Your search keyword '"Matthew C. Judson"' showing total 24 results

1. Molecular and behavioral consequences of Ube3a gene overdosage in mice

Author

A. Mattijs Punt, Matthew C. Judson, Michael S. Sidorov, Brittany N. Williams, Naomi S. Johnson, Sabine Belder, Dion den Hertog, Courtney R. Davis, Maximillian S. Feygin, Patrick F. Lang, Mehrnoush Aghadavoud Jolfaei, Patrick J. Curran, Wilfred F.J. van IJcken, Ype Elgersma, and Benjamin D. Philpot

Subjects

Neuroscience, Medicine

Abstract

Chromosome 15q11.2–q13.1 duplication syndrome (Dup15q syndrome) is a severe neurodevelopmental disorder characterized by intellectual disability, impaired motor coordination, and autism spectrum disorder. Chromosomal multiplication of the UBE3A gene is presumed to be the primary driver of Dup15q pathophysiology, given that UBE3A exhibits maternal monoallelic expression in neurons and that maternal duplications typically yield far more severe neurodevelopmental outcomes than paternal duplications. However, studies into the pathogenic effects of UBE3A overexpression in mice have yielded conflicting results. Here, we investigated the neurodevelopmental impact of Ube3a gene overdosage using bacterial artificial chromosome–based transgenic mouse models (Ube3aOE) that recapitulate the increases in Ube3a copy number most often observed in Dup15q. In contrast to previously published Ube3a overexpression models, Ube3aOE mice were indistinguishable from wild-type controls on a number of molecular and behavioral measures, despite suffering increased mortality when challenged with seizures, a phenotype reminiscent of sudden unexpected death in epilepsy. Collectively, our data support a model wherein pathogenic synergy between UBE3A and other overexpressed 15q11.2–q13.1 genes is required for full penetrance of Dup15q syndrome phenotypes.

Published

2022

2. Dual-isoform hUBE3A gene transfer improves behavioral and seizure outcomes in Angelman syndrome model mice

Author

Matthew C. Judson, Charles Shyng, Jeremy M. Simon, Courtney R. Davis, A. Mattijs Punt, Mirabel T. Salmon, Noah W. Miller, Kimberly D. Ritola, Ype Elgersma, David G. Amaral, Steven J. Gray, and Benjamin D. Philpot

Subjects

Neuroscience, Therapeutics, Medicine

Abstract

Loss of the maternal UBE3A allele causes Angelman syndrome (AS), a debilitating neurodevelopmental disorder. Here, we devised an AS treatment strategy based on reinstating dual-isoform expression of human UBE3A (hUBE3A) in the developing brain. Kozak sequence engineering of our codon-optimized vector (hUBE3Aopt) enabled translation of both short and long hUBE3A protein isoforms at a near-endogenous 3:1 (short/long) ratio, a feature that could help to support optimal therapeutic outcomes. To model widespread brain delivery and early postnatal onset of hUBE3A expression, we packaged the hUBE3Aopt vector into PHP.B capsids and performed intracerebroventricular injections in neonates. This treatment significantly improved motor learning and innate behaviors in AS mice, and it rendered them resilient to epileptogenesis and associated hippocampal neuropathologies induced by seizure kindling. hUBE3A overexpression occurred frequently in the hippocampus but was uncommon in the neocortex and other major brain structures; furthermore, it did not correlate with behavioral performance. Our results demonstrate the feasibility, tolerability, and therapeutic potential for dual-isoform hUBE3A gene transfer in the treatment of AS.

Published

2021

3. Delayed loss of UBE3A reduces the expression of Angelman syndrome-associated phenotypes

Author

Monica Sonzogni, Johanna Hakonen, Mireia Bernabé Kleijn, Sara Silva-Santos, Matthew C. Judson, Benjamin D. Philpot, Geeske M. van Woerden, and Ype Elgersma

Subjects

Ube3a, Angelman syndrome, Mouse model, Seizure, Autism spectrum disorder, Phenotype, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Angelman syndrome (AS) is a severe neurodevelopmental disorder caused by mutations affecting UBE3A gene expression. Previous studies in mice revealed distinct critical periods during neurodevelopment in which reactivation of Ube3a gene expression can prevent the onset of behavioral deficits. Whether UBE3A is required for brain function throughout life is unknown. Here, we address the importance of maintaining UBE3A expression after normal brain development. Findings Using a conditional mouse, we deleted the Ube3a gene at three ages spanning brain maturation. We assessed the consequences of Ube3a gene deletion by testing the mice in behavioral tasks previously shown to produce robust phenotypes in AS model mice. Early embryonic deletion of Ube3a recapitulated all behavioral deficits of AS mice. In contrast, Ube3a gene deletion at 3 or 12 weeks of age did not have a significant effect on most behavioral tasks and did not increase seizure sensitivity. Conclusions Taken together, these results emphasize that UBE3A critically impacts early brain development, but plays a more limited role in adulthood. Our findings provide important considerations for upcoming clinical trials in which UBE3A gene expression is reactivated and suggest that even transient UBE3A reinstatement during a critical window of early development is likely to prevent most adverse Angelman syndrome phenotypes. However, sustained UBE3A expression into adulthood is probably needed for optimal clinical benefit.

