP rs1990622) were significantly associated with FTLD-TDP risk. Intriguingly, the most significant association was in FTLD-TDP patients carrying progranulin (GRN) mutations. Here, we investigated to what extent the coding variant, rs3173615 (p.T185S) in linkage disequilibrium with rs1990622, affects progranulin protein (PGRN) biology and transmembrane protein 106 B (TMEM106B) regulation. First, we confirmed the association of TMEM106B variants with FTLD-TDP in a new cohort of GRN mutation carriers. We next generated and characterized a TMEM106B-specific antibody for investigation of this protein. Enzyme-linked immunoassay analysis of progranulin protein levels showed similar effects upon T185 and S185 TMEM106B over-expression. However, over-expression of T185 consistently led to higher TMEM106B protein levels than S185. Cycloheximide treatment experiments revealed that S185 degrades faster than T185 TMEM106B, potentially due to differences in N-glycosylation at residue N183. Together, our results provide a potential mechanism by which TMEM106B variants lead to differences in FTLD-TDP risk. We studied the p.T185S TMEM106B genetic variant previously implicated in frontotemporal dementia with TAR DNA binding protein 43 pathology caused by progranulin mutations. Our cell culture studies provide evidence that the protective S185 isoform is degraded more rapidly than T185 TMEM106B, potentially due to differences in glycosylation. These findings suggest that low TMEM106B levels might protect against FTLD-TDP in these patients.

Published

2013

15. Age- and disease-dependent increase of the mitophagy marker phospho-ubiquitin in normal aging and Lewy body disease

Author

Alexandra I. Soto, Linda Rousseau, John C. Steele, Ignacio F. Mata, Xu Hou, Zbigniew K. Wszolek, Dominika Truban, Michael G. Heckman, Nancy N. Diehl, Wolfdieter Springer, Neill R. Graff-Radford, Luis Torres, Pawel Tacik, Mario Cornejo-Olivas, José Matías Arbelo, Isidre Ferrer, Dennis W. Dickson, Monica Castanedes Casey, Matthew J. Farrer, Fabienne C. Fiesel, Melissa E. Murray, Wen Lang Lin, Oswaldo Lorenzo-Betancor, Owen A. Ross, and Universitat de Barcelona

Subjects

Male, 0301 basic medicine, Aging, alpha-synuclein, Parkinson's disease, Disease, Mitochondrion, Parkin, Mitocondris, Cohort Studies, Phosphoserine, chemistry.chemical_compound, 0302 clinical medicine, Ubiquitin, Malaltia de Parkinson, Mitophagy, MAPT, parkin, tau, Phosphorylation, Aged, 80 and over, biology, Brain, Middle Aged, Mitochondria, mitochondria, Female, Protein Binding, Lewy Body Disease, autophagy, tau Proteins, PINK1, 03 medical and health sciences, Autofàgia, parkinson disease, Envelliment, ubiquitin, Autophagy, Humans, Molecular Biology, Aged, phospho-ubiquitin, Alpha-synuclein, Cell Biology, PARK2, 030104 developmental biology, chemistry, Mutation, biology.protein, SNCA, Research Paper - Translational, Ubiqüitina, Neuroscience, Biomarkers, 030217 neurology & neurosurgery, HeLa Cells

Abstract

Although exact causes of Parkinson disease (PD) remain enigmatic, mitochondrial dysfunction is increasingly appreciated as a key determinant of dopaminergic neuron susceptibility in both familial and sporadic PD. Two genes associated with recessive, early-onset PD encode the ubiquitin (Ub) kinase PINK1 and the E3 Ub ligase PRKN/PARK2/Parkin, which together orchestrate a protective mitochondrial quality control (mitoQC) pathway. Upon stress, both enzymes cooperatively identify and decorate damaged mitochondria with phosphorylated poly-Ub (p-S65-Ub) chains. This specific label is subsequently recognized by autophagy receptors that further facilitate mitochondrial degradation in lysosomes (mitophagy). Here, we analyzed human post-mortem brain specimens and identified distinct pools of p-S65-Ub-positive structures that partially colocalized with markers of mitochondria, autophagy, lysosomes and/or granulovacuolar degeneration bodies. We further quantified levels and distribution of the ‘mitophagy tag’ in 2 large cohorts of brain samples from normal aging and Lewy body disease (LBD) cases using unbiased digital pathology. Somatic p-S65-Ub structures independently increased with age and disease in distinct brain regions and enhanced levels in LBD brain were age- and Braak tangle stage-dependent. Additionally, we observed significant correlations of p-S65-Ub with LBs and neurofibrillary tangle levels in disease. The degree of co-existing p-S65-Ub signals and pathological PD hallmarks increased in the pre-mature stage, but decreased in the late stage of LB or tangle aggregation. Altogether, our study provides further evidence for a potential pathogenic overlap among different forms of PD and suggests that p-S65-Ub can serve as a biomarker for mitochondrial damage in aging and disease. Abbreviations: BLBD: brainstem predominant Lewy body disease; CCCP: carbonyl cyanide m-chlorophenyl hydrazone; DLB: dementia with Lewy bodies; DLBD: diffuse neocortical Lewy body disease; EOPD: early-onset Parkinson disease; GVB: granulovacuolar degeneration body; LB: Lewy body; LBD: Lewy body disease; mitoQC: mitochondrial quality control; nbM: nucleus basalis of Meynert; PD: Parkinson disease; PDD: Parkinson disease with dementia; p-S65-Ub: PINK1-phosphorylated serine 65 ubiquitin; SN: substantia nigra; TLBD: transitional Lewy body disease; Ub: ubiquitin