Your search keyword '"glial cell"' showing total 1,034 results

1. Neuron-glia crosstalk and inflammatory mediators in migraine pathophysiology.

Author

Song, Yine, Zhao, Shaoru, Peng, Peiyue, Zhang, Chengcheng, Liu, Yuhan, Chen, Ying, Luo, Yuxi, Li, Bin, and Liu, Lu

Subjects

*SATELLITE cells, *PERIPHERAL nervous system, *NEUROGLIA, *SCHWANN cells, *CENTRAL nervous system, *MICROGLIA

Abstract

• Neuroinflammation significantly contributes to the pathophysiology and chronicity of migraines. • Microglia and astrocytes are central to neuroinflammatory responses in migraine development. • Cytokines and chemokines are important in glia-neuron crosstalk during migraine pathogenesis. • [11C] PBR28-targeted imaging and single-cell sequencing advance understanding of neuroinflammation mechanisms in migraine. • Estrogen and TRPM8 emerge as promising personalized therapeutic targets. Migraine is a complex neurological disorder with neuroinflammation playing a crucial role in its pathogenesis. This review provides an overview of the neuroinflammation mechanisms in migraine, focusing on both cellular and molecular aspects. At the cellular level, we examine the role of glial cells, including astrocytes, microglia, oligodendrocytes in the central nervous system, and Schwann cells and satellite glial cells in the peripheral nervous system. On the molecular level, we explore the signaling pathways, including IL-1β, TNF-α, IL-6, and non-coding RNAs, that mediate cell interactions or independent actions. Some of the molecular signaling pathways mentioned, such as TNF-α and IL-1β, have been investigated as druggable targets. Recent advancements, such as [11C] PBR28-targeted imaging for visualizing astrocyte activation and single-cell sequencing for exploring cellular heterogeneity, represent breakthroughs in understanding the mechanisms of neuroinflammation in migraine. By considering factors for personalized treatments, estrogen and TRPM8 emerge as promising therapeutic targets regarding sexual dimorphism. These advancements may help bridge the gap between preclinical findings and clinical applications, ultimately leading to more precise and personalized options for migraine patients. [ABSTRACT FROM AUTHOR]

Published

2024

2. Sigma-1 receptor targeting inhibits connexin 43 based intercellular communication in chronic neuropathic pain.

Author

Denaro, Simona, D'Aprile, Simona, Torrisi, Filippo, Zappalà, Agata, Marrazzo, Agostino, Al-Khrasani, Mahmoud, Pasquinucci, Lorella, Vicario, Nunzio, Parenti, Rosalba, and Parenti, Carmela

Subjects

*SIGMA-1 receptor, *CONNEXIN 43, *SUBCUTANEOUS injections, *CELL junctions, *NOCICEPTORS

Abstract

Background and objective: Neuropathic pain is a chronic condition characterized by aberrant signaling within the somatosensory system, affecting millions of people worldwide with limited treatment options. Herein, we aim at investigating the potential of a sigma-1 receptor (σ1R) antagonist in managing neuropathic pain. Methods: A Chronic Constriction Injury (CCI) model was used to induce neuropathic pain. The potential of (+)-MR200 was evaluated following daily subcutaneous injections of the compound. Its mechanism of action was confirmed by administration of a well-known σ1R agonist, PRE084. Results: (+)-MR200 demonstrated efficacy in protecting neurons from damage and alleviating pain hypersensitivity in CCI model. Our results suggest that (+)-MR200 reduced the activation of astrocytes and microglia, cells known to contribute to the neuroinflammatory process, suggesting that (+)-MR200 may not only address pain symptoms but also tackle the underlying cellular mechanism involved. Furthermore, (+)-MR200 treatment normalized levels of the gap junction (GJ)-forming protein connexin 43 (Cx43), suggesting a reduction in harmful intercellular communication that could fuel the chronicity of pain. Conclusions: This approach could offer a neuroprotective strategy for managing neuropathic pain, addressing both pain symptoms and cellular processes driving the condition. Understanding the dynamics of σ1R expression and function in neuropathic pain is crucial for clinical intervention. [ABSTRACT FROM AUTHOR]

Published

2024

3. Analgesic Effect of Human Placenta Hydrolysate on CFA-Induced Inflammatory Pain in Mice.

Author

Park, Keun-Tae, Jo, Heejoon, Jeon, So-Hyun, Jeong, Kyeongsoo, Im, Minju, Kim, Jae-Won, Jung, Jong-Pil, Jung, Hoe Chang, Lee, Jae hun, and Kim, Woojin

Subjects

*PERIPHERAL nervous system, *SPINAL cord, *NEUROGLIA, *GENE expression, *NEURALGIA

Abstract

To evaluate the efficacy of human placenta hydrolysate (HPH) in a mice model of CFA-induced inflammatory pain. TNF-α, IL-1β, and IL-6 are key pro-inflammatory cytokine factors for relieving inflammatory pain. Therefore, this study investigates whether HPH suppresses CFA-induced pain and attenuates the inflammatory process by regulating cytokines. In addition, the relationship between neuropathic pain and HPH was established by staining GFAP and Iba-1 in mice spinal cord tissues. This study was conducted for a total of day 28, and inflammatory pain was induced in mice by injecting CFA into the right paw at day 0 and day 14, respectively. 100 μL of 20% glucose and polydeoxyribonucleotide (PDRN) and 100, 200, and 300 μL of HPH were administered intraperitoneally twice a week. In the CFA-induced group, cold and mechanical allodynia and pro-inflammatory cytokine factors in the spinal cord and plantar tissue were significantly increased. The five groups of drugs evenly reduced pain and gene expression of inflammatory factors, and particularly excellent effects were confirmed in the HPH 200 and 300 groups. Meanwhile, the expression of GFAP and Iba-1 in the spinal cord was increased by CFA administration but decreased by HPH administration, which was confirmed to suppress damage to peripheral ganglia. The present study suggests that HPH attenuates CFA-induced inflammatory pain through inhibition of pro-inflammatory cytokine factors and protection of peripheral nerves. [ABSTRACT FROM AUTHOR]

Published

2024

4. Development of Mini-brain with Human Brain Cell Lines.

Author

Sung, Hailey

Subjects

CELL lines, ARTIFICIAL intelligence, ARTIFICIAL neural networks, MACHINE learning, NERVOUS system

Abstract

The human brain, a complex organ pivotal to the nervous system, orchestrates crucial functions for cognition and behavior. This research advances 3D brain cell modeling, overcoming traditional limitations. While mouse models present challenges in translatability to human brains, the evolution from non-invasive imaging to 3D culture models, specifically brain organoids, holds promise for understanding neurological disorders. Current limitations in 3D brain cell models, particularly the use of pluripotent stem cells, include high costs, extended development times, and a notable failure rate. In response, this study introduces a novel approach utilizing glial and neuron cells, significantly reducing costs and development time while maintaining a low failure rate. Experimental results demonstrate the successful creation and differentiation of 3D brain models, addressing key limitations. The developed mini-brain model, sustained for 21 days, exhibits resilience and responds differentially to glucose treatment, suggesting potential implications for brain morphology. Cell viability assessments confirm the predominantly live nature of the model, providing a foundation for future investigations. While limitations include a focus on two cell types and 21 days, future endeavors aim to diversify cell types and extend the maturation period. This research marks a significant stride in cost-effective, efficient, and ethical 3D brain modeling, laying the groundwork for continued exploration and comparison with established brain models. [ABSTRACT FROM AUTHOR]

Published

2024

5. Astrocyte dysregulation as an epileptogenic factor: a systematic review

Author

Komang Trisna Sumadewi, Bryan Gervais de Liyis, Ni Made Linawati, I Putu Eka Widyadharma, and I Nyoman Mantik Astawa

Subjects

Astrocyte, Dysregulation, Epilepsy, Glial cell, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Abstract Background Epilepsy initiation involves multifactorial etiologies, including genetic susceptibility, structural anomalies, and glial cell dysregulations, particularly in astrocytes. Despite advancements in understanding various factors, the mechanisms of astrocyte dysregulation in epilepsy, critical for neural homeostasis, remain elusive, requiring comprehensive evaluation of molecular pathways and cellular interactions for future targeted interventions. Methods A systematic search of PubMed, ScienceDirect, and the Cochrane databases up to January 1st 2024 identified relevant studies predominantly from experimental models, forming the basis for an in-depth analysis of astrocytic contributions to epileptic pathophysiology. The aims, subjects, epilepsy induction techniques, assessment methods, and findings of each studies were presented. Results A total of 24 clinical trials met the inclusion criteria and were included in the systematic review. Altered potassium buffering compromises extracellular potassium regulation, fostering hyperexcitability. Aquaporin dysfunction disrupts water homeostasis, aggravating seizure susceptibility. Disturbances in glutamatergic transmission, marked by changes in glutamate transporter function, contribute to excitotoxicity, fueling epileptogenesis. Intricacies in calcium signaling and disruptions in calcium-binding proteins tip intracellular calcium balance towards hyperexcitability. Dysfunctional GABA transporters compromise inhibitory neurotransmission, upsetting excitatory–inhibitory balance. Gap junction protein dysregulation disrupts astroglial networks, impacting neuronal synchronization in epileptogenic circuitry. Compromised BBB allows entry of epileptogenic factors, exacerbating the epileptogenic milieu. Conclusions Collectively, these astrocytic dysregulations unveil intricate contributors to epilepsy onset and progression.