Published

2019

4. Subcellular organization of UBE3A in human cerebral cortex

Author

Alain C. Burette, Matthew C. Judson, Alissa N. Li, Edward F. Chang, William W. Seeley, Benjamin D. Philpot, and Richard J. Weinberg

Subjects

Angelman syndrome, E6-AP, Axon terminal, Mitochondria, Euchromatin, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Loss of UBE3A causes Angelman syndrome, whereas excess UBE3A activity appears to increase the risk for autism. Despite this powerful association with neurodevelopmental disorders, there is still much to be learned about UBE3A, including its cellular and subcellular organization in the human brain. The issue is important, since UBE3A’s localization is integral to its function. Methods We used light and electron microscopic immunohistochemistry to study the cellular and subcellular distribution of UBE3A in the adult human cerebral cortex. Experiments were performed on multiple tissue sources, but our results focused on optimally preserved material, using surgically resected human temporal cortex of high ultrastructural quality from nine individuals. Results We demonstrate that UBE3A is expressed in both glutamatergic and GABAergic neurons, and to a lesser extent in glial cells. We find that UBE3A in neurons has a non-uniform subcellular distribution. In somata, UBE3A preferentially concentrates in euchromatin-rich domains within the nucleus. Electron microscopy reveals that labeling concentrates in the head and neck of dendritic spines and is excluded from the PSD. Strongest labeling within the neuropil was found in axon terminals. Conclusions By highlighting the subcellular compartments in which UBE3A is likely to function in the human neocortex, our data provide insight into the diverse functional capacities of this E3 ligase. These anatomical data may help to elucidate the role of UBE3A in Angelman syndrome and autism spectrum disorder.

Published

2018

5. Loss of UBE3A from TH-expressing neurons suppresses GABA co-release and enhances VTA-NAc optical self-stimulation

Author

Janet Berrios, Alice M. Stamatakis, Pranish A. Kantak, Zoe A. McElligott, Matthew C. Judson, Megumi Aita, Marie Rougie, Garret D. Stuber, and Benjamin D. Philpot

Subjects

Science

Abstract

Mesoaccumbal terminals within the VTA are known to co-release both GABA and dopamine, although the functional role of the former has yet to be determined. Here, the authors find that non-canonical GABA release is regulated by the E3-ubiquitin ligase, UBE3A, and enhances optogenetic self-stimulation.

Published

2016

6. Dual-isoform hUBE3A gene transfer improves behavioral and seizure outcomes in Angelman syndrome model mice

Author

Noah W. Miller, Benjamin D. Philpot, A. Mattijs Punt, Courtney R. Davis, Charles Shyng, Jeremy M. Simon, David G. Amaral, Mirabel T. Salmon, Kimberly Ritola, Steven J. Gray, Ype Elgersma, Matthew C. Judson, Clinical Genetics, and Neurosciences

Subjects

Kozak consensus sequence, Ubiquitin-Protein Ligases, Neurodevelopment, Hippocampus, Therapeutics, Hippocampal formation, Epileptogenesis, Mice, Neurodevelopmental disorder, Gene therapy, Seizures, Angelman syndrome, medicine, UBE3A, Animals, Humans, Amino Acid Sequence, Neocortex, business.industry, General Medicine, medicine.disease, Disease Models, Animal, medicine.anatomical_structure, Treatment Outcome, Angelman Syndrome, business, Neuroscience, Neurological disorders, Research Article

Abstract

Loss of the maternal UBE3A allele causes Angelman syndrome (AS), a debilitating neurodevelopmental disorder. Here, we devised an AS treatment strategy based on reinstating dual-isoform expression of human UBE3A (hUBE3A) in the developing brain. Kozak sequence engineering of our codon-optimized vector (hUBE3Aopt) enabled translation of both short and long hUBE3A protein isoforms at a near-endogenous 3:1 (short/long) ratio, a feature that could help to support optimal therapeutic outcomes. To model widespread brain delivery and early postnatal onset of hUBE3A expression, we packaged the hUBE3Aopt vector into PHP.B capsids and performed intracerebroventricular injections in neonates. This treatment significantly improved motor learning and innate behaviors in AS mice, and it rendered them resilient to epileptogenesis and associated hippocampal neuropathologies induced by seizure kindling. hUBE3A overexpression occurred frequently in the hippocampus but was uncommon in the neocortex and other major brain structures; furthermore, it did not correlate with behavioral performance. Our results demonstrate the feasibility, tolerability, and therapeutic potential for dual-isoform hUBE3A gene transfer in the treatment of AS.

Published

2021

7. Ube3a reinstatement mitigates epileptogenesis in Angelman syndrome model mice

Author

Marie Rougie, Kelly E. Carstens, Bin Gu, Ellen P. Clark, Benjamin D. Philpot, Matthew C. Judson, Serena M. Dudek, and Katherine A Dalton

Subjects

0301 basic medicine, Mossy fiber (hippocampus), congenital, hereditary, and neonatal diseases and abnormalities, Ubiquitin-Protein Ligases, Hippocampus, Epileptogenesis, Mice, 03 medical and health sciences, Epilepsy, 0302 clinical medicine, Seizures, Angelman syndrome, UBE3A, Animals, Humans, Medicine, business.industry, Dentate gyrus, Concise Communication, Flurothyl, General Medicine, medicine.disease, Disease Models, Animal, 030104 developmental biology, Mossy Fibers, Hippocampal, Angelman Syndrome, business, Neuroscience, 030217 neurology & neurosurgery

Abstract

Angelman syndrome (AS) is a neurodevelopmental disorder in which epilepsy is common (~90%) and often refractory to antiepileptics. AS is caused by mutation of the maternal allele encoding the ubiquitin protein ligase E3A (UBE3A), but it is unclear how this genetic insult confers vulnerability to seizure development and progression (i.e., epileptogenesis). Here, we implemented the flurothyl kindling and retest paradigm in AS model mice to assess epileptogenesis and to gain mechanistic insights owed to loss of maternal Ube3a. AS model mice kindled similarly to wild-type mice, but they displayed a markedly increased sensitivity to flurothyl-, kainic acid-, and hyperthermia-induced seizures measured a month later during retest. Pathological characterization revealed enhanced deposition of perineuronal nets in the dentate gyrus of the hippocampus of AS mice in the absence of overt neuronal loss or mossy fiber sprouting. This pro-epileptogenic phenotype resulted from Ube3a deletion in GABAergic but not glutamatergic neurons, and it was rescued by pancellular reinstatement of Ube3a at postnatal day 21 (P21), but not during adulthood. Our results suggest that epileptogenic susceptibility in AS patients is a consequence of the dysfunctional development of GABAergic circuits, which may be amenable to therapies leveraging juvenile reinstatement of UBE3A.

