Your search keyword '"Hobo B"' showing total 15 results

1. Alzheimer-associated APP+1 transgenic mice: frameshift beta-amyloid precursor protein is secreted in cerebrospinal fluid without inducing neuropathology.

Author

Fischer DF, Hol EM, Hobo B, and van Leeuwen FW

Subjects

Animals, Frameshift Mutation, Mice, Mice, Inbred C57BL, Mice, Transgenic, Tissue Distribution, Alzheimer Disease cerebrospinal fluid, Alzheimer Disease pathology, Blood Proteins cerebrospinal fluid, Blood Proteins genetics, Brain pathology, Disease Models, Animal, Neurons metabolism, Poly(A)-Binding Proteins cerebrospinal fluid, Poly(A)-Binding Proteins genetics

Abstract

Biomarkers present in the cerebrospinal fluid (CSF) of Alzheimer Disease patients could be instrumental in guiding diagnosis and monitoring of progression of the disease. We have previously reported on the secretion of a frameshifted form of amyloid-beta precursor protein, APP+1, into the CSF of Alzheimer patients and controls. APP+1 is secreted efficiently in controls, but during the progression of Alzheimer Disease, its secretion is reduced and APP+1 accumulates in tangle-bearing neurons. Here we describe the generation of a transgenic mouse line expressing APP+1 in the brain. These mice do not suffer from overt pathology or neurodegeneration, suggesting that APP+1 is not neurotoxic. To measure APP+1 levels in the CSF, we serially sampled CSF from the cisterna magna in the same mouse over a period of months. Indeed, APP+1 is secreted into the CSF of the transgenic mice, and APP+1 levels are stable over 1 year. This mouse model may guide the study of secretion deficits as found in Alzheimer Disease.

Published

2006

2. N-Acetylglucosamine Kinase–Small Nuclear Ribonucleoprotein Polypeptide N Interaction Promotes Axodendritic Branching in Neurons via Dynein-Mediated Microtubule Transport.

Author

Timalsina, Binod, Choi, Ho Jin, and Moon, Il Soo

Subjects

INDUCED pluripotent stem cells, N-acetylglucosamine, MICROTUBULES, PRADER-Willi syndrome, NEURONS

Abstract

N-acetylglucosamine kinase (NAGK) has been identified as an anchor protein that facilitates neurodevelopment with its non-canonical structural role. Similarly, small nuclear ribonucleoprotein polypeptide N (SNRPN) regulates neurodevelopment and cognitive ability. In our previous study, we revealed the interaction between NAGK and SNRPN in the neuron. However, the precise role in neurodevelopment is elusive. In this study, we investigate the role of NAGK and SNRPN in the axodendritic development of neurons. NAGK and SNRPN interaction is significantly increased in neurons at the crucial stages of neurodevelopment. Furthermore, overexpression of the NAGK and SNRPN proteins increases axodendritic branching and neuronal complexity, whereas the knockdown inhibits neurodevelopment. We also observe the interaction of NAGK and SNRPN with the dynein light-chain roadblock type 1 (DYNLRB1) protein variably during neurodevelopment, revealing the microtubule-associated delivery of the complex. Interestingly, NAGK and SNRPN proteins rescued impaired axodendritic development in an SNRPN depletion model of Prader–Willi syndrome (PWS) patient-derived induced pluripotent stem cell neurons. Taken together, these findings are crucial in developing therapeutic approaches for neurodegenerative diseases. [ABSTRACT FROM AUTHOR]

Published

2023

3. Neuropilin‐1 expression in GnRH neurons regulates prepubertal weight gain and sexual attraction.

Author

Vanacker, Charlotte, Trova, Sara, Shruti, Sonal, Casoni, Filippo, Messina, Andrea, Croizier, Sophie, Malone, Samuel, Ternier, Gaetan, Hanchate, Naresh Kumar, Rasika, S, Bouret, Sebastien G, Ciofi, Philippe, Giacobini, Paolo, and Prevot, Vincent

Subjects

PRECOCIOUS puberty, SEXUAL attraction, WEIGHT gain, NEURONS, HYPOTHALAMUS, OLFACTORY bulb, ENERGY policy