Published

2024

6. Ferroptosis mechanism and Alzheimer's disease.

Author

Lina Feng, Jingyi Sun, Ling Xia, Qiang Shi, Yajun Hou, Lili Zhang, Mingquan Li, Cundong Fan, and Baoliang Sun

Published

2024

7. Exploring the vital role of microglial membrane receptors in Alzheimer’s disease pathogenesis: a comprehensive review.

Author

ZHAO, JUN-FENG, JIANG, YI-RAN, GUO, TIAN-LIN, JIAO, YONG-QING, and WANG, XUN

Subjects

*NEUROGLIA, *NEURODEGENERATION, *ANTI-inflammatory agents, *MICROGLIA, *PROTEIN receptors

Abstract

Neurodegenerative diseases constitute a broad category of diseases caused by the degeneration of the neurons. They are mainly manifested by the gradual loss of neuron structure and function and eventually can cause death or loss of neurons. As the global population ages rapidly, increased people are being diagnosed with neurodegenerative diseases. It has been established that the onset of Alzheimer’s disease (AD) is closely linked with increasing age and its major pathological features include amyloid-beta plaques (Aβ), Tau hyperphosphorylation, Neurofibrillary tangles (NFTs), neuronal death as well as synaptic loss. The involvement of microglia is crucial in the pathogenesis and progression of AD and exhibits a dual role. For instance, in the early stage of AD, microglia surface membrane proteins or receptors can participate in immunophagocytosis, and anti-inflammatory functions and act as a physical barrier after recognizing various ligands such as Aβ and NFTs. However, in the later stage of the disease, membrane receptors on the surface of microglia can cause its activation to release a substantial quantity of pro-inflammatory factors. Which can amplify the neuroinflammatory response. The rapid decline of normal immune phagocytosis can result in the continuous accumulation of abnormal proteins, leading to neuronal dysfunction and destruction of the formed physical barrier as well as the neurovascular microenvironment. It can also increase the transformation of microglia from anti-inflammatory phenotype M2 to pro-inflammatory phenotype M1, induce severe neuronal injury or apoptosis, and aggravate the progression of AD. Due to few articles have focused on the AD-related membrane protein receptors on microglia, thus in this paper, we have reviewed several representative microglial membrane proteins or receptors about their specific roles and functions implicated in AD, and expect that there will be more indepth research and scientific research results in the treatment of AD by targeted regulation of microglia membrane protein receptors in the future. [ABSTRACT FROM AUTHOR]

Published

2024

8. Astrocyte dysregulation as an epileptogenic factor: a systematic review.

Author

Sumadewi, Komang Trisna, de Liyis, Bryan Gervais, Linawati, Ni Made, Widyadharma, I Putu Eka, and Astawa, I Nyoman Mantik

Subjects

*CALCIUM-binding proteins, *GABA transporters, *GTPASE-activating protein, *GLUTAMATE transporters, *INTRACELLULAR calcium

Abstract

Background: Epilepsy initiation involves multifactorial etiologies, including genetic susceptibility, structural anomalies, and glial cell dysregulations, particularly in astrocytes. Despite advancements in understanding various factors, the mechanisms of astrocyte dysregulation in epilepsy, critical for neural homeostasis, remain elusive, requiring comprehensive evaluation of molecular pathways and cellular interactions for future targeted interventions. Methods: A systematic search of PubMed, ScienceDirect, and the Cochrane databases up to January 1st 2024 identified relevant studies predominantly from experimental models, forming the basis for an in-depth analysis of astrocytic contributions to epileptic pathophysiology. The aims, subjects, epilepsy induction techniques, assessment methods, and findings of each studies were presented. Results: A total of 24 clinical trials met the inclusion criteria and were included in the systematic review. Altered potassium buffering compromises extracellular potassium regulation, fostering hyperexcitability. Aquaporin dysfunction disrupts water homeostasis, aggravating seizure susceptibility. Disturbances in glutamatergic transmission, marked by changes in glutamate transporter function, contribute to excitotoxicity, fueling epileptogenesis. Intricacies in calcium signaling and disruptions in calcium-binding proteins tip intracellular calcium balance towards hyperexcitability. Dysfunctional GABA transporters compromise inhibitory neurotransmission, upsetting excitatory–inhibitory balance. Gap junction protein dysregulation disrupts astroglial networks, impacting neuronal synchronization in epileptogenic circuitry. Compromised BBB allows entry of epileptogenic factors, exacerbating the epileptogenic milieu. Conclusions: Collectively, these astrocytic dysregulations unveil intricate contributors to epilepsy onset and progression. [ABSTRACT FROM AUTHOR]

Published

2024

9. A review on the consequences of molecular and genomic alterations following exposure to electromagnetic fields: Remodeling of neuronal network and cognitive changes

Author

Shima Abtin, Fatemehsadat Seyedaghamiri, Zahra Aalidaeijavadi, Amir Mohammad Farrokhi, Fazel Moshrefi, Tayebeh Ziveh, Mohammad Ismail Zibaii, Hadi Aliakbarian, Mostafa Rezaei-Tavirani, and Abbas Haghparast

Subjects

Cognitive neuroscience, Electromagnetic field, Gene expression, Neuronal remodeling, Glial cell, Epigenetics, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The use of electromagnetic fields (EMFs) is essential in daily life. Since 1970, concerns have grown about potential health hazards from EMF. Exposure to EMF can stimulate nerves and affect the central nervous system, leading to neurological and cognitive changes. However, current research results are often vague and contradictory. These effects include changes in memory and learning through changes in neuronal plasticity in the hippocampus, synapses and hippocampal neuritis, and changes in metabolism and neurotransmitter levels. Prenatal exposure to EMFs has negative effects on memory and learning, as well as changes in hippocampal neuron density and histomorphology of hippocampus. EMF exposure also affects the structure and function of glial cells, affecting gate dynamics, ion conduction, membrane concentration, and protein expression. EMF exposure affects gene expression and may change epigenetic regulation through effects on DNA methylation, histone modification, and microRNA biogenesis, and potentially leading to biological changes. Therefore, exposure to EMFs possibly leads to changes in cellular and molecular mechanisms in central nervous system and alter cognitive function.

Published

2024

10. Editorial: 15 years of Frontiers in Cellular Neuroscience: the role of glial cells in schizophrenia and other related disorders

Author

Hai-Ying Shen

Subjects

glial cell, microglial, astrocyte, schizophrenia, neuroinflammation, neuropsychiatric disorders, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Published

2024

11. Mechanisms of Peripheral Sensitization in Neuropathic Pain

Author

Wen, Bei, Xu, Li, Huang, Yuguang, Ma, Chao, editor, and Huang, Yuguang, editor

Published

2024

12. Research progress on P2X7 receptor in cancer pain

Author

ZHANG Zhongwen, ZHAO Rui, ZHANG Haolong, YANG Yuting, BAI Jinxia, ZHANG Haoling WANG Wei

Subjects

p2x7 receptor, cancer pain, glial cell, p2x7 antagonist, Medicine

Abstract

The activation of the P2X7 receptor as an ATP-gated ion channel, triggers the release of pro-inflammatory cytokines in tumor carring individuals and stimulate excitation of injury-causing neurons, thereby exacerbating the transmission of pain. In preclinical cancer pain models, it has the potential to serve as a new therapeutic target for cancer pain management.

