Your search keyword '"Neuronal Outgrowth"' showing total 1,507 results

51. Re-exploration of tetrahydro-β-carboline scaffold: Discovery of selective histone deacetylase 6 inhibitors with neurite outgrowth-promoting and neuroprotective activities.

Author

Wen W, Hu J, Wang C, Yang R, Zhang Y, Huang B, Qiao T, Wang J, and Chen X

Subjects

Rats, Animals, Histone Deacetylase 6, Hydroxamic Acids pharmacology, Neuronal Outgrowth, Histone Deacetylase 1 metabolism, Structure-Activity Relationship, Histone Deacetylase Inhibitors pharmacology, Hydrogen Peroxide pharmacology, Carbolines

Abstract

Histone deacetylase 6 (HDAC6) has drawn more and more attention for its potential application in Alzheimer's disease (AD) therapy. A series of tetrahydro-β-carboline (THβC) hydroxamic acids with aryl linker were synthesized. In enzymatic assay, all compounds exhibited nanomolar IC 50 values. The most promising compound 11d preferentially inhibited HDAC6 (IC 50 , 8.64 nM) with approximately 149-fold selectivity over HDAC1. Molecular simulation revealed that the hydroxamic acid of 11d could bind to the zinc ion by a bidentate chelating manner. In vitro, 11d induced neurite outgrowth of PC12 cells without producing toxic effects and showed obvious neuroprotective activity in a model of H 2 O 2 -induced oxidative stress., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

52. High-Throughput Neurite Outgrowth Assay Using GFP-Labeled iPSC-Derived Neurons

Author

Li Zhang, Shuaizhang Li, and Menghang Xia

Subjects

Neurons, Medical Laboratory Technology, General Immunology and Microbiology, General Neuroscience, Green Fluorescent Proteins, Induced Pluripotent Stem Cells, Neuronal Outgrowth, Humans, Health Informatics, Neurotoxicity Syndromes, General Pharmacology, Toxicology and Pharmaceutics, General Biochemistry, Genetics and Molecular Biology, High-Throughput Screening Assays

Abstract

The potential neurotoxicity from an increasing number of drugs and untested environmental chemicals creates a need to develop reliable and efficient in vitro methods for identifying chemicals that may adversely affect the nervous system. An important process in neurodevelopment is neurite outgrowth, which can be affected by developmental neurotoxicity. Currently, neurite outgrowth assays rely mainly on staining, which requires multiple sample processing steps, particularly washing steps, that may introduce variation and limit throughput. Here, we describe a neurite outgrowth assay that uses induced pluripotent stem cell (iPSC)-derived human cortical glutamatergic neurons and/or spinal motor neurons labeled with green fluorescent protein (GFP) to test compounds in a high-content and high-throughput format. This method enables live and time-lapse imaging of GFP-labeled neurons using an assay plate that is continuously imaged at multiple times after chemical treatment. In this article, we describe how to thaw frozen GFP-labeled neurons, culture them, treat them with a compound of interest, and analyze neurite outgrowth using a high-content imaging platform. In this assay, GFP-labeled iPSC-derived human neurons represent a promising tool for identifying and prioritizing compounds with potential developmental neurotoxicity for further hazard characterization. © 2022 The Authors. Current Protocols published by Wiley Periodicals LLC. This article has been contributed to by U.S. Government employees and their work is in the public domain in the USA. Basic Protocol 1: Thawing and seeding of iPSC-derived neurons Basic Protocol 2: Compound plate preparation and treatment of neurons Basic Protocol 3: High-content imaging and analysis.

Published

2023

53. Exploring the therapeutic potential of neuropeptides in neurodegenerative disease (NDD): A review

Author

Kaur, Ramneek, Singh, Manisha, and Rachana

Published

2016

54. Neurotrophic Proteins in Dentin and Their Effect on Trigeminal Sensory Neurons.

Author

Widbiller, Matthias, Austah, Obadah, Lindner, Sophia R., Sun, Jenny, and Diogenes, Anibal

Subjects

NEUROTROPHINS, GLIAL cell line-derived neurotrophic factor, SENSORY neurons, BRAIN-derived neurotrophic factor, DENTIN, TRP channels

Abstract

A plethora of bioactive molecules present during tooth formation become sequestered in the mineralized dentin matrix and can be released into the pulp tissue after demineralization from carious lesions. However, neurotrophic factors are differentially expressed and secreted during various stages of odontogenesis. Thus, the aims of this study were (1) to investigate their presence and relative abundance in crown and root dentin and (2) to evaluate the bioactivity of dentin-derived proteins on neuronal cells. Dentin matrix proteins (DMPs) were isolated from matched roots and crowns of extracted healthy human third molars. The total protein amount as well as the concentration of growth factors and neurotrophic proteins were quantified. The impact on neuritogenesis was determined with mouse trigeminal neurons in vitro and by a hydrogel implant model in vivo. Transient receptor potential cation channel subfamily V member 1 (TRPV1) sensitization of DMP-conditioned neurons was evaluated by single-cell calcium imaging. The relative concentration of neurotrophic molecules revealed that nerve growth factor is the most abundant neurotrophin with 3-fold increased expression in radicular dentin. Similarly, brain-derived neurotrophic factor and neurotrophin 3 are more abundant in radicular than coronal dentin. Conversely, glial cell line–derived neurotrophic factor is more abundant in coronal dentin, whereas neurotrophin 4 is equally distributed. Dentin matrix proteins promoted neurite outgrowth in vitro and axonal targeting in vivo , with a greater effect observed by radicular dentin extracts. Furthermore, DMPs sensitized TRPV1 responses in mouse trigeminal neurons with greater activity seen with extracts from root dentin. Neurotrophic factors are differentially distributed between coronal and radicular dentin with different effects of dentin-derived proteins on axonal growth and targeting as well as the sensitization of TRPV1. Thus, extracellular proteins from the dentin matrix are likely involved in neurogenic responses to caries and could be exploited in clinical regenerative endodontics to promote reinnervation and enhance tissue regeneration. • Dentin matrix contains neurotrophic proteins with higher concentrations in roots. • Proteins of mineralized dentin matrix promote neuritogenesis and axonal growth. • Dentin matrix proteins sensitize TRPV1 response in trigeminal neurons. [ABSTRACT FROM AUTHOR]

Published

2019

55. Tuftelin Is Required for NGF-Induced Differentiation of PC12 Cells.

Author

Shilo, Dekel, Cohen, Gadi, Blumenfeld, Anat, Goren, Koby, Hanhan, Salem, Sharon, Shay, Haze, Amir, Deutsch, Dan, and Lazarovici, Philip

Abstract

Nerve growth factor (NGF) promotes pleiotropic gene transcription-dependent biological effects, in neuronal and non-neuronal cells, including survival, proliferation, differentiation, neuroprotection, pain, and angiogenesis. It is hypothesized that during odontogenesis, NGF may be implicated in morphogenetic and mineralization events by affecting proliferation and/or differentiation of dental cells. Tuftelin belongs to the enamel associated teeth proteins and is thought to play a role in enamel mineralization. We previously reported that tuftelin transcript and protein, which are ubiquitously expressed in various tissues of embryos, adults, and tumors, were significantly upregulated during NGF-induced PC12 differentiation. To further confirm the involvement of tuftelin in the differentiation process, we established a tuftelin-knockdown neuronal PC12 cell model, using a non-cytotoxic siRNA directed towards sequences at the 3′ UTR of the tuftelin gene. Using real-time PCR, we quantified tuftelin mRNA expression and found that tuftelin siRNA, but not scrambled siRNA or transfection reagents, efficiently depleted about 60% of NGF-induced tuftelin mRNA transcripts. The effect of tuftelin siRNA was quantified up to 6 days of NGF-induced differentiation. Using immunofluorescence and western blot analyses, we also found a direct correlation between reduction of 60–80% in tuftelin protein expression and inhibition of about 50–70% in NGF-induced differentiation of the cells, as was detected after 3–6 days of treatment. These results demonstrate an important role for tuftelin in NGF-induced differentiation of PC12 cells. Tuftelin could be a useful target for drug development in disease where neurotrophin therapy is required. [ABSTRACT FROM AUTHOR]

Published

2019

56. Cocultured Schwann Cells Rescue Irradiated Pelvic Neuron Outgrowth and Increase Survival

Author

Joshua T, Randolph, Elena S, Pak, Jennifer C, McMains, Bridget F, Koontz, and Johanna L, Hannan

Subjects

Male, Tyrosine 3-Monooxygenase, Urology, Endocrinology, Diabetes and Metabolism, Neuronal Outgrowth, Coculture Techniques, Rats, Rats, Sprague-Dawley, Psychiatry and Mental health, Endocrinology, Reproductive Medicine, Nitrergic Neurons, Animals, Humans, Schwann Cells, Cells, Cultured

Abstract

BackgroundProstatic radiation therapy (RT) leads to erectile dysfunction by damaging peri-prostatic pro-erectile nerves of the pelvic ganglion. Schwann cells (SC) facilitate neuronal repair after mechanical injury, however, their role in repair of pelvic neurons post-radiation hasn’t been explored.AimTo determine if SCs cocultured with primary pelvic neurons can rescue neuronal survival and growth after ex vivo RT.MethodsMajor pelvic ganglia (MPG) were collected from adult male Sprague-Dawley rats (n = 12) to isolate SCs. SCs received RT (0 or 8 Gy), were plated on coated coverslips and grown to confluence before the addition of neurons. Additional MPGs were irradiated (0 or 8 Gy) and digested to isolate pelvic neurons. Dissociated neurons were plated alone or atop SC-coated coverslips to create 6 experimental groups (n = 3/grp): (i) Control (CON) MPG, (ii) RT MPG, (iii) CON SC + CON MPG, (iv) CONSC + RT MPG, (v) RT SC + CON MPG, and (iv) RT SC + RT MPG. After 72 hours, coverslips were fixed and stained for beta-tubulin (neuron marker), S100 (SC marker), neuronal nitric oxide synthase (nitrergic marker), tyrosine hydroxylase (sympathetic marker), and terminal deoxynucleotidyl transferase dUTP nick-end labeling.OutcomesWe measured neurite length, branching, specific neuron populations and apoptosis.ResultsEx vivo RT decreased MPG neuron length, increased apoptosis and decreased nitrergic neurons in monoculture. Compared to all other groups, CON SC + RT MPG cocultures demonstrated increased neurite outgrowth (P < .001). Neurite branching was decreased in the RT MPG + RT SC coculture, but unchanged in other cocultures. Groups containing RT MPG neurons exhibited increased apoptosis, but coculture with CON SC reduced the degree of RT-induced apoptosis (P < .01). The number of tyrosine hydroxylase positive neurons was unchanged while nitrergic neurons were significantly lower in RT neurons and coculture with CON SCs was unable to prevent nitrergic loss.Clinical TranslationThese findings suggest that SCs may be an important target in prostate cancer patients with radiation-induced pelvic neuropathy to promote MPG neuron survival and neuronal repair after RT.Strengths and LimitationsThis is the first study to characterize the ex vivo ability of SCs to rescue pelvic nerve growth and survival. The study is limited by little supporting mechanistic molecular data and the need to confirm the ability of healthy SCs to promote pelvic neuron survival and repair following prostatic RT in vivo.ConclusionUnirradiated SCs partially mitigated RT-induced MPG apoptosis but did not affect the loss of nitrergic neuron populations suggesting that SCs promote irradiated MPG neuron survival and facilitate intrinsic repair functions.