Published

2018

8. Subcellular organization of UBE3A in human cerebral cortex

Author

Benjamin D. Philpot, William W. Seeley, Alain C. Burette, Matthew C. Judson, Richard J. Weinberg, Edward F. Chang, and Alissa Nana Li

Subjects

Male, 0301 basic medicine, Dendritic spine, Autism, lcsh:RC346-429, Euchromatin, E6-AP, 0302 clinical medicine, Stem Cell Research - Nonembryonic - Human, 80 and over, Axon, gamma-Aminobutyric Acid, Aged, 80 and over, Cerebral Cortex, Neurons, Temporal cortex, Microscopy, Neocortex, Human brain, Middle Aged, Mitochondria, Psychiatry and Mental health, Mental Health, medicine.anatomical_structure, Cerebral cortex, Neurological, Female, Adult, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Ubiquitin-Protein Ligases, Intellectual and Developmental Disabilities (IDD), 1.1 Normal biological development and functioning, Clinical Sciences, and over, Biology, Electron, Young Adult, 03 medical and health sciences, Rare Diseases, Developmental Neuroscience, Underpinning research, Glial Fibrillary Acidic Protein, medicine, UBE3A, Neuropil, Humans, Axon terminal, Molecular Biology, lcsh:Neurology. Diseases of the nervous system, Aged, Epilepsy, Research, Neurosciences, Stem Cell Research, Brain Disorders, Microscopy, Electron, 030104 developmental biology, Angelman syndrome, Neuroscience, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Background Loss of UBE3A causes Angelman syndrome, whereas excess UBE3A activity appears to increase the risk for autism. Despite this powerful association with neurodevelopmental disorders, there is still much to be learned about UBE3A, including its cellular and subcellular organization in the human brain. The issue is important, since UBE3A’s localization is integral to its function. Methods We used light and electron microscopic immunohistochemistry to study the cellular and subcellular distribution of UBE3A in the adult human cerebral cortex. Experiments were performed on multiple tissue sources, but our results focused on optimally preserved material, using surgically resected human temporal cortex of high ultrastructural quality from nine individuals. Results We demonstrate that UBE3A is expressed in both glutamatergic and GABAergic neurons, and to a lesser extent in glial cells. We find that UBE3A in neurons has a non-uniform subcellular distribution. In somata, UBE3A preferentially concentrates in euchromatin-rich domains within the nucleus. Electron microscopy reveals that labeling concentrates in the head and neck of dendritic spines and is excluded from the PSD. Strongest labeling within the neuropil was found in axon terminals. Conclusions By highlighting the subcellular compartments in which UBE3A is likely to function in the human neocortex, our data provide insight into the diverse functional capacities of this E3 ligase. These anatomical data may help to elucidate the role of UBE3A in Angelman syndrome and autism spectrum disorder.

Published

2018

9. Enhanced Operant Extinction and Prefrontal Excitability in a Mouse Model of Angelman Syndrome

Author

Marie Rougie, Natallia V. Riddick, Matthew C. Judson, Hyojin Kim, Sheryl S. Moy, Viktoriya D. Nikolova, Alejandra I. Ferrer, Benjamin D. Philpot, and Michael S. Sidorov

Subjects

Male, 0301 basic medicine, Patch-Clamp Techniques, Ubiquitin-Protein Ligases, Prefrontal Cortex, Extinction, Psychological, Executive Function, Mice, 03 medical and health sciences, Cognition, Discrimination, Psychological, 0302 clinical medicine, Neurodevelopmental disorder, Angelman syndrome, Intellectual disability, medicine, UBE3A, Animals, Prefrontal cortex, Research Articles, General Neuroscience, Extinction (psychology), medicine.disease, Mice, Inbred C57BL, Phenotype, 030104 developmental biology, Conditioning, Operant, Angelman Syndrome, Cues, Abnormality, Cognition Disorders, Psychology, Neuroscience, Gene Deletion, 030217 neurology & neurosurgery

Abstract

Angelman syndrome (AS), a neurodevelopmental disorder associated with intellectual disability, is caused by loss of maternal allele expression ofUBE3Ain neurons. Mouse models of AS faithfully recapitulate disease phenotypes across multiple domains, including behavior. Yet in AS, there has been only limited study of behaviors encoded by the prefrontal cortex, a region broadly involved in executive function and cognition. Because cognitive impairment is a core feature of AS, it is critical to develop behavioral readouts of prefrontal circuit function in AS mouse models. One such readout is behavioral extinction, which has been well described mechanistically and relies upon prefrontal circuits in rodents. Here we report exaggerated operant extinction in male AS model mice, concomitant with enhanced excitability in medial prefrontal neurons from male and female AS model mice. Abnormal behavior was specific to operant extinction, as two other prefrontally dependent tasks (cued fear extinction and visuospatial discrimination) were largely normal in AS model mice. Inducible deletion ofUbe3aduring adulthood was not sufficient to drive abnormal extinction, supporting the hypothesis that there is an early critical period for development of cognitive phenotypes in AS. This work represents the first formal experimental analysis of prefrontal circuit function in AS, and identifies operant extinction as a useful experimental paradigm for modeling cognitive aspects of AS in mice.SIGNIFICANCE STATEMENTPrefrontal cortex encodes “high-level” cognitive processes. Thus, understanding prefrontal function is critical in neurodevelopmental disorders where cognitive impairment is highly penetrant. Angelman syndrome is a neurodevelopmental disorder associated with speech and motor impairments, an outwardly happy demeanor, and intellectual disability. We describe a behavioral phenotype in a mouse model of Angelman syndrome and related abnormalities in prefrontal cortex function. We hypothesize that robust and reliable prefrontally encoded behavior may be used to model cognitive impairments in Angelman syndrome.