Abstract

Hypothalamic neurons expressing gonadotropin‐releasing hormone (GnRH), the "master molecule" regulating reproduction and fertility, migrate from their birthplace in the nose to their destination using a system of guidance cues, which include the semaphorins and their receptors, the neuropilins and plexins, among others. Here, we show that selectively deleting neuropilin‐1 in new GnRH neurons enhances their survival and migration, resulting in excess neurons in the hypothalamus and in their unusual accumulation in the accessory olfactory bulb, as well as an acceleration of mature patterns of activity. In female mice, these alterations result in early prepubertal weight gain, premature attraction to male odors, and precocious puberty. Our findings suggest that rather than being influenced by peripheral energy state, GnRH neurons themselves, through neuropilin–semaphorin signaling, might engineer the timing of puberty by regulating peripheral adiposity and behavioral switches, thus acting as a bridge between the reproductive and metabolic axes. Synopsis: By regulating GnRH neuronal survival, migration and activity, the expression of Neuropilin 1 in GnRH neurons regulates sexual attraction, prepubertal weight gain and the timing of puberty. Nrp1 expression in GnRH neurons controls their number and distribution during embryogenesis.The lack of Nrp1 expression in GnRH neurons triggers early sexual behavior.GnRH neurons are directly involved in prepubertal weight gain.Disrupting Nrp1 signaling in GnRH neurons leads to central precocious puberty. [ABSTRACT FROM AUTHOR]

Published

2020

4. A primary neural cell culture model to study neuron, astrocyte, and microglia interactions in neuroinflammation.

Author

Goshi, Noah, Morgan, Rhianna K., Lein, Pamela J., and Seker, Erkin

Subjects

ASTROCYTES, CELL culture, INFLAMMATION, PRIMARY cell culture, NEURONS, CENTRAL nervous system

Abstract

Background: Interactions between neurons, astrocytes, and microglia critically influence neuroinflammatory responses to insult in the central nervous system. In vitro astrocyte and microglia cultures are powerful tools to study specific molecular pathways involved in neuroinflammation; however, in order to better understand the influence of cellular crosstalk on neuroinflammation, new multicellular culture models are required.Methods: Primary cortical cells taken from neonatal rats were cultured in a serum-free "tri-culture" medium formulated to support neurons, astrocytes, and microglia, or a "co-culture" medium formulated to support only neurons and astrocytes. Caspase 3/7 activity and morphological changes were used to quantify the response of the two culture types to different neuroinflammatory stimuli mimicking sterile bacterial infection (lipopolysaccharide (LPS) exposure), mechanical injury (scratch), and seizure activity (glutamate-induced excitotoxicity). The secreted cytokine profile of control and LPS-exposed co- and tri-cultures were also compared.Results: The tri-culture maintained a physiologically relevant representation of neurons, astrocytes, and microglia for 14 days in vitro, while the co-cultures maintained a similar population of neurons and astrocytes, but lacked microglia. The continuous presence of microglia did not negatively impact the overall health of the neurons in the tri-culture, which showed reduced caspase 3/7 activity and similar neurite outgrowth as the co-cultures, along with an increase in the microglia-secreted neurotrophic factor IGF-1 and a significantly reduced concentration of CX3CL1 in the conditioned media. LPS-exposed tri-cultures showed significant astrocyte hypertrophy, increase in caspase 3/7 activity, and the secretion of a number of pro-inflammatory cytokines (e.g., TNF, IL-1α, IL-1β, and IL-6), none of which were observed in LPS-exposed co-cultures. Following mechanical trauma, the tri-culture showed increased caspase 3/7 activity, as compared to the co-culture, along with increased astrocyte migration towards the source of injury. Finally, the microglia in the tri-culture played a significant neuroprotective role during glutamate-induced excitotoxicity, with significantly reduced neuron loss and astrocyte hypertrophy in the tri-culture.Conclusions: The tri-culture consisting of neurons, astrocytes, and microglia more faithfully mimics in vivo neuroinflammatory responses than standard mono- and co-cultures. This tri-culture can be a useful tool to study neuroinflammation in vitro with improved accuracy in predicting in vivo neuroinflammatory phenomena. [ABSTRACT FROM AUTHOR]

Published

2020

5. ORANGE: A CRISPR/Cas9-based genome editing toolbox for epitope tagging of endogenous proteins in neurons.

Author

Willems, Jelmer, de Jong, Arthur P. H., Scheefhals, Nicky, Mertens, Eline, Catsburg, Lisa A. E., Poorthuis, Rogier B., de Winter, Fred, Verhaagen, Joost, Meye, Frank J., and MacGillavry, Harold D.