Published

2024

13. P2X7 受体在癌痛中作用的研究进展.

Author

张忠文, 赵瑞, 张浩龙, 杨钰婷, 白金霞, 张浩令, and 王薇

Abstract

The activation of the P2X7 receptor as an ATP-gated ion channel, triggers the release of pro-inflammatory cytokines in tumor carring individuals and stimulate excitation of injury-causing neurons, thereby exacerbating the transmission of pain. In preclinical cancer pain models, it has the potential to serve as a new therapeutic target for cancer pain management. [ABSTRACT FROM AUTHOR]

Published

2024

14. Endothelin-1-mediated Brainstem Glial Activation Produces Asthmatic Airway Vagal Hypertonia Via Enhanced ATP-P2X4 Receptor Signaling in Sprague–Dawley Rats.

Author

Lin, Yun, Liu, Tian, Chen, Hong, Zeng, Ming, Hu, Shunwei, Yu, Xiaoning, Chen, Yonghua, Xia, Chunmei, Wang, Jin, and Wang, Jijiang

Abstract

The occurrence of major asthma symptoms is largely attributed to airway vagal hypertonia, of which the central mechanisms remain unclear. This study tests the hypotheses that endothelin-1-mediated brainstem glial activation produces asthmatic airway vagal hypertonia via enhanced action of adenosine 5’-triphosphate on neuronal purinergic P2X4 receptors. A rat model of asthma was prepared using ovalbumin. Airway vagal tone was evaluated by the recurrent laryngeal discharge and plethysmographic measurement of pulmonary function. The changes in the brainstem were examined using ELISA, Western blot, luciferin-luciferase, quantitative reverse transcription-polymerase chain reaction, enzyme activity assay and immunofluorescent staining, respectively. The results showed that in the medulla of rats, endothelin receptor type B and P2X4 receptors were primarily expressed in astrocytes and neurons, respectively, and both of which, along with endothelin-1 content, were significantly increased after ovalbumin sensitization. Ovalbumin sensitization significantly increased recurrent laryngeal discharge, which was blocked by acute intracisternal injection of P2X4 receptor antagonist 5-BDBD, knockdown of brainstem P2X4 receptors, and chronic intraperitoneal injection of endothelin receptor type B antagonist BQ788, respectively. Ovalbumin sensitization activated microglia and astrocytes and significantly decreased ecto-5’-nucleotidase activity in the medulla, and all of which, together with the increase of medullary P2X4 receptor expression and decrease of pulmonary function, were reversed by chronic BQ788 treatment. These results demonstrated that in rats, allergic airway challenge activates both microglia and astrocytes in the medulla via enhanced endothelin-1/endothelin receptor type B signaling, which subsequently causes airway vagal hypertonia via augmented adenosine 5’-triphosphate/P2X4 receptor signaling in central neurons of airway vagal reflex. [ABSTRACT FROM AUTHOR]

Published

2024

15. Research progress of retinal neurovascular unit injury in glaucoma

Author

Ouyang Lingyi, He Tao, and Xing Yiqiao

Subjects

glaucoma, retinal neurovascular unit, retinal ganglion cell, glial cell, microvascular cell, Ophthalmology, RE1-994

Abstract

Glaucoma is one of the leading causes of vision loss worldwide. More and more studies have suggested that glaucoma is a complicated retinal neurovascular disease. The homeostasis imbalance of retinal neurovascular unit(RNVU)composed of neurons, glial cells and microvascular cells not only induces changes in microvascular structure and glial cells, but also affects the nerve tissue of the retina, resulting in vision loss, which there is no effective treatment to reverse, currently. Exploring the cellular composition and molecular structure of RNVU and investigating the destruction mechanism of normal cellular environment and intercellular connections in glaucoma are of great significance in exploring the pathogenesis and the treatment of glaucoma. The research progress on structural changes and dysfunction of RNVU in glaucoma are reviewed, hoping to provide new ideas for the treatment of glaucoma.

Published

2024

16. Analgesic Effect of Human Placenta Hydrolysate on CFA-Induced Inflammatory Pain in Mice

Author

Keun-Tae Park, Heejoon Jo, So-Hyun Jeon, Kyeongsoo Jeong, Minju Im, Jae-Won Kim, Jong-Pil Jung, Hoe Chang Jung, Jae hun Lee, and Woojin Kim

Subjects

human placenta hydrolysate, inflammatory pain, pro-inflammatory cytokine, glial cell, Medicine, Pharmacy and materia medica, RS1-441

Abstract

To evaluate the efficacy of human placenta hydrolysate (HPH) in a mice model of CFA-induced inflammatory pain. TNF-α, IL-1β, and IL-6 are key pro-inflammatory cytokine factors for relieving inflammatory pain. Therefore, this study investigates whether HPH suppresses CFA-induced pain and attenuates the inflammatory process by regulating cytokines. In addition, the relationship between neuropathic pain and HPH was established by staining GFAP and Iba-1 in mice spinal cord tissues. This study was conducted for a total of day 28, and inflammatory pain was induced in mice by injecting CFA into the right paw at day 0 and day 14, respectively. 100 μL of 20% glucose and polydeoxyribonucleotide (PDRN) and 100, 200, and 300 μL of HPH were administered intraperitoneally twice a week. In the CFA-induced group, cold and mechanical allodynia and pro-inflammatory cytokine factors in the spinal cord and plantar tissue were significantly increased. The five groups of drugs evenly reduced pain and gene expression of inflammatory factors, and particularly excellent effects were confirmed in the HPH 200 and 300 groups. Meanwhile, the expression of GFAP and Iba-1 in the spinal cord was increased by CFA administration but decreased by HPH administration, which was confirmed to suppress damage to peripheral ganglia. The present study suggests that HPH attenuates CFA-induced inflammatory pain through inhibition of pro-inflammatory cytokine factors and protection of peripheral nerves.

Published

2024

17. Energy optimisation predicts the capacity of ion buffering in the brain.

Author

Maex, Reinoud

Subjects

*INTRACELLULAR space, *ION sources, *EXTRACELLULAR space, *CONCENTRATION gradient, *NEUROGLIA

Abstract

Neurons store energy in the ionic concentration gradients they build across their cell membrane. The amount of energy stored, and hence the work the ions can do by mixing, can be enhanced by the presence of ion buffers in extra- and intracellular space. Buffers act as sources and sinks of ions, however, and unless the buffering capacities for different ion species obey certain relationships, a complete mixing of the ions may be impeded by the physical conditions of charge neutrality and isotonicity. From these conditions, buffering capacities were calculated that enabled each ion species to mix completely. In all valid buffer distributions, the Ca 2 + ions were buffered most, with a capacity exceeding that of Na + and K + buffering by at least an order of magnitude. The similar magnitude of the (oppositely directed) Na + and K + gradients made extracellular space behave as a Na + – K + exchanger. Anions such as Cl - were buffered least. The great capacity of the extra- and intracellular Ca 2 + buffers caused a large influx of Ca 2 + ions as is typically observed during energy deprivation. These results explain many characteristics of the physiological buffer distributions but raise the question how the brain controls the capacity of its ion buffers. It is suggested that neurons and glial cells, by their great sensitivity to gradients of charge and osmolarity, respectively, sense deviations from electro-neutral and isotonic mixing, and use these signals to tune the chemical composition, and buffering capacity, of the extra- and intracellular matrices. [ABSTRACT FROM AUTHOR]

Published

2023

18. A basement membrane extract-based three-dimensional culture system promotes the neuronal differentiation of cochlear Sox10-positive glial cells in vitro

Author

Junze Lu, Man Wang, Xue Wang, Yu Meng, Fang Chen, Jinzhu Zhuang, Yuechen Han, Haibo Wang, and Wenwen Liu