Published

2022

57. Promoting Neuronal Outgrowth Using Ridged Scaffolds Coated with Extracellular Matrix Proteins

Author

Ahad M. Siddiqui, Rosa Brunner, Gregory M. Harris, Alan Lee Miller, Brian E. Waletzki, Ann M. Schmeichel, Jean E. Schwarzbauer, Jeffrey Schwartz, Michael J. Yaszemski, Anthony J. Windebank, and Nicolas N. Madigan

Subjects

neuronal outgrowth, cell attachment, Schwann cells, extracellular matrix, scaffolds, spinal cord, Biology (General), QH301-705.5

Abstract

Spinal cord injury (SCI) results in cell death, demyelination, and axonal loss. The spinal cord has a limited ability to regenerate, and current clinical therapies for SCI are not effective in helping promote neurologic recovery. We have developed a novel scaffold biomaterial that is fabricated from the biodegradable hydrogel oligo(poly(ethylene glycol)fumarate) (OPF). We have previously shown that positively charged OPF scaffolds (OPF+) in an open spaced, multichannel design can be loaded with Schwann cells to support axonal generation and functional recovery following SCI. We have now developed a hybrid OPF+ biomaterial that increases the surface area available for cell attachment and that contains an aligned microarchitecture and extracellular matrix (ECM) proteins to better support axonal regeneration. OPF+ was fabricated as 0.08 mm thick sheets containing 100 μm high polymer ridges that self-assemble into a spiral shape when hydrated. Laminin, fibronectin, or collagen I coating promoted neuron attachment and axonal outgrowth on the scaffold surface. In addition, the ridges aligned axons in a longitudinal bipolar orientation. Decreasing the space between the ridges increased the number of cells and neurites aligned in the direction of the ridge. Schwann cells seeded on laminin coated OPF+ sheets aligned along the ridges over a 6-day period and could myelinate dorsal root ganglion neurons over 4 weeks. This novel scaffold design, with closer spaced ridges and Schwann cells, is a novel biomaterial construct to promote regeneration after SCI.

Published

2021

58. eEF1A2 knockdown impairs neuronal proliferation and inhibits neurite outgrowth of differentiating neurons

Author

Kanitin Rumpansuwon, Athinan Prommahom, and Permphan Dharmasaroja

Subjects

Neurons, 1-Methyl-4-phenylpyridinium, Tyrosine 3-Monooxygenase, Caspase 3, General Neuroscience, Neuronal Outgrowth, Cell Differentiation, Tretinoin, Neuroblastoma, Ki-67 Antigen, Peptide Elongation Factor 1, Cell Line, Tumor, Humans, Cell Proliferation

Abstract

The translation elongation factor-1, alpha-2 (eEF1A2) plays an important role in protein synthesis. Mutations in this gene have been described in individuals with neurodevelopmental disorders. Here, we silenced the expression of eEFA2 in human SH-SY5Y neuroblastoma cells and observed its roles in neuronal proliferation and differentiation upon induction with retinoic acid.eEF1A2 were silenced using siRNA transfection. Cell proliferation was qualitatively evaluated by Ki-67 immunocytochemistry. Neuronal differentiation was induced with retinoic acid for 3, 5, 7 and 10 days. Neurite length was measured. The expression of microtubule-associated protein 2 (MAP2) was analyzed by western blotting. Tyrosine hydroxylase expression was visualized by immunofluorescence. Cytotoxicity to a neurotoxin, 1-methyl-4-phenylpyridinium (MPP+), was assessed by the 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl-2H-tetrazolium bromide (MTT) assay and western blotting of cleaved caspase-3.eEF1A2 knockdown suppressed the proliferative activity of undifferentiated SH-SY5Y cells as shown by decreased Ki-67 immunostaining. Upon retinoic acid-induction, differentiated neurons with eEF1A2 knockdown exhibited shorter neurite length than untransfected cells, which was associated with the reduction of tyrosine hydroxylase and suppression of MAP2 at 10 days of differentiation. eEF1A2 knockdown decreased the survival of neurons, which was clearly observed in undifferentiated and short-term differentiated cells. Upon treatment with MPP+, cells with eEF1A2 knockdown showed a further reduction in cell survival and an increase of cleaved caspase-3 protein.Our results suggest that eEF1A2 may be required for neuronal proliferation and differentiation of SH-SY5Y cells. Increased cell death susceptibility against MPP+ in eEF1A2-knockdown neurons may imply the neuroprotective role of eEF1A2.

Published

2022

59. Mllt11 Regulates Migration and Neurite Outgrowth of Cortical Projection Neurons during Development

Author

Danielle Stanton-Turcotte, Karolynn Hsu, Samantha A. Moore, Makiko Yamada, James P. Fawcett, and Angelo Iulianella

Subjects

Cerebral Cortex, Male, Neurons, Proteomics, General Neuroscience, Neuronal Outgrowth, Neocortex, Axons, Corpus Callosum, Mice, Proto-Oncogene Proteins, Neural Pathways, Animals, Female

Abstract

The formation of connections within the mammalian neocortex is highly regulated by both extracellular guidance mechanisms and intrinsic gene expression programs. There are two types of cortical projection neurons (CPNs): those that project locally and interhemispherically and those that project to subcerebral structures such as the thalamus, hindbrain, and spinal cord. The regulation of cortical projection morphologies is not yet fully understood at the molecular level. Here, we report a role for Mllt11 (Myeloid/lymphoid or mixed-lineage leukemia; translocated to chromosome 11/All1 Fused Gene From Chromosome 1q) in the migration and neurite outgrowth of callosal projection neurons during mouse brain formation. We show thatMllt11expression is exclusive to developing neurons and is enriched in the developing cortical plate (CP) during the formation of the superficial cortical layers. In cultured primary cortical neurons, Mllt11 is detected in varicosities and growth cones as well as the soma. Using conditional loss-of-function and gain-of-function analysis we show that Mllt11 is required for neuritogenesis and proper migration of upper layer CPNs. Loss ofMllt11in the superficial cortex of male and female neonates leads to a severe reduction in fibers crossing the corpus callosum (CC), a progressive loss in the maintenance of upper layer projection neuron gene expression, and reduced complexity of dendritic arborization. Proteomic analysis revealed that Mllt11 associates with stabilized microtubules, andMllt11loss affected microtubule staining in callosal axons. Taken together, our findings support a role for Mllt11 in promoting the formation of mature upper-layer neuron morphologies and connectivity in the cerebral cortex.SIGNIFICANCE STATEMENTThe regulation of cortical projection neuron (CPN) morphologies is an area of active investigation since the time of Cajal. Yet the molecular mechanisms of how the complex dendritic and axonal morphologies of projection neurons are formed remains incompletely understood. Although conditional mutagenesis analysis in the mouse, coupled with overexpression assays in the developing fetal brain, we show that a novel protein called Mllt11 is sufficient and necessary to regulate the dendritic and axonal characteristics of callosal projection neurons in the developing mammalian neocortex. Furthermore, we show that Mllt11 interacts with microtubules, likely accounting for its role in neuritogenesis.

Published

2022

60. <scp>BET</scp> protein inhibition in macrophages enhances dorsal root ganglion neurite outgrowth in female mice

Author

Georgina Palomés‐Borrajo, Xavier Navarro, and Clara Penas

Subjects

Inflammation, Macrophages, Neurite outgrowth, Neuronal Outgrowth, chemical and pharmacologic phenomena, hemic and immune systems, Nerve Regeneration, Crush Injuries, Mice, Cellular and Molecular Neuroscience, nervous system, Culture Media, Conditioned, Ganglia, Spinal, Neurites, BET proteins, Cytokines, Regeneration, Animals, Female, Cells, Cultured

Abstract

Altres ajuts: acords transformatius de la UAB Peripheral nerve regeneration is limited after injury, especially in humans, due to the large distance the axons have to grow in the limbs. This process is highly dependent on the expression of neuroinflammatory factors produced by macrophages and glial cells. Given the importance of the epigenetic BET proteins on inflammation, we aimed to ascertain if BET inhibition may have an effect on axonal outgrowth. For this purpose, we treated female mice with JQ1 or vehicle after sciatic nerve crush injury and analyzed target reinnervation. We also used dorsal root ganglion (DRG) culture explants to analyze the effects of direct BET inhibition or treatment with conditioned medium from BET-inhibited macrophages. We observed that although JQ1 produced an enhancement of IL-4, IL-13, and GAP43 expression, it did not have an effect on sensory or motor reinnervation after crush injury in vivo. In contrast, JQ1 reduced neurite growth when interacting directly with DRG neurons ex vivo, whereas conditioned medium from JQ1-treated macrophages promoted neurite outgrowth. Therefore, BET-inhibited macrophages secrete pro-regenerative factors that induce neurite outgrowth, and that may counteract the direct inhibition of BET proteins in neurons in vivo. Finally, we observed an activation of the STAT6 pathway in DRG explants treated with conditioned medium from JQ1-treated macrophages. In conclusion, this study demonstrates that BET protein inhibition in macrophages provides a mechanism to enhance axonal outgrowth. However, specific targeting of BET proteins to macrophages will be needed to efficiently enhance functional recovery after nerve injury.

Published

2022

61. Photoacoustic Carbon Nanotubes Embedded Silk Scaffolds for Neural Stimulation and Regeneration

Author

Nan Zheng, Vincent Fitzpatrick, Ran Cheng, Linli Shi, David L. Kaplan, and Chen Yang

Subjects

Tissue Engineering, Tissue Scaffolds, Nanotubes, Carbon, Neuronal Outgrowth, Silk, General Engineering, Animals, General Physics and Astronomy, General Materials Science, Fibroins, Rats

Abstract

Neural interfaces using biocompatible scaffolds provide crucial properties, such as cell adhesion, structural support, and mass transport, for the functional repair of nerve injuries and neurodegenerative diseases. Neural stimulation has also been found to be effective in promoting neural regeneration. This work provides a generalized strategy to integrate photoacoustic (PA) neural stimulation into hydrogel scaffolds using a nanocomposite hydrogel approach. Specifically, polyethylene glycol (PEG)-functionalized carbon nanotubes (CNT), highly efficient photoacoustic agents, are embedded into silk fibroin to form biocompatible and soft photoacoustic materials. We show that these photoacoustic functional scaffolds enable nongenetic activation of neurons with a spatial precision defined by the area of light illumination, promoting neuron regeneration. These CNT/silk scaffolds offered reliable and repeatable photoacoustic neural stimulation, and 94% of photoacoustic-stimulated neurons exhibit a fluorescence change larger than 10% in calcium imaging in the light-illuminated area. The on-demand photoacoustic stimulation increased neurite outgrowth by 1.74-fold in a rat dorsal root ganglion model, when compared to the unstimulated group. We also confirmed that promoted neurite outgrowth by photoacoustic stimulation is associated with an increased concentration of neurotrophic factor (BDNF). As a multifunctional neural scaffold, CNT/silk scaffolds demonstrated nongenetic PA neural stimulation functions and promoted neurite outgrowth, providing an additional method for nonpharmacological neural regeneration.

Published

2022

62. Nematic Templated Complex Nanofiber Structures by Projection Display

Author

Juan Chen, Oluwafemi Isaac Akomolafe, Netra Prasad Dhakal, Mahesh Pujyam, Omar Skalli, Jinghua Jiang, and Chenhui Peng

Subjects

Neurons, Mice, Cell Survival, Neuronal Outgrowth, Nanofibers, Animals, Biocompatible Materials, General Materials Science, Azo Compounds, Cell Line, Liquid Crystals, Nerve Regeneration

Abstract

Oriented arrays of nanofibers are ubiquitous in nature and have been widely used in recreation of the biological functions such as bone and muscle tissue regenerations. However, it remains a challenge to produce nanofiber arrays with a complex organization by using current fabrication techniques such as electrospinning and extrusion. In this work, we propose a method to fabricate the complex organization of nanofiber structures templated by a spatially varying ordered liquid crystal host, which follows the pattern produced by a maskless projection display system. By programming the synchronization of the rotated polarizer and projected segments with different shapes, various configurations of nanofiber organization ranging from a single to two-dimensional lattice of arbitrary topological defects are created in a deterministic manner. The nanofiber arrays can effectively guide and promote neurite outgrowth. The application of nanofibers with arced profiles and topological defects on neural tissue organization is also demonstrated. This finding, combined with the versatility and programmability of nanofiber structures, suggests that they will help solve challenges in nerve repair, neural regeneration, and other related tissue engineering fields.