Subjects

GENOME editing, NEUROTRANSMITTER receptors, SCAFFOLD proteins, FLUORESCENT proteins, HIGH resolution imaging, NEURONS, GENETIC vectors, MOLECULAR cloning

Abstract

The correct subcellular distribution of proteins establishes the complex morphology and function of neurons. Fluorescence microscopy techniques are invaluable to investigate subcellular protein distribution, but they suffer from the limited ability to efficiently and reliably label endogenous proteins with fluorescent probes. We developed ORANGE: Open Resource for the Application of Neuronal Genome Editing, which mediates targeted genomic integration of epitope tags in rodent dissociated neuronal culture, in organotypic slices, and in vivo. ORANGE includes a knock-in library for in-depth investigation of endogenous protein distribution, viral vectors, and a detailed two-step cloning protocol to develop knock-ins for novel targets. Using ORANGE with (live-cell) superresolution microscopy, we revealed the dynamic nanoscale organization of endogenous neurotransmitter receptors and synaptic scaffolding proteins, as well as previously uncharacterized proteins. Finally, we developed a mechanism to create multiple knock-ins in neurons, mediating multiplex imaging of endogenous proteins. Thus, ORANGE enables quantification of expression, distribution, and dynamics for virtually any protein in neurons at nanoscale resolution. This study describes the development of a genome editing toolbox (ORANGE) for endogenous tagging of proteins in neurons. This open resource allows the investigation of protein localization and dynamics in neurons using live-cell and super-resolution imaging techniques. [ABSTRACT FROM AUTHOR]

Published

2020

6. Expression of a Mutant SEMA3A Protein with Diminished Signalling Capacity Does Not Alter ALS-Related Motor Decline, or Confer Changes in NMJ Plasticity after BotoxA-Induced Paralysis of Male Gastrocnemic Muscle.

Author

Moloney, Elizabeth B., Hobo, Barbara, De Winter, Fred, and Verhaagen, Joost

Subjects

NEUROPLASTICITY, MOTOR ability, CELL communication, PROTEIN expression, SKELETAL muscle, MUSCLE physiology, EFFERENT pathways

Abstract

Terminal Schwann cells (TSCs) are specialized cells that envelop the motor nerve terminal, and play a role in the maintenance and regeneration of neuromuscular junctions (NMJs). The chemorepulsive protein semaphorin 3A (SEMA3A) is selectively up-regulated in TSCs on fast-fatigable muscle fibers following experimental denervation of the muscle (BotoxA-induced paralysis or crush injury to the sciatic nerve) or in the motor neuron disease amyotrophic lateral sclerosis (ALS). Re-expression of SEMA3A in this subset of TSCs is thought to play a role in the selective plasticity of nerve terminals as observed in ALS and following BotoxA-induced paralysis. Using a mouse model expressing a mutant SEMA3A with diminished signaling capacity, we studied the influence of SEMA3A signaling at the NMJ with two denervation paradigms; a motor neuron disease model (the G93A-hSOD1 ALS mouse line) and an injury model (BotoxA-induced paralysis). ALS mice that either expressed 1 or 2 mutant SEMA3A alleles demonstrated no difference in ALS-induced decline in motor behavior. We also investigated the effects of BotoxA-induced paralysis on the sprouting capacity of NMJs in the K108N-SEMA3A mutant mouse, and observed no change in the differential neuronal plasticity found at NMJs on fast-fatigable or slow muscle fibers due to the presence of the SEMA3A mutant protein. Our data may be explained by the residual repulsive activity of the mutant SEMA3A, or it may imply that SEMA3A alone is not a key component of the molecular signature affecting NMJ plasticity in ALS or BotoxA-induced paralysis. Interestingly, we did observe a sex difference in motor neuron sprouting behavior after BotoxA-induced paralysis in WT mice which we speculate may be an important factor in the sex dimorphic differences seen in ALS. [ABSTRACT FROM AUTHOR]

Published

2017

7. HERC 1 Ubiquitin Ligase Mutation Affects Neocortical, CA3 Hippocampal and Spinal Cord Projection Neurons: An Ultrastructural Study.