Subjects

Hearing loss, Spiral ganglion neuron, Glial cell, Differentiation, Basement membrane extract-based three-dimensional culture, Sox10, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Spiral ganglion neurons (SGNs) in the mammalian cochleae are essential for the delivery of acoustic information, and damage to SGNs can lead to permanent sensorineural hearing loss as SGNs are not capable of regeneration. Cochlear glial cells (GCs) might be a potential source for SGN regeneration, but the neuronal differentiation ability of GCs is limited and its properties are not clear yet. Here, we characterized the cochlear Sox10-positive (Sox10+) GCs as a neural progenitor population and developed a basement membrane extract-based three-dimensional (BME-3D) culture system to promote its neuronal generation capacity in vitro. Firstly, the purified Sox10+ GCs, isolated from Sox10-creER/tdTomato mice via flow cytometry, were able to form neurospheres after being cultured in the traditional suspension culture system, while significantly more neurospheres were found and the expression of stem cell-related genes was upregulated in the BME-3D culture group. Next, the BME-3D culture system promoted the neuronal differentiation ability of Sox10+ GCs, as evidenced by the increased number, neurite outgrowth, area of growth cones, and synapse density as well as the promoted excitability of newly induced neurons. Notably, the BME-3D culture system also intensified the reinnervation of newly generated neurons with HCs and protected the neurospheres and derived-neurons against cisplatin-induced damage. Finally, transcriptome sequencing analysis was performed to identify the characteristics of the differentiated neurons. These findings suggest that the BME-3D culture system considerably promotes the proliferation capacity and neuronal differentiation efficiency of Sox10+ GCs in vitro, thus providing a possible strategy for the SGN regeneration study.

Published

2024

19. Persistent neuroinflammation of the right insular cortex in children with juvenile idiopathic arthritis: a proton MRS study.

Author

Han, Haiwei, Weng, Yifei, Liang, Hongyan, Yi, Cuili, Lin, Kezhao, Wu, Hua, Xiao, Jihong, and Han, Chengkun

Subjects

*JUVENILE idiopathic arthritis, *INSULAR cortex, *PROTON magnetic resonance spectroscopy, *NEUROINFLAMMATION, *SLEEP interruptions

Abstract

Objective: The aim of this study of children with juvenile idiopathic arthritis (JIA) was to use proton magnetic resonance spectroscopy (1H-MRS) to compare the levels of five neurometabolites in the right and left insular cortexes of subjects in three groups: JIA-active, JIA-inactive, and healthy controls (HCs). Methods: Two inflammation markers and five psychometric scores were determined. 1H-MRS was used to measure the levels of total N-acetylaspartate (NAA), total choline (Cho), myo-inositol (mI), and glutamate (Glu), and the complex of glutamine and glutamate (Glx) relative to total creatine (tCr) in the right and left insular cortexes of participants. Results: Intra-group comparisons indicated that each group had higher levels of NAA/tCr, Glu/tCr, Glx/tCr, and mI/tCr in the right insula, and higher levels of Cho/tCr in the left insula. Inter-group comparisons of the right insula indicated that the JIA-active and JIA-inactive groups had higher levels of Cho/tCr than the HC group, but none of the other inter-group differences were statistically significant. The score of the Sleep Disturbance Scale for Children (SDCD) had an inverse correlation with the level of Cho/tCr in the right insular cortex of patients in the JIA-inactive group. Conclusions: Relative to the HC group, the right insular cortex of subjects in the JIA-active and the JIA-inactive groups had greater levels of Cho/tCr, suggesting increased inflammation in this region. The Cho/tCr level in the right insular cortex had an inverse correlation with SDCD score in the JIA-inactive group. Key Points • Healthy controls and JIA patients had higher levels of tNAA/tCr, Glu/tCr, Glx/tCr, and mI/tCr in the right insula, and higher levels of Cho/tCr in the left insula. • A greater level of Cho/tCr in the right insula of JIA-active and JIA-inactive patients indicated neuroinflammation in this region. • The Cho/tCr level in the right insular cortex had an inverse correlation with SDCD score in the JIA-inactive group. [ABSTRACT FROM AUTHOR]

Published

2023

20. PKM2 Nuclear Translocation Promotes Glial Cell Activation and Aggravates the Brain Injury of Intracerebral Hemorrhage.

Author

Xiao-Yi Xiong, Yan-Jing Liang, Xin-Xiao Zhang, Su-Hao Yang, Zhan-Qiong Zhong, Shu-Qing Liu, Jia-Yi Sun, Yong Tang, and Shu-Guang Yu

Subjects

*NEUROGLIA, *BRAIN injuries, *CEREBRAL hemorrhage, *GLIAL fibrillary acidic protein, *HEMATOXYLIN & eosin staining

Abstract

Background: The purpose of this study was to investigate the potential involvement of pyruvate kinase M2 (PKM2), an enzyme acting as a rate-limiting enzyme in the final phase of glycolysis, in the regulation of glial activation and brain damage of intracerebral hemorrhage (ICH). Methods: Western blotting and immunofluorescence were performed to investigate PKM2 expression, terminal deoxynucleotidyl transferase deoxyurinary triphosphate (dUTP) nick end labeling staining, hematoxylin and eosin staining, and behavioral tests were employed to evaluate the brain damage of ICH mice, and RNA-seq and bioinformatic analyses were performed to detect gene expression changes in ICH mice treated with TEPP-46. Results: Increased PKM2 levels in perihematomal brain tissue were found starting from 3 days following ICH and peaked at 5 and 7 days post ICH. The increased expression of PKM2 was mainly co-localized with glial fibrillary acidic protein (GFAP)+ astrocytes and ionized calcium binding adaptor molecule-1 (IBA-1)+ microglia. Furthermore, we observed a notable increase in the nuclear translocation of PKM2 in glial cells following ICH. TEPP-46 treatment significantly reduced PKM2 nuclear translocation, and effectively attenuated glial activation and brain injury, and improved functional recovery of mice with ICH. RNA-seq data indicated that 91.1% (205/225) of differentially expressed genes (DEGs) were down-regulated in the TEPP-46 treated groups compared with the vehicle-treated groups in ICH brains. Furthermore, bioinformatic analyses revealed that these down-regulated DEGs were involved in a variety of biological processes, including autophagy and metabolic processes. In addition, the majority of these downregulated DEGs had a primary high expression in neurons, with subsequent expression seen in endothelial cells, microglia, and astrocytes. Conclusions: These results indicate that increased PKM2 nuclear translocation promotes the activation of glial cells after ICH, hence aggravating ICH-induced brain damage, and aggravates the brain injury induced by ICH. This highlights a potential therapeutic target for inhibiting glial activation to attenuate brain injury after ICH. [ABSTRACT FROM AUTHOR]

Published

2023

21. Single-cell RNAseq analysis of spinal locomotor circuitry in larval zebrafish

Author

Jimmy J Kelly, Hua Wen, and Paul Brehm

Subjects

transcriptomics, synaptic transmission, ion channels, glial cell, neurons, Medicine, Science, Biology (General), QH301-705.5

Abstract

Identification of the neuronal types that form the specialized circuits controlling distinct behaviors has benefited greatly from the simplicity offered by zebrafish. Electrophysiological studies have shown that in addition to connectivity, understanding of circuitry requires identification of functional specializations among individual circuit components, such as those that regulate levels of transmitter release and neuronal excitability. In this study, we use single-cell RNA sequencing (scRNAseq) to identify the molecular bases for functional distinctions between motoneuron types that are causal to their differential roles in swimming. The primary motoneuron, in particular, expresses high levels of a unique combination of voltage-dependent ion channel types and synaptic proteins termed functional ‘cassettes.’ The ion channel types are specialized for promoting high-frequency firing of action potentials and augmented transmitter release at the neuromuscular junction, both contributing to greater power generation. Our transcriptional profiling of spinal neurons further assigns expression of this cassette to specific interneuron types also involved in the central circuitry controlling high-speed swimming and escape behaviors. Our analysis highlights the utility of scRNAseq in functional characterization of neuronal circuitry, in addition to providing a gene expression resource for studying cell type diversity.