Published

2018

10. Decreased Axon Caliber Underlies Loss of Fiber Tract Integrity, Disproportional Reductions in White Matter Volume, and Microcephaly in Angelman Syndrome Model Mice

Author

Ashley Rumple, Martin Styner, Courtney Thaxton, Alaine L. Pribisko, Mark D. Shen, Alain C. Burette, Matthew C. Judson, Wilmer A. Del Cid, Beatriz Paniagua, Richard J. Weinberg, and Benjamin D. Philpot

Subjects

Male, 0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Microcephaly, Ubiquitin-Protein Ligases, Biology, White matter, Mice, 03 medical and health sciences, Nerve Fibers, 0302 clinical medicine, Neurodevelopmental disorder, Angelman syndrome, medicine, UBE3A, Animals, Axon, Research Articles, Loss function, Mice, Knockout, General Neuroscience, medicine.disease, White Matter, Axons, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Female, Angelman Syndrome, Neuroscience, 030217 neurology & neurosurgery, Neurotypical

Abstract

Angelman syndrome (AS) is a debilitating neurodevelopmental disorder caused by loss of function of the maternally inherited UBE3A allele. It is currently unclear how the consequences of this genetic insult unfold to impair neurodevelopment. We reasoned that by elucidating the basis of microcephaly in AS, a highly penetrant syndromic feature with early postnatal onset, we would gain new insights into the mechanisms by which maternal UBE3A loss derails neurotypical brain growth and function. Detailed anatomical analysis of both male and female maternal Ube3a-null mice reveals that microcephaly in the AS mouse model is primarily driven by deficits in the growth of white matter tracts, which by adulthood are characterized by densely packed axons of disproportionately small caliber. Our results implicate impaired axon growth in the pathogenesis of AS and identify noninvasive structural neuroimaging as a potentially valuable tool for gauging therapeutic efficacy in the disorder.SIGNIFICANCE STATEMENT People who maternally inherit a deletion or nonfunctional copy of the UBE3A gene develop Angelman syndrome (AS), a severe neurodevelopmental disorder. To better understand how loss of maternal UBE3A function derails brain development, we analyzed brain structure in a maternal Ube3a knock-out mouse model of AS. We report that the volume of white matter (WM) is disproportionately reduced in AS mice, indicating that deficits in WM development are a major factor underlying impaired brain growth and microcephaly in the disorder. Notably, we find that axons within the WM pathways of AS model mice are abnormally small in caliber. This defect is associated with slowed nerve conduction, which could contribute to behavioral deficits in AS, including motor dysfunction.

Published

2017

11. Delayed loss of UBE3A reduces the expression of Angelman syndrome-associated phenotypes

Author

Johanna Hakonen, Sara Silva-Santos, Matthew C. Judson, Benjamin D. Philpot, Mireia Bernabé Kleijn, Geeske M. van Woerden, Ype Elgersma, Monica Sonzogni, and Neurosciences

Subjects

Male, Aging, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Neurology, Ubiquitin-Protein Ligases, Short Report, Biology, Bioinformatics, lcsh:RC346-429, Mouse model, 03 medical and health sciences, 0302 clinical medicine, Neurodevelopmental disorder, Developmental Neuroscience, Angelman syndrome, UBE3A, medicine, Animals, Autism spectrum disorder, Molecular Biology, lcsh:Neurology. Diseases of the nervous system, 030304 developmental biology, 0303 health sciences, Neuropsychology, medicine.disease, Seizure, Phenotype, Human genetics, Mice, Inbred C57BL, Psychiatry and Mental health, Ube3a, Female, Gene Deletion, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Background Angelman syndrome (AS) is a severe neurodevelopmental disorder caused by mutations affecting UBE3A gene expression. Previous studies in mice revealed distinct critical periods during neurodevelopment in which reactivation of Ube3a gene expression can prevent the onset of behavioral deficits. Whether UBE3A is required for brain function throughout life is unknown. Here, we address the importance of maintaining UBE3A expression after normal brain development. Findings Using a conditional mouse, we deleted the Ube3a gene at three ages spanning brain maturation. We assessed the consequences of Ube3a gene deletion by testing the mice in behavioral tasks previously shown to produce robust phenotypes in AS model mice. Early embryonic deletion of Ube3a recapitulated all behavioral deficits of AS mice. In contrast, Ube3a gene deletion at 3 or 12 weeks of age did not have a significant effect on most behavioral tasks and did not increase seizure sensitivity. Conclusions Taken together, these results emphasize that UBE3A critically impacts early brain development, but plays a more limited role in adulthood. Our findings provide important considerations for upcoming clinical trials in which UBE3A gene expression is reactivated and suggest that even transient UBE3A reinstatement during a critical window of early development is likely to prevent most adverse Angelman syndrome phenotypes. However, sustained UBE3A expression into adulthood is probably needed for optimal clinical benefit. Electronic supplementary material The online version of this article (10.1186/s13229-019-0277-1) contains supplementary material, which is available to authorized users.