Author

Ruiz, Rocío, Pérez-Villegas, Eva María, Bachiller, Sara, Luis Rosa, José, and Angel Armengol, José

Subjects

LIGASES, HIPPOCAMPUS (Brain), SPINAL cord, NEURONS, PURKINJE cells

Abstract

The spontaneous mutation tambaleante is caused by the Gly483Glu substitution in the highly conserved N terminal RCC1-like domain of the HERC1 protein, which leads to the increase of mutated protein levels responsible for cerebellar Purkinje cell death by autophagy. Until now, Purkinje cells have been the only central nervous neurons reported as being targeted by the mutation, and their degeneration elicits an ataxic syndrome in adult mutant mice. However, the ultrastructural analysis performed here demonstrates that signs of autophagy, such as autophagosomes, lysosomes, and altered mitochondria, are present in neocortical pyramidal, CA3 hippocampal pyramidal, and spinal cord motor neurons. The main difference is that the reduction in the number of neurons affected in the tambaleante mutation in the neocortex, the hippocampus, and the spinal cord is not so evident as the dramatic loss of cerebellar Purkinje cells. Interestingly, signs of autophagy are absent in both interneurons and neuroglia cells. Affected neurons have in common that they are projection neurons which receive strong and varied synaptic inputs, and possess the highest degree of neuronal activity. Therefore, because the integrity of the ubiquitin-proteasome system is essential for protein degradation and hence, for normal protein turnover, it could be hypothesized that the deleterious effects of the misrouting of these pathways would depend directly on the neuronal activity. [ABSTRACT FROM AUTHOR]

Published

2016

8. Nrp1, a Neuronal Regulator, Enhances DDR2-ERK-Runx2 Cascade in Osteoblast Differentiation via Suppression of DDR2 Degradation.

Author

Zhang, Yan, Su, Jin, Teng, Yue, Zhang, Jian, Wang, Jiang, Li, Kun, Yao, Libo, and Li, Xu

Subjects

NEURONS, OSTEOBLASTS, CELL differentiation, MESSENGER RNA, IMMUNOSUPPRESSION, IMMUNOBLOTTING, IMMUNOFLUORESCENCE

Abstract

Background: Osteoblastogenesis is under delicate control by multiple factors and hormones. Recent reports indicated the involvement of immunological and neuronal regulators. However, the role of neuropilin 1 (Nrp1) in osteoblastogenesis remains obscure. Methods: Real-time PCR was carried out to detect the mRNA of osteoblastic markers, Nrp1, and discoidin domain receptor 2 (DDR2). Immunoblot was performed to test the protein of Nrp1 and DDR2. Osteogenic differentiation was evaluated by mRNA analysis of osteogenic markers, and determination of ALP activity and OCN secretion. The intercellular signaling effectors were examined by immunoblot. Immunofluorescent assays were performed to detect the localization of Nrp1 and DDR2. Half-life determination assay was executed to test the DDR2 stability. Results: The expression of Nrp1 paralleled with that of DDR2 during osteoblastogensis. Nrp1 overexpression enhanced DDR2-induced stimulation of osteoblastogensis, whereas Nrp1 silencing caused attenuation. Nrp1 overexpression increased the phosphorylation of DDR2, ERK1/2 and Runx2. Nrp1 co-localized with DDR2 in the cellular membrane of differentiated MC3T3-E1. Enhanced or attenuated Nrp1 expression did not alter the mRNA transcript of DDR2. Nrp1 overexpression prolonged the half-life of DDR2 protein. Conclusion: Our results originally demonstrated the stimulatory role of Nrp1 in DDR2-induced osteoblast differentiation, providing molecular evidence for exploiting Nrp1 and DDR2 as targets to treat bone-related disease. © 2015 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2015

9. Segregated labeling of olfactory bulb projection neurons based on their birthdates.

Author

Imamura, Fumiaki and Greer, Charles A.