Published

2023

22. Complement factor B is essential for the proper function of the peripheral auditory system.

Author

Brown, LaShardai N., Barth, Jeremy L., Jafri, Shabih, Rumschlag, Jeffrey A., Jenkins, Tyreek R., Atkinson, Carl, and Hainan Lang

Subjects

AUDITORY pathways, MACULAR degeneration, SENSORINEURAL hearing loss, NEURAL crest, ACOUSTIC nerve, PHAGOCYTOSIS

Abstract

Sensorineural hearing loss is associated with dysfunction of cochlear cells. Although immune cells play a critical role in maintaining the inner ear microenvironment, the precise immune-related molecular mechanisms underlying the pathophysiology of hearing loss remain unclear. The complement cascade contributes to the regulation of immune cell activity. Additionally, activation of the complement cascade can lead to the cellular opsonization of cells and pathogens, resulting in their engulfment and elimination by phagocytes. Complement factor B (fB) is an essential activator protein in the alternative complement pathway, and variations in the fB gene are associated with age-related macular degeneration. Here we show that mice of both sexes deficient in fB functional alleles (fB-/-) demonstrate progressive hearing impairment. Transcriptomic analysis of auditory nerves from adult mice detected 706 genes that were significantly differentially expressed between fB-/- and wild-type control animals, including genes related to the extracellular matrix and neural development processes. Additionally, a subset of differentially expressed genes was related to myelin function and neural crest development. Histological and immunohistochemical investigations revealed pathological alterations in auditory nerve myelin sheathes of fB-/- mice. Pathological alterations were also seen in the stria vascularis of the cochlear lateral wall in these mice. Our results implicate fB as an integral regulator of myelin maintenance and stria vascularis integrity, underscoring the importance of understanding the involvement of immune signaling pathways in sensorineural hearing loss. [ABSTRACT FROM AUTHOR]

Published

2023

23. Blended Glial Cell’s Spiking Neural Network

Author

Liying Tao, Pan Li, Meihua Meng, Zonglin Yang, Xiaozhuang Liu, Jinhua Hu, Ji Dong, Shushan Qiao, Tianchun Ye, and Delong Shang

Subjects

Glial cell, spiking neural networks, spatiotemporal information integration, sudoku solver, Electrical engineering. Electronics. Nuclear engineering, TK1-9971

Abstract

Spiking Neural Networks (SNNs), the third generation of artificial neural networks, have been widely employed. However, the realization of advanced artificial intelligence is challenging due to the dearth of efficient spatiotemporal information integration models. Inspired by brain neuroscientists, this paper proposes a novel spiking neural network - Blended Glial Cell’s Spiking Neural Network (BGSNN). BGSNN introduces glial cells as spatiotemporal information processing units based on neurons and synapses, and also provides four new network dynamics connection models which extend the information processing dimension, enhance the network global information integration in the spatiotemporal domain, as well as the plasticity of neurons and synapses. In this paper, a BGSNN application - Sudoku solver is designed and implemented on the “WenTian” neuromorphic prototype. On the Easybrain dataset, the BGSNN solver achieves 100% accuracy, outperforming the same structure SNN solver by 97% at the Evil difficulty level, and has faster converges speed compared with the SOTA Sudoku solver LSGA. On the kaggle dataset, the BGSNN solver achieves over 99.99% accuracy, outperforming the publicly available optimal DNN solver under this dataset by 3.82%. In addition, BGSNN exhibits good parallelism and sparsity, decreasing computation by at least 92.9% compared to serial solvers and reducing sparsity by 88% compared to the equal fully dense DNN. BGSNN improves the expression, feedback, and regulation capabilities of neural networks while maintaining the advantages of SNN parallel sparsity, making it simpler to implement advanced artificial intelligence.

Published

2023

24. General Principles of Ophthalmic Pathology

Author

Syed, Nasreen A., Albert, Daniel M., Garner, Alec, White, Valerie A., Stagner, Anna M., Section editor, Wolkow, Natalie, Section editor, Dryja, Thaddeus, Section editor, Jakobiec, Frederick A., Section editor, Albert, Daniel M., editor, Miller, Joan W., editor, Azar, Dimitri T., editor, and Young, Lucy H., editor

Published

2022

25. Biology of Motivation, Dopamine, and Brain Circuits That Mediate Pleasure

Author

Freed, William J. and Freed, William J.

Published

2022

26. Normalization of Neuroinflammation: A New Strategy for Treatment of Persistent Pain and Memory/Emotional Deficits in Chronic Pain

Author

Liu XG

Subjects

ion channels, synaptic plasticity, cytokine, glial cell, monocytes, Pathology, RB1-214, Therapeutics. Pharmacology, RM1-950

Abstract

Xian-Guo Liu Pain Research Center and Department of Physiology, Zhongshan School of Medicine of Sun Yat-sen University, Guangzhou, People’s Republic of ChinaCorrespondence: Xian-Guo Liu, Pain Research Center and Department of Physiology, Zhongshan School of Medicine of Sun Yat-sen University, 74 Zhongshan Road2, Hemulou 806, Guangzhou, 510080, People’s Republic of China, Tel/Fax +86 87331956, Email liuxg@mail.sysu.edu.cnAbstract: Chronic pain, which affects around 1/3 of the world population and is often comorbid with memory deficit and mood depression, is a leading source of suffering and disability. Studies in past decades have shown that hyperexcitability of primary sensory neurons resulting from abnormal expression of ion channels and central sensitization mediated pathological synaptic plasticity, such as long-term potentiation in spinal dorsal horn, underlie the persistent pain. The memory/emotional deficits are associated with impaired synaptic connectivity in hippocampus. Dysregulation of numerous endogenous proteins including receptors and intracellular signaling molecules is involved in the pathological processes. However, increasing knowledge contributes little to clinical treatment. Emerging evidence has demonstrated that the neuroinflammation, characterized by overproduction of pro-inflammatory cytokines and glial activation, is reliably detected in humans and animals with chronic pain, and is sufficient to induce persistent pain and memory/emotional deficits. The abnormal expression of ion channels and pathological synaptic plasticity in spinal dorsal horn and in hippocampus are resulting from neuroinflammation. The neuroinflammation is initiated and maintained by the interactions of circulating monocytes, glial cells and neurons. Obviously, unlike infectious diseases and cancer, which are caused by pathogens or malignant cells, chronic pain is resulting from alterations of cells and molecules which have numerous physiological functions. Therefore, normalization (counterbalance) but not simple inhibition of the neuroinflammation is the right strategy for treating neuronal disorders. Currently, no such agent is available in clinic. While experimental studies have demonstrated that intracellular Mg2+ deficiency is a common feature of chronic pain in animal models and supplement Mg2+ are capable of normalizing the neuroinflammation, activation of upregulated proteins that promote recovery, such as translocator protein (18k Da) or liver X receptors, has a similar effect. In this article, relevant experimental and clinical evidence is reviewed and discussed.Keywords: ion channels, synaptic plasticity, cytokine, glial cell, monocytes

Published

2022

27. Inflammation in pathogenesis of chronic pain: Foe and friend.

Author

Fang, Xiao-Xia, Zhai, Meng-Nan, Zhu, Meixuan, He, Cheng, Wang, Heng, Wang, Juan, and Zhang, Zhi-Jun

Abstract

Chronic pain is a refractory health disease worldwide causing an enormous economic burden on individuals and society. Accumulating evidence suggests that inflammation in the peripheral nervous system (PNS) and central nervous system (CNS) is the major factor in the pathogenesis of chronic pain. The inflammation in the early- and late phase may have distinctive effects on the initiation and resolution of pain, which can be viewed as friend or foe. On the one hand, painful injuries lead to the activation of glial cells and immune cells in the PNS, releasing pro-inflammatory mediators, which contribute to the sensitization of nociceptors, leading to chronic pain; neuroinflammation in the CNS drives central sensitization and promotes the development of chronic pain. On the other hand, macrophages and glial cells of PNS and CNS promote pain resolution via anti-inflammatory mediators and specialized pro-resolving mediators (SPMs). In this review, we provide an overview of the current understanding of inflammation in the deterioration and resolution of pain. Further, we summarize a number of novel strategies that can be used to prevent and treat chronic pain by controlling inflammation. This comprehensive view of the relationship between inflammation and chronic pain and its specific mechanism will provide novel targets for the treatment of chronic pain. [ABSTRACT FROM AUTHOR]

Published

2023

28. Non-neutralizing antibodies to SARS-Cov-2-related linear epitopes induce psychotic-like behavior in mice.

Author

Jinming Xu, Hui Wei, Pengsheng You, Jiaping Sui, Jianbo Xiu, Wanwan Zhu, and Qi Xu