Published

2019

12. GABAergic Neuron-Specific Loss of Ube3a Causes Angelman Syndrome-Like EEG Abnormalities and Enhances Seizure Susceptibility

Author

Ian F. G. King, Michael L. Wallace, Michael S. Sidorov, Benjamin D. Philpot, Mark J. Zylka, Ype Elgersma, Bin Gu, Geeske M. van Woerden, Richard J. Weinberg, Alain C. Burette, Ji Eun E. Han, Matthew C. Judson, and Neurosciences

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Neocortex, medicine.diagnostic_test, General Neuroscience, Electroencephalography, Biology, medicine.disease, 03 medical and health sciences, Epilepsy, Glutamatergic, 030104 developmental biology, 0302 clinical medicine, Neurodevelopmental disorder, medicine.anatomical_structure, Angelman syndrome, UBE3A, medicine, GABAergic, Neuroscience, 030217 neurology & neurosurgery

Abstract

Loss of maternal UBE3A causes Angelman syndrome (AS), a neurodevelopmental disorder associated with severe epilepsy. We previously implicated GABAergic deficits onto layer (L) 2/3 pyramidal neurons in the pathogenesis of neocortical hyperexcitability, and perhaps epilepsy, in AS model mice. Here we investigate consequences of selective Ube3a loss from either GABAergic or glutamatergic neurons, focusing on the development of hyperexcitability within L2/3 neocortex and in broader circuit and behavioral contexts. We find that GABAergic Ube3a loss causes AS-like increases in neocortical EEG delta power, enhances seizure susceptibility, and leads to presynaptic accumulation of clathrin-coated vesicles (CCVs) – all without decreasing GABAergic inhibition onto L2/3 pyramidal neurons. Conversely, glutamatergic Ube3a loss fails to yield EEG abnormalities, seizures, or associated CCV phenotypes, despite impairing tonic inhibition onto L2/3 pyramidal neurons. These results substantiate GABAergic Ube3a loss as the principal cause of circuit hyperexcitability in AS mice, lending insight into ictogenic mechanisms in AS.

Published

2016

13. Allelic specificity of Ube3a Expression In The Mouse Brain During Postnatal Development

Author

Wilmer A. Del Cid, Benjamin D. Philpot, Jason O. Sosa-Pagan, Ji Eun Han, and Matthew C. Judson

Subjects

Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Cell type, General Neuroscience, Biology, medicine.disease, Phenotype, Cell biology, Neurodevelopmental disorder, Angelman syndrome, medicine, UBE3A, Gene silencing, Allele, Genomic imprinting

Abstract

Genetic alterations of the maternal UBE3A allele result in Angelman syndrome (AS), a neurodevelopmental disorder characterized by severe developmental delay, lack of speech, and difficulty with movement and balance. The combined effects of maternal UBE3A mutation and cell type-specific epigenetic silencing of paternal UBE3A are hypothesized to result in a complete loss of functional UBE3A protein in neurons. However, the allelic specificity of UBE3A expression in neurons and other cell types in the brain has yet to be characterized throughout development, including the early postnatal period when AS phenotypes emerge. Here we define maternal and paternal allele-specific Ube3a protein expression throughout postnatal brain development in the mouse, a species which exhibits orthologous epigenetic silencing of paternal Ube3a in neurons and AS-like behavioral phenotypes subsequent to maternal Ube3a deletion. We find that neurons downregulate paternal Ube3a protein expression as they mature and, with the exception of neurons born from postnatal stem cell niches, do not express detectable paternal Ube3a beyond the first postnatal week. By contrast, neurons express maternal Ube3a throughout postnatal development, during which time localization of the protein becomes increasingly nuclear. Unlike neurons, astrocytes and oligodendrotyes biallelically express Ube3a. Notably, mature oligodendrocytes emerge as the predominant Ube3a-expressing glial cell type in the cortex and white matter tracts during postnatal development. These findings demonstrate the spatiotemporal characteristics of allele-specific Ube3a expression in key brain cell types, thereby improving our understanding of the developmental parameters of paternal Ube3a silencing and the cellular basis of AS.

Published

2014

14. Loss of UBE3A from TH-expressing neurons suppresses GABA co-release and enhances VTA-NAc optical self-stimulation

Author

Marie Rougie, Zoe A. McElligott, Pranish A. Kantak, Benjamin D. Philpot, Garret D. Stuber, Megumi Aita, Janet Berrios, Alice M. Stamatakis, and Matthew C. Judson

Subjects

0301 basic medicine, Patch-Clamp Techniques, Dopamine, General Physics and Astronomy, Synaptic Transmission, Nucleus Accumbens, Stereotaxic Techniques, Mice, 0302 clinical medicine, Self Stimulation, Neural Pathways, In Situ Hybridization, Fluorescence, gamma-Aminobutyric Acid, Mice, Knockout, Neurons, Multidisciplinary, Behavior, Animal, Dopaminergic, Glutamate receptor, Immunohistochemistry, Ventral tegmental area, medicine.anatomical_structure, Biochemistry, Reinforcement, Psychology, medicine.drug, Tyrosine 3-Monooxygenase, Science, Ubiquitin-Protein Ligases, Neurotransmission, Biology, Nucleus accumbens, General Biochemistry, Genetics and Molecular Biology, gamma-Aminobutyric acid, Article, 03 medical and health sciences, Reward, medicine, Animals, Motivation, Dopaminergic Neurons, Ventral Tegmental Area, General Chemistry, Mice, Inbred C57BL, Optogenetics, 030104 developmental biology, nervous system, Stereotaxic technique, Neuroscience, 030217 neurology & neurosurgery

Abstract

Motivated reward-seeking behaviours are governed by dopaminergic ventral tegmental area projections to the nucleus accumbens. In addition to dopamine, these mesoaccumbal terminals co-release other neurotransmitters including glutamate and GABA, whose roles in regulating motivated behaviours are currently being investigated. Here we demonstrate that loss of the E3-ubiquitin ligase, UBE3A, from tyrosine hydroxylase-expressing neurons impairs mesoaccumbal, non-canonical GABA co-release and enhances reward-seeking behaviour measured by optical self-stimulation., Mesoaccumbal terminals within the VTA are known to co-release both GABA and dopamine, although the functional role of the former has yet to be determined. Here, the authors find that non-canonical GABA release is regulated by the E3-ubiquitin ligase, UBE3A, and enhances optogenetic self-stimulation.