Subjects

OLFACTORY bulb, NEURONS, BIRTH date, ELECTROPORATION, NEURAL circuitry

Abstract

Mitral and tufted cells are the projection neurons of the olfactory bulb ( OB). We previously reported that somata location and innervation patterns were different between early- and late-born mitral cells (Imamura et al., 2011). Here, we introduced a plasmid that drives the expression of a GFP gene into the mouse OB using in utero electroporation, and demonstrated that we can deliver the plasmid vectors into distinct subsets of OB projection neurons by changing the timing of electroporation after fertilisation. The electroporation performed at embryonic day (E)10 preferentially labeled mitral cells in the accessory OB and main OB mitral cells in dorsomedial mitral cell layer ( MCL). In contrast, the E12 electroporation introduced the plasmid vectors preferentially into main OB mitral cells in the ventrolateral MCL and tufted cells. Combining these data with BrdU injections, we confirmed that E10 and E12 electroporation preferentially labeled early- and late-born projection neurons, respectively. This work introduces a novel method for segregated labeling of mouse olfactory bulb projection neurons based on their birthdates. With this technique we found that early- and late-born projection neurons extend their secondary dendrites in the deep and superficial external plexiform layer ( EPL), respectively. Although a similar segregation has been suggested for mitral vs. tufted cell dendrites, we found mitral cells projecting secondary dendrites into the superficial EPL in E12-electroporated main OB. Our observations indicate that timing of neurogenesis regulates not only somata location and innervation patterns but also the laminar organisation of projection neuron dendrites in the EPL. [ABSTRACT FROM AUTHOR]

Published

2015

10. Neuropathological Staging of Spinocerebellar Ataxia Type 2 by Semiquantitative 1 C2-Positive Neuron Typing. Nuclear Translocation of Cytoplasmic 1 C2 Underlies Disease Progression of Spinocerebellar Ataxia Type 2.

Author

Koyano, Shigeru, Yagishita, Saburo, Kuroiwa, Yoshiyuki, Tanaka, Fumiaki, and Uchihara, Toshiki

Subjects

SPINOCEREBELLAR ataxia, NEUROLOGICAL disorders, NEURONS, CYTOPLASM, TRINUCLEOTIDE repeats

Abstract

Spinocerebellar ataxia type 2 ( SCA2) is a hereditary neurodegenerative disorder caused by the expansion of the trinucleotide CAG repeats encoding elongated polyglutamine tract in ataxin-2, the SCA2 gene product. Polyglutamine diseases comprise nine genetic entities, including seven different forms of spinocerebellar ataxias, Huntington's disease, and spinal and bulbar muscular atrophy. These are pathologically characterized by neuronal loss and intranuclear aggregates or inclusions of mutant proteins including expanded polyglutamine in selected neuronal groups. Previously, we examined immunolocalization of ubiquitin, expanded polyglutamine (probed by 1 C2 antibody), and ataxin-2 in genetically confirmed SCA2 patients. In the present study, we expanded this approach by distinguishing different patterns of subcellular 1 C2 immunoreactivity ('granular cytoplasmic,' 'cytoplasmic and nuclear' and 'nuclear with inclusions.') and by quantifying their regional frequencies in three autopsied SCA2 brains at different stage of the disease. Comparison with neuronal loss and gliosis revealed that overall 1 C2 immunoreactivity was paralleled with their severity. Furthermore, appearance of granular cytoplasmic pattern corresponded to early stage, cytoplasmic and nuclear pattern to active stage, and nuclear with inclusions pattern to final stage. We conclude that this 1 C2-immunoreactive typing may be useful for evaluating the overall severity and extent of affected regions and estimating the neuropathological stage of SCA2. [ABSTRACT FROM AUTHOR]

Published

2014

11. Orexin (hypocretin) gene transfer diminishes narcoleptic sleep behavior in mice.

Author

Liu, Meng, Thankachan, Stephen, Kaur, Satvinder, Begum, Suraiya, Blanco‐Centurion, Carlos, Sakurai, Takeshi, Yanagisawa, Masashi, Neve, Rachael, and Shiromani, Priyattam J.

Subjects

OREXINS, HYPOTHALAMIC hormones, GENETIC transformation, NEURONS, NEUROSCIENCES, CEREBROSPINAL fluid, LABORATORY mice

Abstract

Gene transfer has proven to be an effective neurobiological tool in a number of neurodegenerative diseases, but it is not known if it can correct a sleep disorder. Narcolepsy is a neurodegenerative sleep disorder linked to the loss of neurons containing the neuropeptide orexin, also known as hypocretin. Here, a replication-defective herpes simplex virus-1 amplicon-based vector was constructed to transfer the gene for mouse prepro-orexin into mice with a genetic deletion of the orexin gene. After in vitro tests confirmed successful gene transfer into cells, the gene vector was delivered to the lateral hypothalamus of orexin knockout (KO) mice where the orexin peptide was robustly expressed in the somata and processes of numerous neurons, and the peptide product was detected in the cerebrospinal fluid. During the 4-day life-span of the vector the incidence of cataplexy declined by 60%, and the levels of rapid eye movement sleep during the second half of the night were similar to levels in wild-type mice, indicating that narcoleptic sleep–wake behavior in orexin KO mice can be improved by targeted gene transfer. [ABSTRACT FROM AUTHOR]

Published

2008

12. Activation of the Notch pathway in Down syndrome: cross-talk of Notch and APP.

Author

Fischer, David F., Van Dijk, Renske, Sluijs, Jacqueline A., Nair, Suresh M., Racchi, Marco, Levelt, Christiaan N., Van Leeuwen, Fred W., and Hol, Elly M.