Subjects

SARS-CoV-2, NEUROGLIA, COVID-19, IMMUNOGLOBULINS, NEURAL inhibition

Abstract

Objective: An increasing number of studies have reported that numerous patients with coronavirus disease 2019 (COVID-19) and vaccinated individuals have developed central nervous system (CNS) symptoms, and that most of the antibodies in their sera have no virus-neutralizing ability. We tested the hypothesis that non-neutralizing anti-S1-111 IgG induced by the spike protein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) could negatively affect the CNS. Methods: After 14-day acclimation, the grouped ApoE-/- mice were immunized four times (day 0, day 7, day 14, day 28) with different spike-protein-derived peptides (coupled with KLH) or KLH via subcutaneous injection. Antibody level, state of glial cells, gene expression, prepulse inhibition, locomotor activity, and spatial working memory were assessed from day 21. Results: An increased level of anti-S1-111 IgG was measured in their sera and brain homogenate after the immunization. Crucially, anti-S1-111 IgG increased the density of microglia, activated microglia, and astrocytes in the hippocampus, and we observed a psychomotor-like behavioral phenotype with defective sensorimotor gating and impaired spontaneity among S1-111-immunized mice. Transcriptome profiling showed that up-regulated genes in S1-111-immunized mice were mainly associated with synaptic plasticity and mental disorders. Discussion: Our results show that the non-neutralizing antibody anti-S1-111 IgG induced by the spike protein caused a series of psychotic-like changes in model mice by activating glial cells and modulating synaptic plasticity. Preventing the production of anti-S1-111 IgG (or other non-neutralizing antibodies) may be a potential strategy to reduce CNS manifestations in COVID-19 patients and vaccinated individuals. [ABSTRACT FROM AUTHOR]

Published

2023

29. Concise review: Current understanding of extracellular vesicles to treat neuropathic pain.

Author

Kexin Zhang, Pei Li, Yuanyuan Jia, Ming Liu, and Jingjing Jiang

Subjects

NEURAL transmission, EXOSOMES, NEURALGIA, CELL physiology, RNA, MACROPHAGES, MOLECULAR biology, NEUROINFLAMMATION, CELL communication, DNA methylation, TRANSFERASES, NEUROGLIA, EXTRACELLULAR vesicles

Abstract

Extracellular vesicles (EVs) including exosomes are vesicular vesicles with phospholipid bilayer implicated in many cellular interactions and have the ability to transfer multiple types of cargo to cells. It has been found that EVs can package various molecules including proteins and nucleic acids (DNA, mRNA, and noncoding RNA). The discovery of EVs as carriers of proteins and various forms of RNA, such as microRNAs (miRNA) and long noncoding RNAs (lncRNA), has raised great interest in the field of drug delivery. Despite the underlying mechanisms of neuropathic pain being unclear, it has been shown that uncontrolled glial cell activation and the neuroinflammation response to noxious stimulation are important in the emergence and maintenance of neuropathic pain. Many studies have demonstrated a role for noncoding RNAs in the pathogenesis of neuropathic pain and EVs may offer possibilities as carriers of noncoding RNAs for potential in neuropathic pain treatment. In this article, the origins and clinical application of EVs and the mechanism of neuropathic pain development are briefly introduced. Furthermore, we demonstrate the therapeutic roles of EVs in neuropathic pain and that this involve vesicular regulation of glial cell activation and neuroinflammation. [ABSTRACT FROM AUTHOR]

Published

2023

30. Changes to GFAP Immunoreactive Astrocytes in Medial Prefrontal Cortex Following Exposure to Chronic Stress and Antioxidant Supplementation in Rat Model.

Author

Asari, Mohd Asnizam, Nawi, Faizah Md, Mohd Amin, Mohammad Syabil Ikhwan, Yusof, Nurul Aiman Mohd, and Sirajudeen, K. N. S.

Subjects

*PSYCHOLOGICAL stress, *PREFRONTAL cortex, *ASTROCYTES, *ANIMAL disease models, *DIETARY supplements

Abstract

Introduction: Astrocytes are responsible for many essential functions of neurons in CNS. It has been recognised that chronic stress affects the morphology of astrocyte. Natural antioxidant such as honey has been used as one of the therapeutic strategies to lessen the damaging effect of chronic stress on our body. Therefore, the aim of the study is to explore the effect of natural antioxidant, Tualang honey (TH) on the morphology of astrocytes following chronic stress exposure. Methods: Thirty-two male rats were randomly divided into the 4 groups: (i) control, (ii) stress, (iii) honey, (iv) stress plus honey groups. TH was administered via oral gavage at dose of 1.0 g/kg body weight pre and post experiment. Chronic stress was exposed to animals in group (ii) and (iv) for consecutive 21 days. Anti GFAP immunohistochemistry method was employed to label astrocytes in the medial prefrontal cortex. The number of GFAP+ astrocytes and several parameters related to astrocyte processes were measured. Results: The present study showed that chronic stress reduced the GFAP immunoreactive astrocyte number and percentage of GFAP immunoreactive material. Chronic stress also caused a reduction in astrocyte process ramification as indicated by a reduction in astrocyte total number of processes, average length of processes and maximum number of intersections. However, antioxidant treatment using TH could not reverse these stress-induced changes to the astrocytes. Conclusion: These results demonstrate that chronic stress decreases the number of GFAP immunoreactive astrocyte and cause shrinking of astrocyte processes in stress-sensitive brain region, but these changes cannot be reversed by antioxidant treatment. [ABSTRACT FROM AUTHOR]

Published

2023

31. Complement factor B is essential for the proper function of the peripheral auditory system

Author

LaShardai N. Brown, Jeremy L. Barth, Shabih Jafri, Jeffrey A. Rumschlag, Tyreek R. Jenkins, Carl Atkinson, and Hainan Lang

Subjects

cochlea, complement factor B, macrophage, auditory nerve, glial cell, myelination, Neurology. Diseases of the nervous system, RC346-429

Abstract

Sensorineural hearing loss is associated with dysfunction of cochlear cells. Although immune cells play a critical role in maintaining the inner ear microenvironment, the precise immune-related molecular mechanisms underlying the pathophysiology of hearing loss remain unclear. The complement cascade contributes to the regulation of immune cell activity. Additionally, activation of the complement cascade can lead to the cellular opsonization of cells and pathogens, resulting in their engulfment and elimination by phagocytes. Complement factor B (fB) is an essential activator protein in the alternative complement pathway, and variations in the fB gene are associated with age-related macular degeneration. Here we show that mice of both sexes deficient in fB functional alleles (fB−/−) demonstrate progressive hearing impairment. Transcriptomic analysis of auditory nerves from adult mice detected 706 genes that were significantly differentially expressed between fB−/− and wild-type control animals, including genes related to the extracellular matrix and neural development processes. Additionally, a subset of differentially expressed genes was related to myelin function and neural crest development. Histological and immunohistochemical investigations revealed pathological alterations in auditory nerve myelin sheathes of fB−/− mice. Pathological alterations were also seen in the stria vascularis of the cochlear lateral wall in these mice. Our results implicate fB as an integral regulator of myelin maintenance and stria vascularis integrity, underscoring the importance of understanding the involvement of immune signaling pathways in sensorineural hearing loss.

Published

2023

32. Glial-dependent clustering of voltage-gated ion channels in Drosophila precedes myelin formation

Author

Simone Rey, Henrike Ohm, Frederieke Moschref, Dagmar Zeuschner, Marit Praetz, and Christian Klämbt

Subjects

glial cell, myelin, axon initial segment, voltage-gated ion channel, Medicine, Science, Biology (General), QH301-705.5

Abstract

Neuronal information conductance often involves the transmission of action potentials. The spreading of action potentials along the axonal process of a neuron is based on three physical parameters: the axial resistance of the axon, the axonal insulation by glial membranes, and the positioning of voltage-gated ion channels. In vertebrates, myelin and channel clustering allow fast saltatory conductance. Here, we show that in Drosophila melanogaster voltage-gated sodium and potassium channels, Para and Shal, co-localize and cluster in an area resembling the axon initial segment. The local enrichment of Para but not of Shal localization depends on the presence of peripheral wrapping glial cells. In larvae, relatively low levels of Para channels are needed to allow proper signal transduction and nerves are simply wrapped by glial cells. In adults, the concentration of Para increases and is prominently found at the axon initial segment of motor neurons. Concomitantly, these axon domains are covered by a mesh of glial processes forming a lacunar structure that possibly serves as an ion reservoir. Directly flanking this domain glial processes forming the lacunar area appear to collapse and closely apposed stacks of glial cell processes can be detected, resembling a myelin-like insulation. Thus, Drosophila development may reflect the evolution of myelin which forms in response to increased levels of clustered voltage-gated ion channels.