Published

2022

63. Regulatory effects of nicotine on neurite outgrowth in rat superior cervical ganglia cells

Author

Hiromu Kawasaki, Toshiaki Sendou, Fusako Takayama, Hayato Hino, Yoshihisa Kitamura, and Shingo Takatori

Subjects

Nicotine, medicine.medical_specialty, Nicotinic acetylcholine receptors, alpha7 Nicotinic Acetylcholine Receptor, Neurite, Neuronal Outgrowth, RM1-950, Superior Cervical Ganglion, chemistry.chemical_compound, Internal medicine, Neurites, medicine, Rat superior cervical ganglia cells, Animals, Nerve Growth Factors, Cells, Cultured, Pharmacology, Control level, biology, Tyrosine hydroxylase, Neurite outgrowth, Antagonist, Rats, medicine.anatomical_structure, Endocrinology, chemistry, Cervical ganglia, biology.protein, Molecular Medicine, Hexamethonium, Therapeutics. Pharmacology, Neurotrophin, medicine.drug

Abstract

We have reported that nicotine has a neurotrophic action on peripheral adrenergic nerves in vivo, which is mediated by α7 nicotinic acetylcholine receptors (nAChRs). To clarify the possible mechanisms, the present study further investigated the effect of nicotine on neurite outgrowth in tyrosine hydroxylase (TH)-positive superior cervical ganglia (SCG) cells isolated from neonatal rats in vitro. Nicotine at low concentrations (0.01–0.3 mM) increased the number of neurite outgrowths in TH-immunopositive SCG cells, while high concentrations of nicotine (1–10 mM) gradually reduced it, and only 10 mM nicotine was markedly inhibited compared to the control. A 100 μM of nicotine-induced increase in neurite numbers depended on the exposure time and was inhibited by treatment with the nAChR antagonist hexamethonium (Hex) and α7 nAChR antagonist α-bungarotoxin (α-Bgtx). The nicotine (10 mM)-induced a significant decrease in neurite outgrowth in SCG, which was perfectly canceled by Hex to the control level but not by α-Bgtx. These results suggest that nicotine has a regulatory neurotrophic action mediated by both α7 nAChR and other subtypes in TH-positive SCG cells of rats.

Published

2022

64. Repeated administration of acrylamide for 28 days reduces late-stage progenitor cells and immature granule cells accompanying impaired neurite outgrowth in the adult hippocampal neurogenesis in young-adult rats

Author

Bunichiro, Ogawa, Yutaka, Nakanishi, Masaki, Wakamatsu, Yasunori, Takahashi, and Makoto, Shibutani

Subjects

Male, Doublecortin Domain Proteins, Acrylamide, Neural Stem Cells, Neurogenesis, Neuronal Outgrowth, Animals, Apoptosis, Toxicology, Hippocampus, Rats

Abstract

Acrylamide (AA) is a neurotoxicant that causes synaptic impairment in distal axons. We previously found that developmental exposure to AA decreased proliferation of late-stage neural progenitor cells (NPCs) in the hippocampal neurogenesis of the dentate gyrus (DG) in rats. To investigate whether hippocampal neurogenesis is similarly affected by AA exposure in a general toxicity study, AA was administered to 7-week-old male rats via oral gavage at dosages of 0, 5, 10, and 20 mg/kg for 28 days. In the subgranular zone (SGZ) and granule cell layer, AA decreased the densities of doublecortin-positive

Published

2022

65. Advanced Hollow Cathode Discharge Plasma Treatment of Unique Bilayered Fibrous Nerve Guidance Conduits for Enhanced/Oriented Neurite Outgrowth.

Author

Aliakbarshirazi S, Ghobeira R, Asadian M, Narimisa M, Nikiforov A, De Baere I, Van Paepegem W, De Geyter N, Declercq H, and Morent R

Subjects

Rats, Animals, Tissue Engineering methods, Nerve Regeneration, Neuronal Outgrowth, Tissue Scaffolds chemistry, Neurites physiology

Abstract

Despite all recent progresses in nerve tissue engineering, critical-sized nerve defects are still extremely challenging to repair. Therefore, this study targets the bridging of critical nerve defects and promoting an oriented neuronal outgrowth by engineering innovative nerve guidance conduits (NGCs) synergistically possessing exclusive topographical, chemical, and mechanical cues. To do so, a mechanically adequate mixture of polycaprolactone (PCL) and polylactic- co -glycolic acid (PLGA) was first carefully selected as base material to electrospin nanofibrous NGCs simulating the extracellular matrix. The electrospinning process was performed using a newly designed 2-pole air gap collector that leads to a one-step deposition of seamless NGCs having a bilayered architecture with an inner wall composed of highly aligned fibers and an outer wall consisting of randomly oriented fibers. This architecture is envisaged to afford guidance cues for the extension of long neurites on the underlying inner fiber alignment and to concurrently provide a sufficient nutrient supply through the pores of the outer random fibers. The surface chemistry of the NGCs was then modified making use of a hollow cathode discharge (HCD) plasma reactor purposely designed to allow an effective penetration of the reactive species into the NGCs to eventually treat their inner wall. X-ray photoelectron spectroscopy (XPS) results have indeed revealed a successful O 2 plasma modification of the inner wall that exhibited a significantly increased oxygen content (24 → 28%), which led to an enhanced surface wettability. The treatment increased the surface nanoroughness of the fibers forming the NGCs as a result of an etching effect. This effect reduced the ultimate tensile strength of the NGCs while preserving their high flexibility. Finally, pheochromocytoma (PC12) cells were cultured on the NGCs to monitor their ability to extend neurites which is the base of a good nerve regeneration. In addition to remarkably improved cell adhesion and proliferation on the plasma-treated NGCs, an outstanding neural differentiation occurred. In fact, PC12 cells seeded on the treated samples extended numerous long neurites eventually establishing a neural network-like morphology with an overall neurite direction following the alignment of the underlying fibers. Overall, PCL/PLGA NGCs electrospun using the 2-pole air gap collector and O 2 plasma-treated using an HCD reactor are promising candidates toward a full repair of critical nerve damage.

Published

2024

66. Herpes simplex virus type 1 modifies the protein composition of extracellular vesicles to promote neurite outgrowth and neuroinfection.

Author

Sun G, Kropp KA, Kirchner M, Plückebaum N, Selich A, Serrero M, Dhingra A, Cabrera JR, Ritter B, Bauerfeind R, Wyler E, Landthaler M, Schambach A, Sodeik B, Mertins P, and Viejo-Borbolla A

Subjects

Humans, Galectin 1 metabolism, Neuronal Outgrowth, Glycoproteins metabolism, Herpesvirus 1, Human physiology, Herpes Simplex, Communicable Diseases, Extracellular Vesicles metabolism

Abstract

The highly prevalent herpes simplex virus type 1 (HSV-1) causes a range of diseases, including cold sores, blinding keratitis, and life-threatening encephalitis. HSV-1 initially replicates in epithelial cells, enters the peripheral nervous system via neurites, and establishes lifelong infection in the neuronal cell bodies. Neurites are highly dynamic structures that grow or retract in response to attractive or repulsive cues, respectively. Here, we show that infection with HSV-1, but not with a mutant virus lacking glycoprotein G (gG), reduced the repulsive effect of epithelial cells on neurite outgrowth and facilitated HSV-1 invasion of neurons. HSV-1 gG was required and sufficient to induce neurite outgrowth by modifying the protein composition of extracellular vesicles, increasing the amount of neurotrophic and neuroprotective proteins, including galectin-1. Antibodies directed against galectin-1 neutralized the capacity of extracellular vesicles released from HSV-1-infected cells to promote neurite outgrowth. Our study provides new insights into the neurotropism of HSV-1 and identifies a viral protein that modifies the protein composition of extracellular vesicles to stimulate neurite outgrowth and invasion of the nervous system.IMPORTANCEHerpes simplex virus type 1 (HSV-1) must infect neurites (or nerve endings) to establish a chronic infection in neurons. Neurites are highly dynamic structures that retract or grow in the presence of repulsive or attractive proteins. Some of these proteins are released by epithelial cells in extracellular vesicles and act upon interaction with their receptor present on neurites. We show here that HSV-1 infection of epithelial cells modulated their effect on neurites, increasing neurite growth. Mechanistically, HSV-1 glycoprotein G (gG) modifies the protein composition of extracellular vesicles released by epithelial cells, increasing the amount of attractive proteins that enhance neurite outgrowth and facilitate neuronal infection. These results could inform of therapeutic strategies to block HSV-1 induction of neurite outgrowth and, thereby, neuronal infection., Competing Interests: The authors declare no conflict of interest.

Published

2024

67. Type I collagen concentration affects neurite outgrowth of adult rat DRG explants by altering mechanical properties of hydrogels.

Author

Nguyen UN, Lee FS, Caparaso SM, Leoni JT, Redwine AL, and Wachs RA

Subjects

Rats, Animals, Ganglia, Spinal, Neurites physiology, Collagen pharmacology, Neuronal Outgrowth, Cells, Cultured, Collagen Type I, Hydrogels pharmacology

Abstract

Type I collagen is a predominant fibrous protein that makes up the extracellular matrix. Collagen enhances cell attachment and is commonly used in three-dimensional culture systems, to mimic the native extracellular environment, for primary sensory neurons such as dorsal root ganglia (DRG). However, the effects of collagen concentration on adult rat DRG neurite growth have not been assessed in a physiologically relevant, three-dimensional culture. This study focuses on the effects of type I collagen used in a methacrylated hyaluronic acid (MAHA)-laminin-collagen gel (triple gel) on primary adult rat DRG explants in vitro . DRGs were cultured in triple gels, and the neurite lengths and number of support cells were quantified. Increased collagen concentration significantly reduced neurite length but did not affect support cell counts. Mechanical properties, fiber diameter, diffusivity, and mesh size of the triple gels with varying collagen concentration were characterized to further understand the effects of type I collagen on hydrogel property that may affect adult rat DRG explants. Gel stiffness significantly increased as collagen concentration increased and is correlated to DRG neurite length. Collagen concentration also significantly impacted fiber diameter but there was no correlation with DRG neurite length. Increasing collagen concentration had no significant effect on mesh size and diffusivity of the hydrogel. These data suggest that increasing type I collagen minimizes adult rat DRG explant growth in vitro while raising gel stiffness. This knowledge can help develop more robust 3D culture platforms to study sensory neuron growth and design biomaterials for nerve regeneration applications.

Published

2024

68. The PTB and PRR domains of numb regulate neurite outgrowth by influencing voltage-gated calcium channel expression and kinetics.

Author

Wang G, Zhang Z, Li J, Han J, and Lu C

Subjects

Rats, Animals, Calcium Channels genetics, Protein Isoforms genetics, Protein Isoforms metabolism, Protein Isoforms pharmacology, Neuronal Outgrowth, Calcium metabolism, Intracellular Signaling Peptides and Proteins metabolism, Membrane Proteins genetics, Membrane Proteins metabolism, Neurons metabolism

Abstract

Numb is an evolutionarily conserved protein that regulates the differentiation of neuronal progenitor cells through unknown mechanisms. Numb has four alternative splice variants with different lengths of phosphotyrosine-binding (PTB) and proline-rich regions (PRR) domains. In this study, we demonstrated that Numb expression was increased in the primary cultures of rat cortical and hippocampal neurons over time in vitro, and Numb antisense inhibited neurite outgrowth. We verified that cells overexpressing short PTB (SPTB) or long PTB (LPTB) domains exhibited differentiation or proliferation, respectively. SPTB-mediated differentiation was related to the PRR domains, as cells expressing SPTB/LPRR had longer dendrites and more branched dendrites than cells expressing SPTB/SPRR. The differentiation of both cell types was completely blocked by the Ca 2+ chelator. Western blot analysis revealed the increased total protein expression of voltage-gated calcium channel (VGCC) subunit α1C and α1D in cells expressing SPTB and LPTB Numb. The increased expression of the VGCC β3 subunit was only observed in cells expressing SPTB Numb. Immunocytochemistry further showed that SPTB-mediated cell differentiation was associated with increased membrane expression of VGCC subunits α1C, α1D and β3, which corresponded to the higher Ca 2+ current (ICa) densities. Furthermore, we found that VGCC of cells transfected with SPTB/SPRR or SPTB/LPRR Numb isoforms exhibit steady-state inactivation (SSI) in both differentiated and undifferentiated phenotypes. A similar SSI of VGCC was observed in the differentiated cells transfected with SPTB/SPRR or SPTB/LPRR Numb isoforms, whereas a left shift SSI of VGCC in cells expressing SPTB/LPRR was detected in the undifferentiated cells. Collectively, these data indicate that SPTB domain is essential for neurite outgrowth involving in membrane expression of VGCC subunits, and LPRR plays a role in neuronal branching and the regulation of VGCC inactivation kinetics., Competing Interests: Declaration of Competing Interest The authors declared no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

69. Redox Protein Thioredoxin Mediates Neurite Outgrowth in Primary Cultured Mouse Cerebral Cortical Neurons.

Author

Alejandra Llanes-Cuesta M, Hoi V, Ha R, Tan H, Imamul Islam M, Eftekharpour E, and Wang JF