Published

2016

15. A new synaptic player leading to autism risk: Met receptor tyrosine kinase

Author

Pat Levitt, Matthew C. Judson, and Kathie L. Eagleson

Subjects

Hepatocyte growth factor, Candidate gene, Neocortex, Cognitive Neuroscience, Synaptogenesis, medicine.disease, Human genetics, Article, Pathology and Forensic Medicine, Synapse, medicine.anatomical_structure, Autism spectrum disorder, Pediatrics, Perinatology and Child Health, Forebrain, medicine, Autism, Neurology (clinical), Psychology, Neuroscience

Abstract

The validity for assigning disorder risk to an autism spectrum disorder (ASD) candidate gene comes from convergent genetic, clinical, and developmental neurobiology data. Here, we review these lines of evidence from multiple human genetic studies, and non-human primate and mouse experiments that support the conclusion that the MET receptor tyrosine kinase (RTK) functions to influence synapse development in circuits relevant to certain core behavioral domains of ASD. There is association of both common functional alleles and rare copy number variants that impact levels of MET expression in the human cortex. The timing of Met expression is linked to axon terminal outgrowth and synaptogenesis in the developing rodent and primate forebrain, and both in vitro and in vivo studies implicate this RTK in dendritic branching, spine maturation, and excitatory connectivity in the neocortex. This impact can occur in a cell-nonautonomous fashion, emphasizing the unique role that Met plays in specific circuits relevant to ASD.

Published

2011

16. Conserved Subcortical and Divergent Cortical Expression of Proteins Encoded by Orthologs of the Autism Risk Gene MET

Author

Pat Levitt, David G. Amaral, and Matthew C. Judson

Subjects

vision, Cognitive Neuroscience, Neocortex, Nerve Tissue Proteins, Macaque, Conserved sequence, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Species Specificity, biology.animal, medicine, Neuropil, Animals, Genetic Predisposition to Disease, circuitry, HGF, Autistic Disorder, Conserved Sequence, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, biology, social, Articles, Proto-Oncogene Proteins c-met, biology.organism_classification, Macaca mulatta, Mice, Inbred C57BL, Rhesus macaque, medicine.anatomical_structure, Animals, Newborn, Gene Expression Regulation, nervous system, Posterior cingulate, Forebrain, Neuroscience, 030217 neurology & neurosurgery

Abstract

Met receptor tyrosine kinase signaling regulates the growth and development of axons and may contribute to the wiring of cortical and limbic circuits in the rodent forebrain. Whether the orthologous MET receptor functions similarly in the developing primate forebrain is not known but is of considerable interest considering the association of variant MET alleles with social and communication phenotypes in autism. To begin addressing this question, we compared Met/MET protein expression in the developing mouse and rhesus macaque forebrain. There was a strong temporal conservation of expression during the time of rapid axon development and the onset of robust synapse formation. Expression patterns of Met/MET in limbic-related structures were almost identical between species. In marked contrast, there was highly divergent expression in the neocortex. In mouse, Met was broadly distributed throughout neocortex. In the macaque, robust MET expression was largely restricted to the posterior cingulate, inferior temporal, posterior parietal, and visual cortices, including face processing regions. The pattern is consistent with the importance of vision in the social repertoire of the primate. Collectively, these data suggest a conserved developmental function of the MET receptor in wiring together limbic and neocortical circuits that facilitate species-appropriate responses, including social behavior.

Published

2010

17. Evidence of cell-nonautonomous changes in dendrite and dendritic spine morphology in the met-signaling-deficient mouse forebrain

Author

Kathie L. Eagleson, Pat Levitt, Lily Wang, and Matthew C. Judson

Subjects

Male, Dendritic spine, Dendritic Spines, Biology, Medium spiny neuron, Article, Mice, Postsynaptic potential, medicine, Animals, Humans, Cerebral Cortex, Mice, Knockout, Neurons, Neocortex, Pyramidal Cells, General Neuroscience, fungi, Dendrites, Proto-Oncogene Proteins c-met, Cell biology, Cortex (botany), Mice, Inbred C57BL, medicine.anatomical_structure, nervous system, Cerebral cortex, Synapses, Forebrain, Pyramidal cell, Neuroscience, Signal Transduction

Abstract

Human genetic findings and murine neuroanatomical expression mapping have intersected to implicate Met receptor tyrosine kinase signaling in the development of forebrain circuits controlling social and emotional behaviors that are atypical in autism-spectrum disorders (ASD). To clarify roles for Met signaling during forebrain circuit development in vivo, we generated mutant mice (Emx1(Cre)/Met(fx/fx)) with an Emx1-Cre-driven deletion of signaling-competent Met in dorsal pallially derived forebrain neurons. Morphometric analyses of Lucifer yellow-injected pyramidal neurons in postnatal day 40 anterior cingulate cortex (ACC) revealed no statistically significant changes in total dendritic length but a selective reduction in apical arbor length distal to the soma in Emx1(Cre)/Met(fx/fx) neurons relative to wild type, consistent with a decrease in the total tissue volume sampled by individual arbors in the cortex. The effects on dendritic structure appear to be circuit-selective, insofar as basal arbor length was increased in Emx1(Cre)/Met(fx/fx) layer 2/3 neurons. Spine number was not altered on the Emx1(Cre)/Met(fx/fx) pyramidal cell populations studied, but spine head volume was significantly increased (∼20%). Cell-nonautonomous, circuit-level influences of Met signaling on dendritic development were confirmed by studies of medium spiny neurons (MSN), which do not express Met but receive Met-expressing corticostriatal afferents during development. Emx1(Cre)/Met(fx/fx) MSN exhibited robust increases in total arbor length (∼20%). As in the neocortex, average spine head volume was also increased (∼12%). These data demonstrate that a developmental loss of presynaptic Met receptor signaling can affect postsynaptic morphogenesis and suggest a mechanism whereby attenuated Met signaling could disrupt both local and long-range connectivity within circuits relevant to ASD.