Published

2023

33. Evidence of persistent glial cell dysfunction in the anterior cingulate cortex of juvenile idiopathic arthritis children: a proton MRS study

Author

Haiwei Han, Ji Hong Xiao, Yifei Weng, Hongyan Liang, Chengkun Han, Cuili Yi, Kezhao Lin, and Hua Wu

Subjects

Anterior cingulate cortex, Juvenile idiopathic arthritis, Glial cell, Proton magnetic resonance spectroscopy, Pediatrics, RJ1-570, Diseases of the musculoskeletal system, RC925-935

Abstract

Abstract Background This study aims to investigate whether the neurometabolites of the anterior cingulate cortex (ACC) were distinct in patients with active and inactive juvenile idiopathic arthritis (JIA) using the proton magnetic resonance spectroscopy. Methods We measured the levels of total N-acetylaspartate (tNAA), choline (Cho), myo-inositol (ml), glutamate (Glu) and the complex of glutamate and glutamine (Glx) relative to total creatine (tCr) in ACC of each participant. Results Compared with the healthy controls, a significant decrease of total Cho/tCr and Glx/tCr ratio in ACC occurred in active and inactive JIA group. The tCho/Cr level was negatively associated with the serum level of ESR in active JIA patients. There was no difference in NAA/tCr ratio among the three groups, which may imply that no neuron and axonal losses occurred in either active or inactive JIA patients. Conclusions The abnormal neurometabolites in tCho/tCr and Glx/tCr in ACC may indicate that persistent dysfunction of glial cell, while neither neuron nor axonal losses occurred in active and inactive JIA patients.

Published

2022

34. Editorial: New insights into the role of neuroinflammation and glial cells in the development of neurological disorders

Author

Marta Pérez-González, Maite Solas, Yixing Wu, and Virginia Mela

Subjects

neuroinflammation, glial cell, microglia activation, astrogliosis, neurodegeneration, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Published

2023

35. Regulatory role of the endocannabinoid system on glial cells toward cognitive function in Alzheimer’s disease: A systematic review and meta-analysis of animal studies

Author

Mohd Amir Kamaruzzaman, Muhammad Hibatullah Romli, Razif Abas, Sharmili Vidyadaran, Mohamad Taufik Hidayat Baharuldin, Muhammad Luqman Nasaruddin, Vishnumukkala Thirupathirao, Sreenivasulu Sura, Kabul Warsito, Nurul Huda Mohd Nor, Muhammad Amsyar Azwaruddin, Mohammed Abdullah Alshawsh, and Mohamad Aris Mohd Moklas

Subjects

Alzheimer’s disease, cognition, dementia, endocannabinoid, glial cell, microglia, Therapeutics. Pharmacology, RM1-950

Abstract

Objective: Over the last decade, researchers have sought to develop novel medications against dementia. One potential agent under investigation is cannabinoids. This review systematically appraised and meta-analyzed published pre-clinical research on the mechanism of endocannabinoid system modulation in glial cells and their effects on cognitive function in animal models of Alzheimer’s disease (AD).Methods: A systematic review complying with PRISMA guidelines was conducted. Six databases were searched: EBSCOHost, Scopus, PubMed, CINAHL, Cochrane, and Web of Science, using the keywords AD, cannabinoid, glial cells, and cognition. The methodological quality of each selected pre-clinical study was evaluated using the SYRCLE risk of bias tool. A random-effects model was applied to analyze the data and calculate the effect size, while I2 and p-values were used to assess heterogeneity.Results: The analysis included 26 original articles describing (1050 rodents) with AD-like symptoms. Rodents treated with cannabinoid agonists showed significant reductions in escape latency (standard mean difference [SMD] = −1.26; 95% confidence interval [CI]: −1.77 to −0.76, p < 0.00001) and ability to discriminate novel objects (SMD = 1.40; 95% CI: 1.04 to 1.76, p < 0.00001) compared to the control group. Furthermore, a significant decrease in Aβ plaques (SMD = −0.91; 95% CI: −1.55 to −0.27, p = 0.006) was observed in the endocannabinoid-treated group compared to the control group. Trends were observed toward neuroprotection, as represented by decreased levels of glial cell markers including glial fibrillary acid protein (SMD = −1.47; 95% CI: −2.56 to −0.38, p = 0.008) and Iba1 (SMD = −1.67; 95% CI: −2.56 to −0.79, p = 0.0002). Studies on the wild-type mice demonstrated significantly decreased levels of pro-inflammatory markers TNF-α, IL-1, and IL-6 (SMD = −2.28; 95% CI: −3.15 to −1.41, p = 0.00001). Despite the non-significant decrease in pro-inflammatory marker levels in transgenic mice (SMD = −0.47; 95% CI: −1.03 to 0.08, p = 0.09), the result favored the endocannabinoid-treated group over the control group.Conclusion: The revised data suggested that endocannabinoid stimulation promotes cognitive function via modulation of glial cells by decreasing pro-inflammatory markers in AD-like rodent models. Thus, cannabinoid agents may be required to modulate the downstream chain of effect to enhance cognitive stability against concurrent neuroinflammation in AD. Population-based studies and well-designed clinical trials are required to characterize the acceptability and real-world effectiveness of cannabinoid agents.Systematic Review Registration: [https://inplasy.com/inplasy-2022-8-0094/], identifier [Inplasy Protocol 3770].

Published

2023

36. 临床级人脐带间充质干细胞对创伤性脑损伤大鼠神经功能的改善作用.

Author

崔连旭, 江文康, 陆大鸿, 许峻荣, 刘小翠, and 王丙云

Subjects

*MESENCHYMAL stem cells, *BRAIN injuries, *TUMOR necrosis factors, *STEM cells, *CELL transplantation, *CELL suspensions, *UMBILICAL cord

Abstract

BACKGROUND: Traumatic brain injury is one of the most serious neurological diseases with the highest incidence in the world, and there is no effective therapy at present. Studies have shown that mesenchymal stem cells have a certain repair effect on traumatic brain injury. OBJECTIVE: To investigate the effects of clinical-grade umbilical cord mesenchymal stem cells on the improvement of neurological function in rats with traumatic brain injury. METHODS: Forty-five rats were divided into three groups, namely sham operation group (n=15), model group (n=15) and stem cell group (n=15). Except the sham operation group, the modified Feeney free fall method was used to establish the traumatic brain injury model in the model and stem cell groups. At 24 hours after model establishment, the model group was implanted with 20 μL normal saline; and the stem cell group was implanted with 20 μL human umbilical cord mesenchymal stem cell suspension, a total of 1×106 cells. At 1, 3, 7, 14, and 21 days after cell transplantation, the neural function of the rats was evaluated by modified neurological severity scores. At 21 days after injection, the ratio of Bcl-2/Bax mRNA was detected by RT-qPCR. The expression levels of gliocyte markers GFAP and IBA1 were detected by RT-qPCR and immunofluorescence method. At 21 days after injection, plasma levels of tumor necrosis factor alpha, interleukin 6 and interleukin 10 were determined by ELISA. Hematoxylin-eosin staining was used to observe the brain tissue structure. RESULTS AND CONCLUSION: (1) Compared with the model group, modified neurological severity score was significantly lower and the motor function was significantly improved in the stem cell group. (2) Compared with the model group, Bcl-2/Bax mRNA ratio was significantly increased in brain tissue, the expression of GFAP and IBA1 was significantly decreased in the stem cell group, while the expression of tumor necrosis factor alpha, interleukin 6 and interleukin 10 in plasma was not significantly different. (3) Hematoxylin-eosin staining showed that the defect area and edema of brain tissue and neuronal apoptosis were improved in different degrees in the stem cell group. (4) The results show that clinical-grade human umbilical cord mesenchymal stem cells can promote neurological function recovery, reduce neuronal apoptosis and inhibit glial overactivation after traumatic brain injury. [ABSTRACT FROM AUTHOR]

Published

2023

37. 脊髓损伤后神经修复过程中的细胞微环境.