Subjects

Mice, Humans, Animals, Cyclic AMP Response Element-Binding Protein metabolism, Hydrogen Peroxide metabolism, Thioredoxins metabolism, Neurons metabolism, Oxidation-Reduction, Neuronal Outgrowth, RNA, Guide, CRISPR-Cas Systems, Neuroblastoma metabolism

Abstract

Thioredoxin system plays an important role in maintaining the cellular redox balance. Recent evidence suggests that thioredoxin (Trx) system may promote cell survival and neuroprotection. In this study, we explored the role of thioredoxin system in neuronal differentiation using a primary mouse cortical neuronal cell culture. First, Trx and Trx reductase (TrxR) protein levels were analyzed in cultured neurons from 1 to 32 days in vitro (DIV). The result showed that Trx and TrxR protein levels time-dependently increased in the neuron cell culture from 1 to 18 DIV. To establish the role of Trx in neuronal differentiation, Trx gene expression was knockdown in cultured neurons using Trx sgRNA CRISPR/Cas9 technology. Treatment with CRISPR/Cas9/Trx sgRNA decreased Trx protein levels and caused a reduction in dendritic outgrowth and branching of cultured neurons. Then, primary cortical neurons were treated with the Trx inhibitor PX12 to block Trx reducing activity. Treatment with PX12 also reduced dendritic outgrowth and branching. Furthermore, PX12 treatment reduced the ratio of phosphorylated cyclic AMP response element-binding protein (CREB)/total CREB protein levels. To investigate whether CREB phosphorylation is redox regulated, SH-SY5Y cells were treated with H 2 O 2 , which reduced phosphorylated CREB protein levels and increased CREB thiol oxidation. However, treatment with CB3, a Trx-mimetic tripeptide, rescued H 2 O 2 -decreased CREB phosphorylation. Our results suggest that Trx regulates neuronal differentiation and maturation of primary mouse cortical neurons by targeting CREB neurotrophic pathway. Trx may regulate CREB activation by maintaining the cellular redox balance., (Copyright © 2023 IBRO. Published by Elsevier Inc. All rights reserved.)

Published

2024

70. Electroconductive Collagen-Carbon Nanodots Nanocomposite Elicits Neurite Outgrowth, Supports Neurogenic Differentiation and Accelerates Electrophysiological Maturation of Neural Progenitor Spheroids.

Author

Lomboni DJ, Ozgun A, de Medeiros TV, Staines W, Naccache R, Woulfe J, and Variola F

Subjects

Animals, Mice, Biocompatible Materials, Cell Differentiation, Collagen, Neuronal Outgrowth, Nanocomposites, Quality of Life

Abstract

Neuronal disorders are characterized by the loss of functional neurons and disrupted neuroanatomical connectivity, severely impacting the quality of life of patients. This study investigates a novel electroconductive nanocomposite consisting of glycine-derived carbon nanodots (GlyCNDs) incorporated into a collagen matrix and validates its beneficial physicochemical and electro-active cueing to relevant cells. To this end, this work employs mouse induced pluripotent stem cell (iPSC)-derived neural progenitor (NP) spheroids. The findings reveal that the nanocomposite markedly augmented neuronal differentiation in NP spheroids and stimulate neuritogenesis. In addition, this work demonstrates that the biomaterial-driven enhancements of the cellular response ultimately contribute to the development of highly integrated and functional neural networks. Lastly, acute dizocilpine (MK-801) treatment provides new evidence for a direct interaction between collagen-bound GlyCNDs and postsynaptic N-methyl-D-aspartate (NMDA) receptors, thereby suggesting a potential mechanism underlying the observed cellular events. In summary, the findings establish a foundation for the development of a new nanocomposite resulting from the integration of carbon nanomaterials within a clinically approved hydrogel, toward an effective biomaterial-based strategy for addressing neuronal disorders by restoring damaged/lost neurons and supporting the reestablishment of neuroanatomical connectivity., (© 2023 The Authors. Advanced Healthcare Materials published by Wiley-VCH GmbH.)

Published

2024

71. Analysis of Microtubule Polymerization During Axon Outgrowth Using Fluorescently Labeled Microtubule Plus-End Tracking Proteins.

Author

Pérez-Ferrer I and Sánchez-Huertas C

Subjects

Animals, Polymerization, Time-Lapse Imaging methods, Neuronal Outgrowth, Neurons metabolism, Neurons cytology, Mice, Cells, Cultured, Microtubule-Associated Proteins metabolism, Microtubules metabolism, Axons metabolism

Abstract

The study of microtubules arrangements and dynamics during axon outgrowth and pathfinding has gained scientific interest during the last decade, and numerous technical resources for its visualization and analysis have been implemented. In this chapter, we describe the cell culture protocols of embryonic cortical and retinal neurons, the methods for transfecting them with fluorescent reporters of microtubule polymerization, and the procedures for time-lapse imaging and quantification in order to study microtubule dynamics during axon morphogenesis., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

72. Fluorescent Reporter Mice for Nerve Guidance Conduit Assessment: A High-Throughput in vivo Model.

Author

Mohan, Suresh, Hernández, Iván Coto, Wang, Wenjin, Yin, Kaiyang, Sundback, Cathryn A., Wegst, Ulrike G.K., and Jowett, Nate

Abstract

Objective: Use of cell culture and conventional in vivo mammalian models to assess nerve regeneration across guidance conduits is resource-intensive. Herein we describe a high-throughput platform utilizing transgenic mice for stain-free axon visualization paired with rapid cryosection techniques for low-cost screening of novel bioengineered nerve guidance conduit performance.Methods: Interposition repair of sciatic nerve transection in mice expressing yellow fluorescent protein in peripheral neurons (Thy1.2 YFP-16) was performed with various bioengineered neural conduit compositions using a rapid sutureless entubulation technique under isoflurane anesthesia. Axonal ingrowth was assessed at 3 and 6 weeks using epifluorescent microscopy following cryosectioning.Results: Mean procedure time (incision-to-closure) was less than 2½ minutes. Direct operational costs of a 3-week experiment was calculated at $21.47 per animal. Tissue processing steps were minimized to aldehyde fixation, cryoprotection and sectioning, and rapid fluorescent dye staining for conduit visualization. Fluorescent microscopy readily resolved robust axonal sprouting at 3 weeks, with clear elucidation of ingrowth-permissive, semipermissive, or restrictive nerve guidance conduit environments.Conclusion: A rapid and cost-efficient in vivo platform for screening of nerve guidance conduit performance has been described.Level Of Evidence: NA. Laryngoscope, E392-E392, 2018. [ABSTRACT FROM AUTHOR]

Published

2018

73. Phenotypic Screening Following Transcriptomic Deconvolution to Identify Transcription Factors Mediating Axon Growth Induced by a Kinase Inhibitor

Author

Nicholas O’Neill, John L. Bixby, Matt C. Danzi, Hassan Al-Ali, Vance Lemmon, and Jeffrey A. Lowell

Subjects

Central Nervous System, 0301 basic medicine, Phenotypic screening, Neuronal Outgrowth, Central nervous system, Biology, Inhibitory postsynaptic potential, Biochemistry, Analytical Chemistry, Rats, Sprague-Dawley, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Neurites, medicine, Animals, Protein Kinase Inhibitors, Transcription factor, Neurons, Axons, Axon growth, Rats, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, nervous system, High-content screening, Molecular Medicine, Female, A kinase, 030217 neurology & neurosurgery, Transcription Factors, Biotechnology

Abstract

After injury to the central nervous system (CNS), both neuron-intrinsic limitations on regenerative responses and inhibitory factors in the injured CNS environment restrict regenerative axon growth. Instances of successful axon regrowth offer opportunities to identify features that differentiate these situations from that of the normal adult CNS. One such opportunity is provided by the kinase inhibitor RO48, which dramatically enhances neurite outgrowth of neurons in vitro and substantially increased contralateral sprouting of corticospinal tract neurons when infused intraventricularly following unilateral pyramidotomy. The authors present here a transcriptomic deconvolution of RO48-associated axon growth, with the goal of identifying transcriptional regulators associated with axon growth in the CNS. Through the use of RNA sequencing (RNA-seq) and transcription factor binding site enrichment analysis, the authors identified a list of transcription factors putatively driving differential gene expression during RO48-induced neurite outgrowth of rat hippocampal neurons in vitro. The 82 transcription factor motifs identified in this way included some with known association to axon growth regulation, such as Jun, Klf4, Myc, Atf4, Stat3, and Nfatc2, and many with no known association to axon growth. A phenotypic loss-of-function screen was carried out to evaluate these transcription factors for their roles in neurite outgrowth; this screen identified several potential outgrowth regulators. Subsequent validation suggests that the Forkhead box (Fox) family transcription factor Foxp2 restricts neurite outgrowth, while FoxO subfamily members Foxo1 and Foxo3a promote neurite outgrowth. The authors' combined transcriptomic-phenotypic screening strategy therefore allowed identification of novel transcriptional regulators of neurite outgrowth downstream of a multitarget kinase inhibitor.

Published

2021

74. Optimised techniques for high-throughput screening of differentiated SH-SY5Y cells and application for neurite outgrowth assays

Author

Anusha Dravid, Brad Raos, Darren Svirskis, and Simon J. O’Carroll

Subjects

Multidisciplinary, Science, Biological techniques, Neuronal Outgrowth, Cell Differentiation, Article, High-Throughput Screening Assays, Cell Line, Tumor, Neurites, Humans, Medicine, Neuroscience

Abstract

Neuronal models are a crucial tool in neuroscientific research, helping to elucidate the molecular and cellular processes involved in disorders of the nervous system. Adapting these models to a high-throughput format enables simultaneous screening of multiple agents within a single assay. SH-SY5Y cells have been widely used as a neuronal model, yet commonly in an undifferentiated state that is not representative of mature neurons. Differentiation of the SH-SY5Y cells is a necessary step to obtain cells that express mature neuronal markers. Despite this understanding, the absence of a standardised protocol has limited the use of differentiated SH-SY5Y cells in high-throughput assay formats. Here, we describe techniques to differentiate and re-plate SH-SY5Y cells within a 96-well plate for high-throughput screening. SH-SY5Y cells seeded at an initial density of 2,500 cells/well in a 96-well plate provide sufficient space for neurites to extend, without impacting cell viability. Room temperature pre-incubation for 1 h improved the plating homogeneity within the well and the ability to analyse neurites. We then demonstrated the efficacy of our techniques by optimising it further for neurite outgrowth analysis. The presented methods achieve homogenously distributed differentiated SH-SY5Y cells, useful for researchers using these cells in high-throughput screening assays.

Published

2021

75. Differential Regulation of Neurite Outgrowth and Growth Cone Morphology by 3D Fibronectin and Fibronectin-Collagen Extracellular Matrices

Author

Jean E. Schwarzbauer and Archana Sharma

Subjects

Decellularization, biology, Neurite, Chemistry, Decellularized Extracellular Matrix, Regeneration (biology), Growth Cones, Neuronal Outgrowth, Neuroscience (miscellaneous), Article, Extracellular Matrix, Fibronectins, Cell biology, Extracellular matrix, Fibronectin, Cellular and Molecular Neuroscience, Neurology, Neurites, biology.protein, Extracellular, Collagen, Growth cone, Cells, Cultured, Type I collagen

Abstract

The extracellular matrix (ECM) plays a critical role in development, homeostasis, and regeneration of tissue structures and functions. Cell interactions with the ECM are dynamic and cells respond to ECM remodeling by changes in morphology and motility. During nerve regeneration, the ECM facilitates neurite outgrowth and guides axons with target specificity. Decellularized ECMs retain structural, biochemical, and biomechanical cues of native ECM and have the potential to replace damaged matrix to support cell activities during tissue repair. To determine the ECM components that contribute to nerve regeneration, we analyzed neuron-ECM interactions on two types of decellularized ECM. One matrix was composed primarily of fibronectin (FN) fibrils, and the other FN-rich ECM also contained significant numbers of type I collagen (COL I) fibrils. Using primary neurons dissociated from superior cervical ganglion (SCG) explants, we found that neurites were extended on both matrices without a significant difference in average neurite length after 24 h. The most distinctive features of neurites on the FN matrix were numerous short actin-filled protrusions and longer branches extending from neurite shafts. Very few protrusions and branches were detected on FN-COL matrix. Growth cone morphologies also differed with mostly filopodial growth cones on FN matrix whereas on FN-COL matrix, equivalent numbers of filopodial and slender growth cones were formed. Our work provides new information about how changes in major components of the ECM during tissue repair modulate neuron and growth cone morphologies and helps to define the contributions of neuron-ECM interactions to nerve development and regeneration.