Published

2010

18. Dissociation of locomotor and cerebellar deficits in a murine Angelman syndrome model

Author

Benjamin D. Philpot, Chris I. De Zeeuw, Martijn Schonewille, Eleonora Aronica, Zhenyu Gao, Freek E. Hoebeek, Matthew C. Judson, Caroline F. Bruinsma, Ype Elgersma, Geeske M. van Woerden, ANS - Amsterdam Neuroscience, APH - Amsterdam Public Health, Pathology, Cellular and Computational Neuroscience (SILS, FNWI), Faculteit der Geneeskunde, Neurosciences, and Netherlands Institute for Neuroscience (NIN)

Subjects

Male, Cerebellum, Ubiquitin-Protein Ligases, Purkinje cell, Biology, Rotarod performance test, 03 medical and health sciences, Mice, Purkinje Cells, 0302 clinical medicine, Angelman syndrome, medicine, UBE3A, Animals, Humans, Phosphorylation, Gait Disorders, Neurologic, 030304 developmental biology, 0303 health sciences, Learning Disabilities, General Medicine, Anatomy, Reflex, Vestibulo-Ocular, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, medicine.anatomical_structure, nervous system, Cerebellar cortex, Rotarod Performance Test, Synaptic plasticity, Reflex, Female, Angelman Syndrome, Calcium-Calmodulin-Dependent Protein Kinase Type 2, Neuroscience, Protein Processing, Post-Translational, 030217 neurology & neurosurgery, Locomotion, Psychomotor Performance, Research Article

Abstract

Angelman syndrome (AS) is a severe neurological disorder that is associated with prominent movement and balance impairments that are widely considered to be due to defects of cerebellar origin. Here, using the cerebellar-specific vestibulo-ocular reflex (VOR) paradigm, we determined that cerebellar function is only mildly impaired in the Ube3a(m-/P+) mouse model of AS. VOR phase-reversal learning was singularly impaired in these animals and correlated with reduced tonic inhibition between Golgi cells and granule cells. Purkinje cell physiology, in contrast, was normal in AS mice as shown by synaptic plasticity and spontaneous firing properties that resembled those of controls. Accordingly, neither VOR phas-ereversal learning nor locomotion was impaired following selective deletion of Ube3a in Purkinje cells. However, genetic normalization of alpha CaMKII inhibitory phosphorylation fully rescued locomotor deficits despite failing to improve cerebellar learning in AS mice, suggesting extracerebellar circuit involvement in locomotor learning. We confirmed this hypothesis through cerebellum-specific reinstatement of Ube3a, which ameliorated cerebellar learning deficits but did not rescue locomotor deficits. This double dissociation of locomotion and cerebellar phenotypes strongly suggests that the locomotor deficits of AS mice do not arise from impaired cerebellar cortex function. Our results provide important insights into the etiology of the motor deficits associated with AS.

Published

2015

19. Allelic specificity of Ube3a expression in the mouse brain during postnatal development

Author

Matthew C, Judson, Jason O, Sosa-Pagan, Wilmer A, Del Cid, Ji Eun, Han, and Benjamin D, Philpot

Subjects

Male, Mice, Knockout, congenital, hereditary, and neonatal diseases and abnormalities, Ubiquitin-Protein Ligases, Brain, Nerve Fibers, Myelinated, Gene Expression Regulation, Enzymologic, Article, Mice, Inbred C57BL, Mice, Mice, Congenic, Animals, Newborn, Animals, Female, Alleles

Abstract

Genetic alterations of the maternal UBE3A allele result in Angelman syndrome (AS), a neurodevelopmental disorder characterized by severe developmental delay, lack of speech, and difficulty with movement and balance. The combined effects of maternal UBE3A mutation and cell type-specific epigenetic silencing of paternal UBE3A are hypothesized to result in a complete loss of functional UBE3A protein in neurons. However, the allelic specificity of UBE3A expression in neurons and other cell types in the brain has yet to be characterized throughout development, including the early postnatal period when AS phenotypes emerge. Here we define maternal and paternal allele-specific Ube3a protein expression throughout postnatal brain development in the mouse, a species which exhibits orthologous epigenetic silencing of paternal Ube3a in neurons and AS-like behavioral phenotypes subsequent to maternal Ube3a deletion. We find that neurons downregulate paternal Ube3a protein expression as they mature and, with the exception of neurons born from postnatal stem cell niches, do not express detectable paternal Ube3a beyond the first postnatal week. By contrast, neurons express maternal Ube3a throughout postnatal development, during which time localization of the protein becomes increasingly nuclear. Unlike neurons, astrocytes and oligodendrotyes biallelically express Ube3a. Notably, mature oligodendrocytes emerge as the predominant Ube3a-expressing glial cell type in the cortex and white matter tracts during postnatal development. These findings demonstrate the spatiotemporal characteristics of allele-specific Ube3a expression in key brain cell types, thereby improving our understanding of the developmental parameters of paternal Ube3a silencing and the cellular basis of AS.