Subjects

DOWN syndrome, INTELLECTUAL disabilities, AMYLOID, ALZHEIMER'S disease, CEREBRAL cortex, GENE expression, NEURONS

Abstract

Down syndrome (DS) patients suffer from mental retardation, but also display enhanced β-APP production and develop cortical amyloid plaques at an early age. As β-APP and Notch are both processed by γ-secretase, we analyzed expression of the Notch signaling pathway in the adult DS brain and in a model system for DS, human trisomy 21 fibroblasts by quantitative PCR. In adult DS cortex we found that Notchl, Dll1 and Hes1 expression is up-regulated. Moreover, DS fibroblasts and Alzheimer disease cortex also show overexpression of Notchl and Dll1, indicating that enhanced β-APP processing found in both DS and AD could be instrumental in these changes. Using pull-down studies we could demonstrate interaction of APP with Notch 1, suggesting that these transmembrane proteins form heterodimers, but independent of γ-secretase. We could demonstrate binding of the intracellular domain of Notch1 to the APP adaptor protein Fe65. Furthermore, activated Notch1 can transactivate an APP target gene, Kail, and vice versa, activated APP can trans-activate the classical Notch target gene Hes1. These data suggest that Notch expression is activated in Down syndrome, possibly through cross-talk with APP signaling. This interaction might affect brain development, since the Notch pathway plays a pivotal role in neuron-glia differentiation. [ABSTRACT FROM AUTHOR]

Published

2005

13. The role of a-synuclein in the pathogenesis of multiple system atrophy.

Author

Wenning, Gregor K. and Jellinger, Kurt A.

Subjects

OLIGODENDROGLIA, NERVOUS system, NEURONS, PATHOLOGY, GENETICS, AXONS

Abstract

The discovery of glial cytoplasmic inclusions (GCIs) in 1989 helped to define multiple system atrophy (MSA) as a clinicopathological entity, and drew attention to the prominent role played by these inclusions in the pathogenesis of the disorder. Subsequently, GCIs were shown to be highly positive for a-synuclein, a neuronal protein that is normally absent in oligodendroglia except during embryonic development. The source of oligodendroglial a-synuclein aggregation in MSA is unknown. Since genetic overexpression has been excluded, active uptake from dying neurons remains a possibility. The similar topography of oligodendroglial and neuronal pathology in MSA suggests a fundamental disturbance of the functional unit between oligodendroglia, axon, and neuron. Transgenic MSA mouse models are now available to determine these aspects of cellular disturbance experimentally. [ABSTRACT FROM AUTHOR]

Published

2005

14. Expression of a Mutant SEMA3A Protein with Diminished Signalling Capacity Does Not Alter ALS-Related Motor Decline, or Confer Changes in NMJ Plasticity after BotoxA-Induced Paralysis of Male Gastrocnemic Muscle

Author

Barbara Hobo, Elizabeth B. Moloney, Fred De Winter, Joost Verhaagen, Molecular and Cellular Neurobiology, Amsterdam Neuroscience - Neurodegeneration, and Netherlands Institute for Neuroscience (NIN)