Published

2021

76. Distinct small non-coding RNA landscape in the axons and released extracellular vesicles of developing primary cortical neurons and the axoplasm of adult nerves

Author

Raquel Mesquita-Ribeiro, Rafael Sebastián Fort, Alex Rathbone, Joaquina Farias, Cristiano Lucci, Victoria James, Jose Sotelo-Silveira, Maria Ana Duhagon, Federico Dajas-Bailador, Mesquita-Ribeiro R, Fort Canobra Rafael S, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Biología., Rathbone Alex, Farías Joaquina, IIBCE, Lucci Cristiano, James Victoria, Sotelo Silveira José Roberto, IIBCE, Duhagon María Ana, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Biología., and Dajas-Bailador F

Subjects

sncRNAs, Biochemistry & Molecular Biology, MICRORNAS, Neuronal Outgrowth, Cell Communication, Cell Fractionation, Axon, Extracellular Vesicles, 03 medical and health sciences, 0302 clinical medicine, RNA, Transfer, Humans, tRNA-derived fragments, Molecular Biology, FRAGMENTS, TARGETING MAP1B, 030304 developmental biology, EXOSOMES, Neurons, axon, 0303 health sciences, Science & Technology, IDENTIFICATION, PROFILING REVEALS, Computational Biology, High-Throughput Nucleotide Sequencing, Biological Transport, Molecular Sequence Annotation, Cell Biology, Extracellular vesicles, Axons, nervous system, miRNAs, LOCAL PROTEIN-SYNTHESIS, GROWTH, Nucleic Acid Conformation, RNA, Small Untranslated, TRANSLATION, MESSENGER-RNA, Life Sciences & Biomedicine, 030217 neurology & neurosurgery, Research Article, Research Paper, Subcellular Fractions

Abstract

Neurons have highlighted the needs for decentralized gene expression and specific RNA function in somato-dendritic and axonal compartments, as well as in intercellular communication via extracellular vesicles (EVs). Despite advances in miRNA biology, the identity and regulatory capacity of other small non-coding RNAs (sncRNAs) in neuronal models and local subdomains has been largely unexplored.We identified a highly complex and differentially localized content of sncRNAs in axons and EVs during early neuronal development of cortical primary neurons and in adult axons invivo. This content goes far beyond miRNAs and includes most known sncRNAs and precisely processed fragments from tRNAs, sno/snRNAs, Y RNAs and vtRNAs. Although miRNAs are the major sncRNA biotype in whole-cell samples, their relative abundance is significantly decreased in axons and neuronal EVs, where specific tRNA fragments (tRFs and tRHs/tiRNAs) mainly derived from tRNAs Gly-GCC, Val-CAC and Val-AAC predominate. Notably, although 5'-tRHs compose the great majority of tRNA-derived fragments observed invitro, a shift to 3'-tRNAs is observed in mature axons invivo.The existence of these complex sncRNA populations that are specific to distinct neuronal subdomains and selectively incorporated into EVs, equip neurons with key molecular tools for spatiotemporal functional control and cell-to-cell communication. ispartof: RNA BIOLOGY vol:18 issue:sup2 pages:832-855 ispartof: location:United States status: published

Published

2021

77. Discovery of thymosin β4 as a human exerkine and growth factor

Author

Marie Björnholm, Jonas T. Treebak, Atul S. Deshmukh, Niklas Rye Jørgensen, Christoffer Clemmensen, Anna Krook, Alba Gonzalez-Franquesa, Juleen R. Zierath, Emilie Dalbram, Håkan Karlsson, Stanislava Pankratova, Ben Stocks, Morten Hostrup, Sevda Gheibi, Alexander V. Chibalin, Ankita Agrawal, Thomas Nielsen, Melissa L. Borg, and Michael S. Kuefner

Subjects

Male, Proteomics, Physiology, medicine.medical_treatment, Muscle Fibers, Skeletal, Neuronal Outgrowth, Muscular Diseases, Tandem Mass Spectrometry, Cell Line, Tumor, Faculty of Science, medicine, Animals, Humans, Endocrine system, Secreted factor, Muscle, Skeletal, Exercise, Cell Proliferation, Osteoblasts, Chemistry, Growth factor, Skeletal muscle, Cell Biology, Cell biology, Mice, Inbred C57BL, Thymosin, Thymosin beta-4, Disease Models, Animal, medicine.anatomical_structure, Diabetes Mellitus, Type 2, Muscle contraction, Case-Control Studies, Physical Endurance, Insulin Resistance, medicine.symptom, Exerkine, Muscle Contraction, Signal Transduction

Abstract

Skeletal muscle is an endocrine organ secreting exercise-induced factors (exerkines), which play a pivotal role in interorgan cross talk. Using mass spectrometry (MS)-based proteomics, we characterized the secretome and identified thymosin β4 (TMSB4X) as the most upregulated secreted protein in the media of contracting C2C12 myotubes. TMSB4X was also acutely increased in the plasma of exercising humans irrespective of the insulin resistance condition or exercise mode. Treatment of mice with TMSB4X did not ameliorate the metabolic disruptions associated with diet induced-obesity, nor did it enhance muscle regeneration in vivo. However, TMSB4X increased osteoblast proliferation and neurite outgrowth, consistent with its WADA classification as a prohibited growth factor. Therefore, we report TMSB4X as a human exerkine with a potential role in cellular cross talk.

Published

2021

78. PI3K-mTOR-S6K Signaling Mediates Neuronal Viability via Collapsin Response Mediator Protein-2 Expression

Author

Eun J. Na, Hye Yeon Nam, Jiyoung Park, Myung Ah Chung, Hyun Ae Woo, and Hwa-Jung Kim

Subjects

mTOR pathways, PI3K, CRMP-2, neuronal outgrowth, pentylentetrazole, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Collapsin response mediator protein (CRMP)-2 and the mammalian target of rapamycin complex 1 (mTORC1) signaling pathway are associated with common physiological functions such as neuronal polarity, axonal outgrowth and synaptic strength, as well as various brain disorders including epilepsy. But, their regulatory and functional links are unclear. Alterations in CRMP-2 expression that lead to its functional changes are implicated in brain disorders such as epilepsy. Here, we investigate whether changes in CRMP-2 expression, possibly regulated by mTOR-related signaling, correlates with neuronal growth and viability. Inhibition of mTOR and/or phosphoinositol-3-kinase (PI3K) led to deceased p-S6K, and p-S6 signals also reduced CRMP-2 expression. These changes corresponded to inhibition of neuronal viability and proliferation in cultured hippocampal HT-22 cells under both basal serum-free and serum- or insulin-induced mTOR pathway-activated conditions. CRMP-2 expression tended to be increased by mTOR activation, indicated by an increase in p-S6/S6 level, in pentylentetrazole (PTZ)-induced epileptic rat hippocampal tissues was also significantly reduced by mTOR inhibition. Knockdown of CRMP-2 by si-RNA reduced the neuronal viability without changes in mTOR signaling, and overexpression of CRMP-2 recovered the glutamate-induced neurotoxicity and decrease of mTOR signaling in HT-22 cells. In conclusion, CRMP-2 protein expression controlled by the PI3K-mTOR-S6K signaling axis exerts its important functional roles in neuronal growth and survival.

Published

2017

79. Directional control of neurite outgrowth: emerging technologies for Parkinson's disease using magnetic nanoparticles and magnetic field gradients

Author

K. Dhillon, K. Aizel, T. J. Broomhall, E. Secret, T. Goodman, M. Rotherham, N. Telling, J. M. Siaugue, C. Ménager, J. Fresnais, M. Coppey, A. J. El Haj, and M. A. Gates

Subjects

Biomaterials, Magnetic Fields, Neuronal Outgrowth, Neurites, Biomedical Engineering, Biophysics, Animals, Parkinson Disease, Bioengineering, Magnetite Nanoparticles, Biochemistry, Rats, Biotechnology

Abstract

A challenge in current stem cell therapies for Parkinson's disease (PD) is controlling neuronal outgrowth from the substantia nigra towards the targeted area where connectivity is required in the striatum. Here we present progress towards controlling directional neurite extensions through the application of iron-oxide magnetic nanoparticles (MNPs) labelled neuronal cells combined with a magnetic array generating large spatially variant field gradients (greater than 20 T m −1 ). We investigated the viability of this approach in both two-dimensional and organotypic brain slice models and validated the observed changes in neurite directionality using mathematical models. Results showed that MNP-labelled cells exhibited a shift in directional neurite outgrowth when cultured in a magnetic field gradient, which broadly agreed with mathematical modelling of the magnetic force gradients and predicted MNP force direction. We translated our approach to an ex vivo rat brain slice where we observed directional neurite outgrowth of transplanted MNP-labelled cells from the substantia nigra towards the striatum. The improved directionality highlights the viability of this approach as a remote-control methodology for the control and manipulation of cellular growth for regenerative medicine applications. This study presents a new tool to overcome challenges faced in the development of new therapies for PD.

Published

2022

80. Modulation of Early Stage Neuronal Outgrowth through Out-of-Plane Graphene

Author

Laura Matino, Anna Mariano, Chiara Ausilio, Raghav Garg, Tzahi Cohen-Karni, and Francesca Santoro

Subjects

Mechanical Engineering, Neuronal Outgrowth, Neurites, General Materials Science, Bioengineering, Graphite, General Chemistry, Condensed Matter Physics, Axons, Cells, Cultured, Nerve Regeneration

Abstract

The correct wiring of a neural network requires neuron to integrate an incredible repertoire of cues found in their extracellular environment. The astonishing efficiency of this process plays a pivotal role in the correct wiring of the brain during development and axon regeneration. Biologically inspired micro- and nanostructured substrates have been shown to regulate axonal outgrowth. In parallel, several studies investigated graphene's potential as a conductive neural interface, able to enhance cell adhesion, neurite sprouting and outgrowth. Here, we engineered a 3D single- to few-layer fuzzy graphene morphology (3DFG), 3DFG on a collapsed Si nanowire (SiNW) mesh template (NT-3DFGc), and 3DFG on a noncollapsed SiNW mesh template (NT-3DFGnc) as neural-instructive materials. The micrometric protruding features of the NWs templates dictated neuronal growth cone establishment, as well as influencing axon elongation and branching. Furthermore, neurons-to-graphene coupling was investigated with comprehensive view of integrin-mediated contact adhesion points and plasma membrane curvature processes.

Published

2022

81. Branched Chondroitin Sulfate Oligosaccharides Derived from the Sea Cucumber

Author

Weili, Wang, Hui, Mao, Sujuan, Li, Longlong, Zhang, Lian, Yang, Ronghua, Yin, and Jinhua, Zhao

Subjects

Sulfates, Sea Cucumbers, Chondroitin Sulfates, Neuronal Outgrowth, Animals, Oligosaccharides, Disaccharides, Fucose

Abstract

Fucosylated chondroitin sulfate (FCS) from the sea cucumber

Published

2022

82. Mechanosensitive axon outgrowth mediated by L1-laminin clutch interface

Author

Kentarou Baba, Koay Teng Wei, Kouki Abe, Liguo Huang, Naoyuki Inagaki, Yoichiroh Hosokawa, and Kazunori Okano

Subjects

Growth cone membrane, Tractive force, Cell adhesion molecule, Chemistry, Growth Cones, Neuronal Outgrowth, Biophysics, Catch bond, macromolecular substances, Actins, Axons, Coupling (electronics), Protein filament, Mice, Animals, Mechanosensitive channels, Laminin, Growth cone, Cells, Cultured

Abstract

Mechanical properties of the extracellular environment modulate axon outgrowth. Growth cones at the tip of extending axons generate traction force for axon outgrowth by transmitting the force of actin filament retrograde flow, produced by actomyosin contraction and F-actin polymerization, to adhesive substrates through clutch and cell adhesion molecules. A molecular clutch between the actin filament flow and substrate is proposed to contribute to cellular mechanosensing. However, the molecular identity of the clutch interface responsible for mechanosensitive growth cone advance is unknown. We previously reported that mechanical coupling between actin filament retrograde flow and adhesive substrates through the clutch molecule shootin1a and the cell adhesion molecule L1 generates traction force for axon outgrowth and guidance. Here, we show that cultured mouse hippocampal neurons extend longer axons on stiffer substrates under elastic conditions that correspond to the soft brain environments. We demonstrate that this stiffness-dependent axon outgrowth requires actin-adhesion coupling mediated by shootin1a, L1, and laminin on the substrate. Speckle imaging analyses showed that L1 at the growth cone membrane switches between two adhesive states: L1 that is immobilized and that undergoes retrograde movement on the substrate. The duration of the immobilized phase was longer on stiffer substrates; this was accompanied by increases in actin-adhesion coupling and in the traction force exerted on the substrate. These data suggest that the interaction between L1 and laminin is enhanced on stiffer substrates, thereby promoting force generation for axon outgrowth.