Published

2013

20. Subcellular organization of UBE3A in neurons

Author

Benjamin D. Philpot, Kristen D. Phend, Matthew C. Judson, Richard J. Weinberg, Alain C. Burette, and Susan Burette

Subjects

0301 basic medicine, chemistry.chemical_classification, congenital, hereditary, and neonatal diseases and abnormalities, DNA ligase, biology, General Neuroscience, Immunocytochemistry, medicine.disease, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Ubiquitin, chemistry, Axon terminal, Proteasome, Angelman syndrome, biology.protein, medicine, UBE3A, Axon, 030217 neurology & neurosurgery

Abstract

Ubiquitination regulates a broad array of cellular processes, and defective ubiquitination is implicated in several neurological disorders. Loss of the E3 ubiquitin-protein ligase UBE3A causes Angelman syndrome. Despite its clinical importance, the normal role of UBE3A in neurons is still unclear. As a step toward deciphering its possible functions, we performed high-resolution light and electron microscopic immunocytochemistry. We report a broad distribution of UBE3A in neurons, highlighted by concentrations in axon terminals and euchromatin-rich nuclear domains. Our findings suggest that UBE3A may act locally to regulate individual synapses while also mediating global, neuronwide influences through the regulation of gene transcription. J. Comp. Neurol. 525:233-251, 2017. © 2016 Wiley Periodicals, Inc.

Published

2016

21. Angelman syndrome: insights into genomic imprinting and neurodevelopmental phenotypes

Author

Benjamin D. Philpot, Matthew C. Judson, Angela M. Mabb, and Mark J. Zylka

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Ubiquitin-Protein Ligases, Gene Expression, Article, Genomic Imprinting, Mice, Neurodevelopmental disorder, Angelman syndrome, UBE3A, medicine, Animals, Humans, Epigenetics, Regulation of gene expression, Genetics, biology, General Neuroscience, Genetic disorder, Brain, medicine.disease, Ubiquitin ligase, Phenotype, Gene Expression Regulation, biology.protein, Angelman Syndrome, Genomic imprinting

Abstract

Angelman syndrome (AS) is a severe genetic disorder caused by mutations or deletions of the maternally inherited UBE3A gene. UBE3A encodes an E3 ubiquitin ligase that is expressed biallelically in most tissues but is maternally expressed in almost all neurons. In this review, we describe recent advances in understanding the expression and function of UBE3A in the brain and the etiology of AS. We highlight current AS model systems, epigenetic mechanisms of UBE3A regulation, and the identification of potential UBE3A substrates in the brain. In the process, we identify major gaps in our knowledge that, if bridged, could move us closer to identifying treatments for this debilitating neurodevelopmental disorder.

Published

2011

22. Dynamic gene and protein expression patterns of the autism-associated met receptor tyrosine kinase in the developing mouse forebrain

Author

Matthew C. Judson, Daniel B. Campbell, Kathie L. Eagleson, Mica Y. Bergman, and Pat Levitt

Subjects

Neurite, Cellular differentiation, Blotting, Western, Synaptogenesis, In situ hybridization, Biology, Hippocampus, Polymerase Chain Reaction, Article, Mice, Limbic system, Prosencephalon, medicine, Limbic System, Animals, Autistic Disorder, In Situ Hybridization, Homeodomain Proteins, Mice, Knockout, Neurons, Neocortex, General Neuroscience, Age Factors, Gene Expression Regulation, Developmental, Receptor Protein-Tyrosine Kinases, Cell Differentiation, Proto-Oncogene Proteins c-met, Amygdala, Embryo, Mammalian, Immunohistochemistry, Mice, Inbred C57BL, medicine.anatomical_structure, Animals, Newborn, Forebrain, Signal transduction, Neuroscience, Signal Transduction, Transcription Factors

Abstract

The establishment of appropriate neural circuitry depends on the coordination of multiple developmental events across space and time. These events include proliferation, migration, differentiation, and survival-all of which can be mediated by hepatocyte growth factor (HGF) signaling through the Met receptor tyrosine kinase. We previously found a functional promoter variant of the MET gene to be associated with autism spectrum disorder, suggesting that forebrain circuits governing social and emotional function may be especially vulnerable to developmental disruptions in HGF/Met signaling. However, little is known about the spatiotemporal distribution of Met expression in the forebrain during the development of such circuits. To advance our understanding of the neurodevelopmental influences of Met activation, we employed complementary Western blotting, in situ hybridization, and immunohistochemistry to comprehensively map Met transcript and protein expression throughout perinatal and postnatal development of the mouse forebrain. Our studies reveal complex and dynamic spatiotemporal patterns of expression during this period. Spatially, Met transcript is localized primarily to specific populations of projection neurons within the neocortex and in structures of the limbic system, including the amygdala, hippocampus, and septum. Met protein appears to be principally located in axon tracts. Temporally, peak expression of transcript and protein occurs during the second postnatal week. This period is characterized by extensive neurite outgrowth and synaptogenesis, supporting a role for the receptor in these processes. Collectively, these data suggest that Met signaling may be necessary for the appropriate wiring of forebrain circuits, with particular relevance to the social and emotional dimensions of behavior.

Published

2009

23. [P179]: Met signalling modulates cortical pyramidal cell dendritic development in vivo

Author

Matthew C. Judson, Kathie L. Eagleson, and Pat Levitt

Subjects

medicine.anatomical_structure, Signalling, Developmental Neuroscience, In vivo, Chemistry, Cortex (anatomy), medicine, Pyramidal cell, Neuroscience, Developmental Biology

Published

2006

24. [ST6]: Met modulates cortical circuit development in vivo

Author

Pat Levitt, Matthew C. Judson, Mica Y. Bergman, and Kathie L. Eagleson

Subjects

Developmental Neuroscience, In vivo, Biology, Neuroscience, Developmental Biology

Published

2008