Subjects

0301 basic medicine, Male, Botulinum Toxins, Physiology, Motor nerve, lcsh:Medicine, Pathology and Laboratory Medicine, Inbred C57BL, Nervous System, Transgenic, Type A, Motor Neuron Diseases, Mice, Nerve Fibers, 0302 clinical medicine, Animal Cells, Mutant protein, Medicine and Health Sciences, Paralysis, Amyotrophic lateral sclerosis, Botulinum Toxins, Type A, lcsh:Science, Musculoskeletal System, Neurons, Mammals, Denervation, Motor Neurons, Multidisciplinary, Neuronal Plasticity, Muscles, Neurodegenerative Diseases, Neuromuscular Junctions, Anatomy, Cell biology, Electrophysiology, Mutant Strains, medicine.anatomical_structure, Neurology, Vertebrates, Female, Cellular Types, medicine.symptom, Research Article, Signal Transduction, Neuromuscular Junction, Neurophysiology, Mice, Transgenic, Biology, Rodents, Muscle Fibers, Neuromuscular junction, 03 medical and health sciences, Signs and Symptoms, SDG 3 - Good Health and Well-being, Diagnostic Medicine, medicine, Journal Article, Animals, Animal, lcsh:R, Amyotrophic Lateral Sclerosis, Organisms, Biology and Life Sciences, SEMA3A, Semaphorin-3A, Cell Biology, Motor neuron, medicine.disease, Mice, Mutant Strains, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, nervous system, Amino Acid Substitution, Cellular Neuroscience, Amniotes, Synapses, Disease Models, lcsh:Q, Mutant Proteins, Schwann Cells, 030217 neurology & neurosurgery, Neuroscience

Abstract

Terminal Schwann cells (TSCs) are specialized cells that envelop the motor nerve terminal, and play a role in the maintenance and regeneration of neuromuscular junctions (NMJs). The chemorepulsive protein semaphorin 3A (SEMA3A) is selectively up-regulated in TSCs on fast-fatigable muscle fibers following experimental denervation of the muscle (BotoxA-induced paralysis or crush injury to the sciatic nerve) or in the motor neuron disease amyotrophic lateral sclerosis (ALS). Re-expression of SEMA3A in this subset of TSCs is thought to play a role in the selective plasticity of nerve terminals as observed in ALS and following BotoxA-induced paralysis. Using a mouse model expressing a mutant SEMA3A with diminished signaling capacity, we studied the influence of SEMA3A signaling at the NMJ with two denervation paradigms; a motor neuron disease model (the G93A-hSOD1 ALS mouse line) and an injury model (BotoxA-induced paralysis). ALS mice that either expressed 1 or 2 mutant SEMA3A alleles demonstrated no difference in ALS-induced decline in motor behavior. We also investigated the effects of BotoxA-induced paralysis on the sprouting capacity of NMJs in the K108N-SEMA3A mutant mouse, and observed no change in the differential neuronal plasticity found at NMJs on fast-fatigable or slow muscle fibers due to the presence of the SEMA3A mutant protein. Our data may be explained by the residual repulsive activity of the mutant SEMA3A, or it may imply that SEMA3A alone is not a key component of the molecular signature affecting NMJ plasticity in ALS or BotoxA-induced paralysis. Interestingly, we did observe a sex difference in motor neuron sprouting behavior after BotoxA-induced paralysis in WT mice which we speculate may be an important factor in the sex dimorphic differences seen in ALS.

Published

2017

15. Introduction aux réseaux neuronaux

Author

Leuba, Neirynck, Savioz, Vallet, Walzer, Leuba, Neirynck, Savioz, Vallet, and Walzer

Subjects

Cognitive neuroscience, Synapses, Neuropsychology, Neural networks (Neurobiology), Nervous system--Diseases, Neural circuitry, Neurons, Neurobiology

Abstract

Aujourd'hui, les neurosciences et les sciences cognitives se rejoignent pour comprendre les liens existant entre, d'une part, le fonctionnement neuronal, cellulaire et moléculaire, et d'autre part, l'individu psycho-social. Les réseaux neuronaux forment un niveau intermédiaire, constituant l'un des derniers territoires à explorer, no man's land entre éléments plastiques du système nerveux et facultés cognitives, émotionnelles et comportementales. Le développement des connaissances sur les réseaux neuronaux biologiques et artificiels comblera petit à petit cet espace.Rédigé dans un langage clair et compréhensible, cet ouvrage propose une introduction aux réseaux neuronaux, en développant progressivement la manière dont ces derniers permettent de relier la synapse à la psyché. Il expose également, à l'instar de la maladie d'Alzheimer, comment une telle vision'synapto-connexionniste'permet d'analyser les liens entre différents niveaux d'organisation lors de phénomènes de dégénerescence.Introduction aux réseaux neuronaux offrira au lecteur intéressé une connaissance de base en neurosciences et en biologie des réseaux neuronaux autant qu'une vision transdisciplinaire. Il apportera des informations précises, mais également des pistes de réflexion.

Published

2010