Published

2021

83. Molecular Mechanism for PACAP 38-Induced Neurite Outgrowth in PC12 Cells

Author

Fumiko Takenoya, Ai Kimura, Junko Shibato, Michio Yamashita, Seiji Shioda, Takahiro Hirabayashi, Ichiro Takasaki, and Randeep Rakwal

Subjects

MAPK/ERK pathway, Article Subject, Neurite, Neuronal Outgrowth, Neurosciences. Biological psychiatry. Neuropsychiatry, Nerve Tissue Proteins, PC12 Cells, Dephosphorylation, Neurites, Animals, Receptor, Protein kinase B, Glycogen Synthase Kinase 3 beta, Chemistry, Cyclin-dependent kinase 5, Rats, Cell biology, Gene Expression Regulation, Neurology, Cell culture, Intercellular Signaling Peptides and Proteins, Pituitary Adenylate Cyclase-Activating Polypeptide, Neurology (clinical), Collapsin response mediator protein family, RC321-571, Signal Transduction, Research Article

Abstract

The present research investigates the molecular mechanism of neurite outgrowth (protrusion elongation) under pituitary adenylate cyclase-activating polypeptide (PACAP) 38 treatments using a rat adrenal-derived pheochromocytoma cell line—PC12. This study specifically looks into the regulation of PACAP38-induced collapsing response mediator protein 2 (CRMP2) previously identified in a mouse brain ischemia model and which could be recovered by PACAP38 treatment. Previously, DNA microarray analysis revealed that PACAP 38-mediated neuroprotection involved not only CRMP2 but also pathways related to glycogen synthase kinase-3β (GSK-3β) and other signaling components. Thus, to clarify whether CRMP2 acts directly on PACAP38 or through GSK-3β as part of the mechanism of PACAP38-induced neurite outgrowth, we observed neurite outgrowth in the presence of GSK-3β inhibitors and activators. PC12 cells were treated with PACAP38 being added to the cell culture medium at concentrations of 10−7 M, 10−8 M, and 10−9 M. Post PACAP38 treatment, immunostaining was used to confirm protrusion elongation of the PC12 cells, while RT-PCR, two-dimensional gel electrophoresis in conjunction with Western blotting, and inhibition experiments were performed to confirm the expression of the PACAP gene, its receptors, and downstream signaling components. Our data show that neurite protrusion elongation by PACAP38 (10−7 M) in PC12 cells is mediated through the PAC1-R receptor as demonstrated by its suppression by a specific inhibitor PA-8. Inhibitor experiments suggested that PACAP38-triggered neurite protrusion follows a GSK-3β-regulated pathway, where the AKT and cAMP/ERK pathways are involved and where the inhibition of Rho/Roc could enhance neurite protrusion under PACAP38 stimulation. Although we could not yet confirm the exact role and position of CRMP2 in PACAP38-mediated PC12 cell elongation, it appears that its phosphorylation and dephosphorylation have a correlation with the neurite protrusion elongation through the interplay of CDK5, which needs to be investigated further.

Published

2021

84. Schwann Cells Provide Iron to Axonal Mitochondria and Its Role in Nerve Regeneration

Author

Bruno Siqueira Mietto, Katrin Schulz, Samuel David, and Priya Jhelum

Subjects

Sensory Receptor Cells, Transcription, Genetic, Iron, Neuronal Outgrowth, Ferroportin, Schwann cell, Transferrin receptor, Mitochondrion, Iron Chelating Agents, Mice, Ganglia, Spinal, Ranvier's Nodes, Receptors, Transferrin, medicine, Animals, Cation Transport Proteins, Research Articles, Cells, Cultured, biology, Chemistry, General Neuroscience, MITOCHONDRIAL FERRITIN, Ceruloplasmin, Sciatic nerve injury, medicine.disease, Sciatic Nerve, Axons, Mitochondria, Nerve Regeneration, Cell biology, Mice, Inbred C57BL, medicine.anatomical_structure, nervous system, biology.protein, RNA, Female, Schwann Cells, Sciatic nerve, Sciatic Neuropathy

Abstract

Iron is an essential cofactor for several metabolic processes, including the generation of ATP in mitochondria, which is required for axonal function and regeneration. However, it is not known how mitochondria in long axons, such as those in sciatic nerves, acquire iron in vivo. Because of their close proximity to axons, Schwann cells are a likely source of iron for axonal mitochondria in the PNS. Here we demonstrate the critical role of iron in promoting neurite growth in vitro using iron chelation. We also show that Schwann cells express the molecular machinery to release iron, namely, the iron exporter, ferroportin (Fpn) and the ferroxidase ceruloplasmin (Cp). In Cp KO mice, Schwann cells accumulate iron because Fpn requires to partner with Cp to export iron. Axons and Schwann cells also express the iron importer transferrin receptor 1 (TfR1), indicating their ability for iron uptake. In teased nerve fibers, Fpn and TfR1 are predominantly localized at the nodes of Ranvier and Schmidt-Lanterman incisures, axonal sites that are in close contact with Schwann cell cytoplasm. We also show that lack of iron export from Schwann cells in Cp KO mice reduces mitochondrial iron in axons as detected by reduction in mitochondrial ferritin, affects localization of axonal mitochondria at the nodes of Ranvier and Schmidt-Lanterman incisures, and impairs axonal regeneration following sciatic nerve injury. These finding suggest that Schwann cells contribute to the delivery of iron to axonal mitochondria, required for proper nerve repair. SIGNIFICANCE STATEMENT This work addresses how and where mitochondria in long axons in peripheral nerves acquire iron. We show that Schwann cells are a likely source as they express the molecular machinery to import iron (transferrin receptor 1), and to export iron (ferroportin and ceruloplasmin [Cp]) to the axonal compartment at the nodes of Ranvier and Schmidt-Lanterman incisures. Cp KO mice, which cannot export iron from Schwann cells, show reduced iron content in axonal mitochondria, along with increased localization of axonal mitochondria at Schmidt-Lanterman incisures and nodes of Ranvier, and impaired sciatic nerve regeneration. Iron chelation in vitro also drastically reduces neurite growth. These data suggest that Schwann cells are likely to contribute iron to axonal mitochondria needed for axon growth and regeneration.

Published

2021

85. Protein phosphatase 6 promotes neurite outgrowth by promoting mTORC2 activity in N2a cells

Author

Koji Hayakawa, Nobuyuki Fujiwara, Nao Kitamura, Koichi Sato, and Takashi Ohama

Subjects

biology, Neurite, Chemistry, Neuronal Outgrowth, Mechanistic Target of Rapamycin Complex 2, General Medicine, CREB, Biochemistry, mTORC2, N2a cell, Cell biology, Mice, Phosphoprotein Phosphatases, biology.protein, Neuron differentiation, Animals, Humans, Phosphorylation, Molecular Biology, Protein kinase B, Cells, Cultured, PI3K/AKT/mTOR pathway

Abstract

Understanding the molecular mechanism of neuronal differentiation is important to overcome the incurable diseases caused by nervous system damage. Neurite outgrowth is prerequisite for neuronal differentiation and regeneration, and cAMP response element-binding protein (CREB) is one of the major transcriptional factors positively regulating this process. Neuronal differentiation stimuli activate mammalian target of rapamycin (mTOR) complex 2 (mTORC2)/Akt signalling to phosphorylate CREB; however, the precise molecular mechanism of this event has not been fully understood. In this manuscript, we show that neuronal differentiation stimuli increased a protein level of protein phosphatase 6 (PP6), a member of type 2A Ser/Thr protein phosphatases. PP6 knockdown suppressed mTORC2/Akt/CREB signalling and results in failure of neurite outgrowth. SIN1 is a unique component of mTORC2 that enhances mTORC2 activity towards Akt when it is in dephosphorylated form. We found PP6 knockdown increased SIN1 phosphorylation. These data suggest that PP6 may positively regulate neurite outgrowth by dephosphorylating SIN1 to activate mTORC2/Akt/CREB signalling.

Published

2021

86. This title is unavailable for guests, please login to see more information.

Author

Aghanoori, Mohamad-Reza, Aghanoori, Mohamad-Reza, Agarwal, Prasoon, Gauvin, Evan, Nagalingam, Raghu S, Bonomo, Raiza, Yathindranath, Vinith, Smith, Darrell R, Hai, Yan, Lee, Samantha, Jolivalt, Corinne G, Calcutt, Nigel A, Jones, Meaghan J, Czubryt, Michael P, Miller, Donald W, Dolinsky, Vernon W, Mansuy-Aubert, Virginie, Fernyhough, Paul, Aghanoori, Mohamad-Reza, Aghanoori, Mohamad-Reza, Agarwal, Prasoon, Gauvin, Evan, Nagalingam, Raghu S, Bonomo, Raiza, Yathindranath, Vinith, Smith, Darrell R, Hai, Yan, Lee, Samantha, Jolivalt, Corinne G, Calcutt, Nigel A, Jones, Meaghan J, Czubryt, Michael P, Miller, Donald W, Dolinsky, Vernon W, Mansuy-Aubert, Virginie, and Fernyhough, Paul

Published

2022

87. Effects of antiepileptic drugs’ administration during pregnancy on the nerve cell proliferation and axonal outgrowth of human neuroblastoma SH-SY5Y nerve cells

Author

Satoshi Ueshima, Daiki Hira, Tomonobu Okano, Kosuke Shimokawa, and Mikio Kakumoto

Subjects

0301 basic medicine, Phenytoin, SH-SY5Y, Neuronal Outgrowth, Cell, Biophysics, Pharmacology, Lamotrigine, Biochemistry, Neuroblastoma, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Cell Line, Tumor, medicine, Humans, Axon, Child, Molecular Biology, Cell Proliferation, Neurons, Valproic Acid, Epilepsy, Cell growth, Chemistry, Cell Biology, Carbamazepine, medicine.disease, NAV1.1 Voltage-Gated Sodium Channel, 030104 developmental biology, medicine.anatomical_structure, Prenatal Exposure Delayed Effects, 030220 oncology & carcinogenesis, Anticonvulsants, Female, lipids (amino acids, peptides, and proteins), medicine.drug

Abstract

It has been suggested that the intelligence quotient of children born to pregnant women taking 1000 mg or more of valproic acid per day is lower than that of children born to pregnant women taking other antiepileptic drugs. However, the mechanism whereby intelligence quotient is decreased in children exposed to valproic acid during the fetal period has not yet been elucidated. Therefore, we used the human neuroblastoma cell line SH-SY5Y to evaluate the effects of antiepileptic drugs containing valproic acid on nerve cells. We assessed the anti-proliferative effects of drugs in these cells via WST-8 colorimetric assay, using the Cell Counting Kit-8. We also quantified drug effects on axonal elongation from images using ImageJ software. We also evaluated drug effects on mRNA expression levels on molecules implicated in nervous system development and folic acid uptake using real-time PCR. We observed that carbamazepine and lamotrigen were toxic to SH-SY5Y cells at concentrations >500 μM. In contrast, phenytoin and valproic acid were not toxic to these cells. Carbamazepine, lamotrigen, phenytoin, and valproic acid did not affect axonal outgrowth in SH-SY5Y cells. Sodium channel neuronal type 1a (SCN1A) mRNA expression-level ratios increased when valproic acid was supplemented to cells. The overexpression of SCN1A mRNA due to high valproic acid concentrations during the fetal period may affect neurodevelopment. However, since detailed mechanisms have not yet been elucidated, it is necessary to evaluate it by comparing cell axon elongation and SCN1A protein expression due to high-concentration valproic acid exposure.

Published

2021

88. Developmental Neurotoxicity of Fipronil and Rotenone on a Human Neuronal In Vitro Test System

Author

Gerd Bicker, Silke Dempewolf, Saime Tan, Anne Schmitz, and Michael Stern

Subjects

0301 basic medicine, Insecticides, Neurite, DNT, Neuronal Outgrowth, 010501 environmental sciences, Pharmacology, Toxicology, medicine.disease_cause, 01 natural sciences, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, Cell Movement, In vivo, Rotenone, Precursor cell, medicine, Humans, NTera-2, NTERA-2, Migration, Fipronil, 0105 earth and related environmental sciences, Neurons, Dose-Response Relationship, Drug, General Neuroscience, Neurite outgrowth, NT2, Cell Differentiation, In vitro, 030104 developmental biology, chemistry, Differentiation, Pyrazoles, Original Article, Neurotoxicity Syndromes, Oxidative stress

Abstract

Pesticide exposure during in utero and early postnatal development can cause a wide range of neurological defects. However, relatively few insecticides have been recognized as developmental neurotoxicants, so far. Recently, discovery of the insecticide, fipronil, in chicken eggs has raised public concern. The status of fipronil as a potential developmental neurotoxicant is still under debate. Whereas several in vivo and in vitro studies suggest specific toxicity, other in vitro studies could not confirm this concern. Here, we tested fipronil and its main metabolic product, fipronil sulfone both at concentrations between 1.98 and 62.5 µM, alongside with the established developmental neurotoxicant, rotenone (0.004–10 µM) in vitro on the human neuronal precursor cell line NT2. We found that rotenone impaired all three tested DNT endpoints, neurite outgrowth, neuronal differentiation, and precursor cell migration in a dose-dependent manner and clearly separable from general cytotoxicity in the nanomolar range. Fipronil and fipronil sulfone specifically inhibited cell migration and neuronal differentiation, but not neurite outgrowth in the micromolar range. The rho-kinase inhibitor Y-27632 counteracted inhibition of migration for all three compounds (EC50 between 12 and 50 µM). The antioxidant, n-acetyl cysteine, could ameliorate the inhibitory effects of fipronil on all three tested endpoints (EC 50 between 84 and 164 µM), indicating the involvement of oxidative stress. Fipronil sulfone had a stronger effect than fipronil, confirming the importance to test metabolic products alongside original pesticides. We conclude that in vitro fipronil and fipronil sulfone display specific developmental neurotoxicity on developing human model neurons. Supplementary Information The online version contains supplementary material available at 10.1007/s12640-021-00364-8.

Published

2021

89. Achyranthes bidentata polypeptide k enhances the survival, growth and axonal regeneration of spinal cord motor neurons in vitro

Author

Fei Ding, Qiong Cheng, Ergai Cai, and Shu Yu

Subjects

0301 basic medicine, Neurofilament, Neurite, Cell Survival, medicine.medical_treatment, Muscle Fibers, Skeletal, Neuronal Outgrowth, Primary Cell Culture, Neuromuscular Junction, In Vitro Techniques, Neuroprotection, Neuromuscular junction, Rats, Sprague-Dawley, 03 medical and health sciences, GAP-43 Protein, 0302 clinical medicine, Neurofilament Proteins, Peripheral Nerve Injuries, medicine, Animals, Achyranthes bidentata, Achyranthes, Motor Neurons, biology, Plant Extracts, General Neuroscience, Regeneration (biology), Axotomy, biology.organism_classification, Spinal cord, Axons, Coculture Techniques, Nerve Regeneration, Rats, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Spinal Cord, nervous system, Peptides, 030217 neurology & neurosurgery

Abstract

Achyranthes bidentata polypeptide k (ABPPk), a powerful active component from a traditional Chinese medicinal herb-Achyranthes bidentata Bl., has exhibited promising neuroprotective activity due to its multiple-targeting capability. However, the effect of ABPPk on the survival, growth and axonal regeneration of spinal cord motor neurons remains unclear. Here, a modified method, which is more optimized for embryonic cells in ambient carbon dioxide levels, was used for acquisition of rat embryonic spinal cord motor neurons with high survival and purity. ABPPk concentration-dependently enhanced the neuronal viability and promoted the neurite outgrowth. Co-culture of motor neurons and skeletal myocytes model indicated that ABPPk enhanced the neuromuscular junction development and maturation. A microfluidic axotomy model was further established for the axonal disconnection, and ABPPk significantly accelerated the axonal regeneration of motor neurons. Furthermore, we demonstrated that the upregulation of three neurofilament protein subunits in motor neurons might be relevant to the mechanisms of the growth-promoting effect of ABPPk. Our findings provide an experimental and theoretical basis for the development of ABPPk as a potential application in the development of treatment strategy for nerve injury diseases.

Published

2021

90. Abundant oleoyl-lysophosphatidylethanolamine in brain stimulates neurite outgrowth and protects against glutamate toxicity in cultured cortical neurons

Author

Shiori Kawase, Taiga Kurihara, Takeshi Uemura, Tamotsu Tsukahara, Yoshikazu Matsuda, Kazutoshi Hisano, Hisao Haniu, Naoto Saito, Tetsuhiko Mimura, and Hironori Yoshida

Subjects

Male, MAPK/ERK pathway, Spectrometry, Mass, Electrospray Ionization, Neurite, Neuronal Outgrowth, Excitotoxicity, Glutamic Acid, medicine.disease_cause, Biochemistry, Mice, chemistry.chemical_compound, Neurites, medicine, Animals, Phosphorylation, Extracellular Signal-Regulated MAP Kinases, Protein kinase A, Molecular Biology, Cells, Cultured, Protein Kinase C, Protein kinase C, Neurons, Phospholipase C, Chemistry, Glutamate receptor, Brain, Lysophosphatidylethanolamine, General Medicine, Cell biology, Mice, Inbred C57BL, Type C Phospholipases, GTP-Binding Protein alpha Subunits, Gq-G11, Lysophospholipids, Chromatography, Liquid, Signal Transduction

Abstract

Lysophosphatidylethanolamines (LPEs) are bioactive lysophospholipids that have been suggested to play important roles in several biological processes. We performed a quantitative analysis of LPE species and showed their composition in mouse brain. We examined the roles of oleoyl-LPE (18:1 LPE), which is one of the abundant LPE species in brain. In cultured cortical neurons, application of 18:1 LPE-stimulated neurite outgrowth. The effect of 18:1 LPE on neurite outgrowth was inhibited by Gq/11 inhibitor YM-254890, phospholipase C (PLC) inhibitor U73122, protein kinase C (PKC) inhibitor Go6983 or mitogen-activated protein kinase (MAPK) inhibitor U0126. Additionally, 18:1 LPE increased the phosphorylation of MAPK/extracellular signal-regulated kinase 1/2. These results suggest that the action of 18:1 LPE on neurite outgrowth is mediated by the Gq/11/PLC/PKC/MAPK pathway. Moreover, we found that application of 18:1 LPE protects neurons from glutamate-induced excitotoxicity. This effect of 18:1 LPE was suppressed by PKC inhibitor Go6983. These results suggest that 18:1 LPE protects neurons from glutamate toxicity via PKC inhibitor Go6983-sensitive PKC subtype. Collectively, our results demonstrated that 18:1 LPE stimulates neurite outgrowth and protects against glutamate toxicity in cultured cortical neurons. Our findings provide insights into the physiological or pathological roles of 18:1 LPE in the brain.

Published

2021

91. Docosahexanoic acid signals through the Nrf2–Nqo1 pathway to maintain redox balance and promote neurite outgrowth

Author

Brodie Buchner-Duby, Jing X. Kang, Scott D. Ryan, David W.L. Ma, Jennifer Drolet, Morgan G. Stykel, and Carla Coackley

Subjects

Docosahexaenoic Acids, Transcription, Genetic, genetic structures, Neurite, NF-E2-Related Factor 2, Neuronal Outgrowth, Antioxidant response element, Biology, digestive system, environment and public health, Redox, Antioxidants, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, NAD(P)H Dehydrogenase (Quinone), Animals, Humans, Molecular Biology, 030304 developmental biology, Neurons, 0303 health sciences, Brief Report, food and beverages, Dendrites, Cell Biology, respiratory system, Cell biology, Oxidative Stress, Balance (accounting), lipids (amino acids, peptides, and proteins), Oxidation-Reduction, 030217 neurology & neurosurgery, Signal Transduction

Abstract

Evidence suggests that n-3 polyunsaturated fatty acids may act as activators of the Nrf2 antioxidant pathway. The antioxidant response, in turn, promotes neuronal differentiation and neurite outgrowth. Nrf2 has recently been suggested to be a cell intrinsic mediator of docosohexanoic acid (DHA) signaling. In the current study, we assessed whether DHA-mediated axodendritic development was dependent on activation of the Nrf2 pathway and whether Nrf2 protected from agrochemical-induced neuritic retraction. Expression profiling of the DHA-enriched Fat-1 mouse brain relative to wild type showed a significant enrichment of genes associated with neuronal development and neuronal projection and genes associated with the Nrf2-transcriptional pathway. Moreover, we found that primary cortical neurons treated with DHA showed a dose-dependent increase in Nrf2 transcriptional activity and Nrf2-target gene expression. DHA-mediated activation of Nrf2 promoted neurite outgrowth and inhibited oxidative stress-induced neuritic retraction evoked by exposure to agrochemicals. Finally, we provide evidence that this effect is largely dependent on induction of the Nrf2-target gene NAD(P)H: (quinone acceptor) oxidoreductase 1 (NQO1), and that silencing of either Nrf2 or Nqo1 blocks the effects of DHA on the axodendritic compartment. Collectively, these data support a role for the Nrf2-NQO1 pathway in DHA-mediated axodendritic development and protection from agrochemical exposure.

Published

2021

92. Neurite Outgrowth-Promoting Compounds from the Petals of

Author

Takeru, Koga, Hideyuki, Ito, Yuji, Iwaoka, Toshiro, Noshita, and Akihiro, Tai

Subjects

Flavonoids, Glucosides, Neuronal Outgrowth, Animals, Paeonia, PC12 Cells, Rats

Abstract

Isorhamnetin-3

Published

2022

93. ARNO is recruited by the neuronal adaptor FE65 to potentiate ARF6-mediated neurite outgrowth

Author

Yuqi Zhai, Wai Wa Ray Chan, Wen Li, and Kwok-Fai Lau

Subjects

Neurons, ADP-Ribosylation Factor 6, ADP-Ribosylation Factors, Nucleotides, General Neuroscience, Immunology, GTPase-Activating Proteins, Neuronal Outgrowth, Guanine Nucleotide Exchange Factors, General Biochemistry, Genetics and Molecular Biology

Abstract

ADP-ribosylation factor 6 (ARF6) is a small GTPase that has a variety of neuronal functions including stimulating neurite outgrowth, a crucial process for the establishment and maintenance of neural connectivity. As impaired and atrophic neurites are often observed in various brain injuries and neurological diseases, understanding the intrinsic pathways that stimulate neurite outgrowth may provide insights into developing strategies to trigger the reconnection of injured neurons. The neuronal adaptor FE65 has been shown to interact with ARF6 and potentiate ARF6-mediated neurite outgrowth. However, the precise mechanism that FE65 activates ARF6 remains unclear, as FE65 does not possess a guanine nucleotide exchange factor (GEF) domain/function. Here, we show that FE65 interacts with the ARF6 GEF, namely the ARF nucleotide-binding site opener (ARNO). Moreover, a complex consisting of ARNO, ARF6 and FE65 is detected. Notably, FE65 potentiates the stimulatory effect of ARNO on ARF6-mediated neurite outgrowth, and the effect of FE65 is abrogated by an FE65 mutation that disrupts FE65–ARNO interaction. Additionally, the intramolecular interaction for mediating the autoinhibited conformation of ARNO is attenuated by FE65. Moreover, FE65 potentiates the effects of wild-type ARNO, but not the monomeric mutant, suggesting an association between FE65 and ARNO dimerization. Collectively, we demonstrate that FE65 binds to and activates ARNO and, consequently, potentiates ARF6-mediated neurite outgrowth.

Published

2022

94. WNK1/HSN2 mediates neurite outgrowth and differentiation via a OSR1/GSK3β-LHX8 pathway

Author

Masahiro, Shimizu and Hiroshi, Shibuya

Subjects

Alanine, Glycogen Synthase Kinase 3 beta, Multidisciplinary, Proline, WNK Lysine-Deficient Protein Kinase 1, LIM-Homeodomain Proteins, Neuronal Outgrowth, Cholinergic Agents, Humans, Hereditary Sensory and Autonomic Neuropathies, Protein Serine-Threonine Kinases, Transcription Factors

Abstract

With no lysine kinase 1 (WNK1) phosphorylates and activates STE20/SPS1-related proline-alanine-rich protein kinase (SPAK) and oxidative stress responsive kinase 1 (OSR1) to regulate ion homeostasis in the kidney. Mutations in WNK1 result in dysregulation of the WNK1-SPAK/OSR1 pathway and cause pseudohypoaldosteronism type II (PHAII), a form of hypertension. WNK1 is also involved in the autosomal recessive neuropathy, hereditary sensory and autonomic neuropathy type II (HSANII). Mutations in a neural-specific splice variant of WNK1 (HSN2) cause HSANII. However, the mechanisms underlying HSN2 regulation in neurons and effects of HSN2 mutants remain unclear. Here, we found that HSN2 regulated neurite outgrowth through OSR1 activation and glycogen synthase kinase 3β (GSK3β). Moreover, HSN2-OSR1 and HSN2-GSK3β signalling induced expression of LIM homeobox 8 (Lhx8), which is a key regulator of cholinergic neural function. The HSN2-OSR1/GSK3β-LHX8 pathway is therefore important for neurite outgrowth. Consistently, HSN2 mutants reported in HSANII patients suppressed SPAK and OSR1 activation and LHX8 induction. Interestingly, HSN2 mutants also suppressed neurite outgrowth by preventing interaction of between wild-type HSN2 and GSK3β. These results indicate that HSN2 mutants cause dysregulation of neurite outgrowth via GSK3β in the HSN2 and/or WNK1 pathways.

Published

2022

95. SLITRK1-mediated noradrenergic projection suppression in the neonatal prefrontal cortex

Author

Minoru Hatayama, Kei-ichi Katayama, Yukie Kawahara, Hayato Matsunaga, Noriko Takashima, Yoshimi Iwayama, Yoshifumi Matsumoto, Akinori Nishi, Takeo Yoshikawa, and Jun Aruga

Subjects

Male, Norepinephrine, Neuronal Outgrowth, Infant, Newborn, Neurites, Humans, Membrane Proteins, Prefrontal Cortex, Medicine (miscellaneous), Nerve Tissue Proteins, General Agricultural and Biological Sciences, Axons, General Biochemistry, Genetics and Molecular Biology

Abstract

SLITRK1 is an obsessive-compulsive disorder spectrum-disorders-ssociated gene that encodes a neuronal transmembrane protein. Here we show that SLITRK1 suppresses noradrenergic projections in the neonatal prefrontal cortex, and SLITRK1 functions are impaired by SLITRK1 mutations in patients with schizophrenia (S330A, a revertant of Homo sapiensspecific residue) and bipolar disorder (A444S). Slitrk1-KO newborns exhibit abnormal vocalizations, and their prefrontal cortices show excessive noradrenergic neurites and reduced Semaphorin3A expression, which suppresses noradrenergic neurite outgrowth in vitro. Slitrk1 can bind Dynamin1 and L1 family proteins (Neurofascin and L1CAM), as well as suppress Semaphorin3A-induced endocytosis. Neurofascin-binding kinetics is altered in S330A and A444S mutations. Consistent with the increased obsessive-compulsive disorder prevalence in males in childhood, the prefrontal cortex of male Slitrk1-KO newborns show increased noradrenaline levels, and serotonergic varicosity size. This study further elucidates the role of noradrenaline in controlling the development of the obsessive-compulsive disorder-related neural circuit., Communications Biology, 5 (1), art. no. 935

Published

2022

96. PRG3 and PRG5 C-Termini: Important Players in Early Neuronal Differentiation

Author

Nicola Brandt, Jan Philipp Willmer, Maurilyn S. Ayon-Olivas, Veronika Banicka, Martin Witt, Andreas Wree, Isabel Groß, Anne Gläser, Jens Hausmann, and Anja U. Bräuer

Subjects

Inorganic Chemistry, Neurons, Organic Chemistry, Brain, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, PRG3/LPPR1, PRG5/LPPR5, PRG4/LPPR2, neuronal outgrowth, hippocampal neurons, Hippocampus, Spectroscopy, Catalysis, Computer Science Applications

Abstract

The functional importance of neuronal differentiation of the transmembrane proteins’ plasticity-related genes 3 (PRG3) and 5 (PRG5) has been shown. Although their sequence is closely related, they promote different morphological changes in neurons. PRG3 was shown to promote neuritogenesis in primary neurons; PRG5 contributes to spine induction in immature neurons and the regulation of spine density and morphology in mature neurons. Both exhibit intracellularly located C-termini of less than 50 amino acids. Varying C-termini suggested that these domains shape neuronal morphology differently. We generated mutant EGFP-fusion proteins in which the C-termini were either swapped between PRG3 and PRG5, deleted, or fused to another family member, plasticity-related gene 4 (PRG4), that was recently shown to be expressed in different brain regions. We subsequently analyzed the influence of overexpression in immature neurons. Our results point to a critical role of the PRG3 and PRG5 C-termini in shaping early neuronal morphology. However, the results suggest that the C-terminus alone might not be sufficient for promoting the morphological effects induced by PRG3 and PRG5.

Published

2022

97. Insulin stimulates atypical protein kinase C-mediated phosphorylation of the neuronal adaptor FE65 to potentiate neurite outgrowth by activating ARF6-Rac1 signaling

Author

Dennis Dik‐Long Chau, Wen Li, Wai Wa Ray Chan, Jacquelyne Ka‐Li Sun, Yuqi Zhai, Hei‐Man Chow, and Kwok‐Fai Lau

Subjects

Neurons, rac1 GTP-Binding Protein, Neuronal Outgrowth, Neuropeptides, Nuclear Proteins, Nerve Tissue Proteins, Biochemistry, Mice, Glucose, ADP-Ribosylation Factor 6, Genetics, Neurites, Serine, Animals, Insulin, Phosphorylation, Molecular Biology, Protein Kinase C, Biotechnology

Abstract

Neurite outgrowth is a fundamental process in neurons that produces extensions and, consequently, neural connectivity. Neurite damage and atrophy are observed in various brain injuries and disorders. Understanding the intrinsic pathways of neurite outgrowth is essential for developing strategies to stimulate neurite regeneration. Insulin is a pivotal hormone in the regulation of glucose homeostasis. There is increasing evidence for the neurotrophic functions of insulin, including the induction of neurite outgrowth. However, the associated mechanism remains elusive. Here, we demonstrate that insulin potentiates neurite outgrowth mediated by the small GTPases ADP-ribosylation factor 6 (ARF6) and Ras-related C3 botulinum toxin substrate 1 (Rac1) through the neuronal adaptor FE65. Moreover, insulin enhances atypical protein kinase Cι/λ (PKCι/λ) activation and FE65 phosphorylation at serine 459 (S459) in neurons and mouse brains. In vitro and cellular assays show that PKCι/λ phosphorylated FE65 at S459. Consistently, insulin potentiates FE65 S459 phosphorylation only in the presence of PKCι/λ. Phosphomimetic studies show that an FE65 S459E mutant potently activates ARF6, Rac1, and neurite outgrowth. Notably, this phosphomimetic mutation enhances the FE65-ARF6 interaction, a process that promotes ARF6-Rac1-mediated neurite outgrowth. Likewise, insulin treatment and PKCι/λ overexpression potentiate the FE65-ARF6 interaction. Conversely, PKCι/λ knockdown suppresses the stimulatory effect of FE65 on ARF6-Rac1-mediated neurite outgrowth. The effect of insulin on neurite outgrowth is also markedly attenuated in PKCι/λ knockdown neurons, in the presence and absence of FE65. Our findings reveal a novel mechanism linking insulin with ARF6-Rac1-dependent neurite extension through the PKCι/λ-mediated phosphorylation of FE65.

Published

2022

98. Spirocyclohexadienone‐Type Neolignans with Neuroprotective and Neurite Outgrowth Enhancing Activities from Magnolia liliiflora

Author

Xing‐De Wu, Jian‐Lin Hu, Wei Nie, Ming Hu, Jin‐Da Li, Yi‐Fan Shen, Lin‐Fen Ding, and Liu‐Dong Song

Subjects

Neuronal Outgrowth, Bioengineering, General Chemistry, General Medicine, PC12 Cells, Biochemistry, Lignans, Rats, Magnolia, Nerve Growth Factor, Neurites, Animals, Molecular Medicine, Corticosterone, Molecular Biology

Abstract

Three rare spirocyclohexadienone-type neolignans, magnoflorins A-C (1-3), and three known analogs (4-6), were isolated from the leaves of Magnolia liliiflora. Magnoflorin D (4) was obtained from natural resources for the first time. The chemical structures and absolute configurations of 1-4 were elucidated through detailed analysis of HR-ESI-MS, IR

Published

2022

99. Involvement of strawberry notch homologue 1 in neurite outgrowth of cortical neurons

Author

Munkhsoyol Erkhembaatar, Iroha Yamamoto, Fuduki Inoguchi, Kosuke Taki, Satoru Yamagishi, Leanne Delaney, Nishibe Mariko, Takaya Abe, Hiroshi Kiyonari, Carina Hanashima, Hayato Naka‐kaneda, Dai Ihara, and Yu Katsuyama

Subjects

Cerebral Cortex, Mice, Knockout, Neurons, Nex-Cre, cortical neurons, Neuronal Outgrowth, Cell Biology, strawberry notch, Mice, cortical plate, Neurites, Animals, Humans, neurite growth, Cells, Cultured, Developmental Biology

Abstract

When the regulation of axonal and dendritic growth is altered, the neuronal network becomes disordered, which may contribute to the development of psychiatric disorders. Some genome analyses have suggested relationships between mutations in strawberry notch homologue 1 (SBNO1) and neurodevelopmental disorders. However, the function of SBNO1 has not yet been reported. Here, SBNO1 expression pattern during the development of the cerebral cortex in mice was examined. SBNO1 was strongly expressed in the cortical plate and its expression was maintained at a low level during the postnatal stage. CRISPR/Cas9-based knockout of Sbno1 in Neuro2A cultured cells showed delayed growth of neurites. A cortical neuron-specific conditional knockout mouse was constructed, which resulted in hypotrophy of axon bundles and dendrites in cortical neurons. Thus, when mutated, SBNO1 is a candidate gene for psychiatric diseases, such as schizophrenia, as suggested by human genome studies.

Published

2022

100. The cyclin G-associated kinase (GAK) inhibitor SGC-GAK-1 inhibits neurite outgrowth and synapse formation

Author

Jun Egawa, Reza K. Arta, Vance P. Lemmon, Melissa Muños-Barrero, Yan Shi, Michihiro Igarashi, and Toshiyuki Someya

Subjects

Cyclin G, Cellular and Molecular Neuroscience, Cyclins, Neuronal Outgrowth, Synapses, Cyclic GMP-Dependent Protein Kinases, Neurites, Protein Kinase Inhibitors, Molecular Biology

Abstract

Protein kinases are responsible for protein phosphorylation and are involved in important signal transduction pathways; however, a considerable number of poorly characterized kinases may be involved in neuronal development. Here, we considered cyclin G-associated kinase (GAK) as a candidate regulator of neurite outgrowth and synaptogenesis by examining the effects of the selective GAK inhibitor SGC-GAK-1. SGC-GAK-1 treatment of cultured neurons reduced neurite length and decreased synapse number and phosphorylation of neurofilament 200-kDa subunits relative to the control. In addition, the related kinase inhibitor erlotinib, which has distinct specificity and potency from SGC-GAK-1, had no effect on neurite growth, unlike SGC-GAK-1. These results suggest that GAK may be physiologically involved in normal neuronal development, and that decreased GAK function and the resultant impaired neurite outgrowth and synaptogenesis may be related to neurodevelopmental disorders.

Published

2022