Author

朱正桓, 邹红军, 宋志文, and 刘锦波

Subjects

*TUMOR necrosis factors, *SPINAL cord injuries, *NEURAL stem cells, *CELL anatomy, *SPARE parts, *AXONS

Abstract

BACKGROUND: Previous studies have shown that a single change in the expression of a gene or the state of a cell in the area of spinal cord injury has no significant effect on functional recovery after spinal cord injury. An increasing number of evidence shows that the regulation of cellular microenvironment after spinal cord injury is a key factor hindering the recovery of neurological function. OBJECTIVE: To review the biological characteristics of cellular microenvironment before and after spinal cord injury, including the effect and mechanism of mutual regulation among different kinds of cells and extracellular components on nerve repair after spinal cord injury. METHODS: The first author retrieved the databases including PubMed and Web of Science for articles published from January 2000 to December 2021 using the key words of “spinal cord injury, glial cell, neuron, immune cell, neural stem cell, extracellular matrix, cytokine, extracellular vesicle, regeneration”. Finally, 64 articles were selected for analysis. RESULTS AND CONCLUSION: (1) After spinal cord injury, among the cellular components of the cellular microenvironment, the interaction among glial cells, which account for the highest proportion, and the interaction with neurons are particularly critical. (2) Among the extracellular components after spinal cord injury, the hydrogels with good biocompatibility used to imitate natural extracellular matrix can effectively simulate and reconstruct the cellular microenvironment in the injured area and promote axonal elongation. (3) Among the extracellular regulatory factors after spinal cord injury, proinflammatory factors such as tumor necrosis factor-α and interleukin-1β aggravate the inflammatory storm of cellular microenvironment. Using receptor inhibitors or blocking related pathways to down-regulate the expression of adverse extracellular regulatory factors is an effective therapeutic method in the cellular microenvironment. At the same time, there are also studies on increasing the expression of anti-inflammatory factors such as interleukin-10 in the microenvironment of the spinal cord and on inhibiting the development of inflammation in the injured area. (4) Recently, extracellular vesicles have also played an important role in the cellular microenvironment as carriers of information. (5) This article reveals multiple sets of mutual regulatory relationships between cellular components and extracellular components in the cellular microenvironment after spinal cord injury, emphasizing that the neuroreparative effects of various components in the cellular microenvironment are not isolated. [ABSTRACT FROM AUTHOR]

Published

2023

38. Inflammation in pathogenesis of chronic pain: Foe and friend.

Author

Xiao-Xia Fang, Meng-Nan Zhai, Meixuan Zhu, Cheng He, Heng Wang, Juan Wang, and Zhi-Jun Zhang

Subjects

*CHRONIC pain, *PERIPHERAL nervous system, *INFLAMMATION, *CENTRAL nervous system, *NEUROGLIA, *CENTRAL nervous system injuries

Abstract

Chronic pain is a refractory health disease worldwide causing an enormous economic burden on individuals and society. Accumulating evidence suggests that inflammation in the peripheral nervous system (PNS) and central nervous system (CNS) is the major factor in the pathogenesis of chronic pain. The inflammation in the early- and late phase may have distinctive effects on the initiation and resolution of pain, which can be viewed as friend or foe. On the one hand, painful injuries lead to the activation of glial cells and immune cells in the PNS, releasing pro-inflammatory mediators, which contribute to the sensitization of nociceptors, leading to chronic pain; neuroinflammation in the CNS drives central sensitization and promotes the development of chronic pain. On the other hand, macrophages and glial cells of PNS and CNS promote pain resolution via anti-inflammatory mediators and specialized pro-resolving mediators (SPMs). In this review, we provide an overview of the current understanding of inflammation in the deterioration and resolution of pain. Further, we summarize a number of novel strategies that can be used to prevent and treat chronic pain by controlling inflammation. This comprehensive view of the relationship between inflammation and chronic pain and its specific mechanism will provide novel targets for the treatment of chronic pain. [ABSTRACT FROM AUTHOR]

Published

2023

39. Olfactory Ensheathing Cells for Spinal Cord Injury: The Cellular Superpowers for Nerve Repair.

Author

Oieni, Francesca, Reshamwala, Ronak, and St John, James

Subjects

*SPINAL cord injuries, *NERVOUS system injuries, *NEUROINFLAMMATION, *CELL transplantation, *NERVOUS system regeneration, *PHAGOCYTOSIS

Abstract

Neurotrauma injuries are notoriously difficult to deal with both clinically as well as experimentally, as the cellular and molecular events ensuing after injury complicate the neuroinflammatory processes. Spinal cord injuries are further complicated by the formation of scars at the injury sites, which can provide a physical barrier to repair. The lack of effective clinical therapy for spinal cord injury underscores the need for experimental approaches to generate effective therapies. To repair the injury, cell transplantation offers the potential to replace lost cells and create a permissive bridge to promote neural regeneration across the injury site. Olfactory ensheathing cells (OECs), which are the glia of the olfactory nerve, stand apart from other candidate cell types due to their innate natural abilities to manage nerve injury and promote repair and regeneration. This is evidenced by their physiological role in the daily repair and maintenance of the olfactory nerve. Here, we explain their properties in relation to their physiological role and their most relevant cellular attributes, including cellular interactions, phagocytosis, migration, axonal guidance and support, and modulation of neuroinflammation. We highlight some critical drawbacks in the current approaches and identify some ways to address them. [ABSTRACT FROM AUTHOR]

Published

2022

40. Correlations between Clinical and Histopathologic Characteristics in Idiopathic Epiretinal Membrane.

Author

Wang, Lei-Chi, Lo, Wen-Jung, Huang, Ya-Yun, Chou, Yu-Bai, Li, An-Fei, Chen, Shih-Jen, Chou, Teh-Ying, and Lin, Tai-Chi

Subjects

*PARS plana, *NEUROGLIA, *CELL imaging, *IMMUNOHISTOCHEMISTRY, *IMMUNOSTAINING, *VITRECTOMY

Abstract

To investigate correlations between clinical and histopathologic characteristics of idiopathic epiretinal membrane (ERM). Retrospective interventional case series. In total, 87 eyes from 87 patients with idiopathic ERM who underwent pars plana vitrectomy with peeling of the ERM from 2019 to 2020 were included. The outcomes of clinical ophthalmic examination, including measurement of best-corrected visual acuity (BCVA) and spectral-domain OCT (SD-OCT), before and after surgery were reviewed. Surgical specimens were fixed in formalin and embedded in paraffin for histologic and immunohistochemical analysis. The association between morphological characteristics revealed on SD-OCT images and the cellular composition of the surgically excised ERM demonstrated with immunohistochemical staining were the main outcome measures. Changes in the BCVA and central macular thickness (CMT) were assessed through a comparison of preoperative and postoperative measurements. Based on SD-OCT morphological characteristics in the foveal area, 15 cases were classified into group 1A (mainly outer retinal thickening), 39 into group 1B (more tenting of the outer retina and distorted inner retina), and 33 into group 1C (prominent inner retina thickening). Overall, postoperative final BCVA and CMT at 1 year improved in all groups. Patients who presented with a better initial BCVA exhibited a more favorable final BCVA. Epiretinal membranes in group 1C demonstrated the greatest decrease in CMT compared with those in groups 1B and 1A, but the final CMT did not differ among the groups. A negative correlation between the density of hyalocytes (P = 0.003) and myofibroblasts (P = 0.047) was noted between the 3 groups. Total cell density and glial cell density of the ERMs were strongly associated with poor final BCVA and BCVA improvement. The present study provides new histopathologic information regarding the formation and progression of idiopathic ERM. Glial cell proliferation plays a predominant role in these processes. Epiretinal membranes with high cellularity and glial cell density may cause damage to the retina structure, resulting in poor postoperative visual outcomes. These findings provide additional evidence supporting early surgical intervention in patients with idiopathic ERM reported with visual disturbance. [ABSTRACT FROM AUTHOR]

Published

2022

41. The Effect of Varied Concentrations of Sialic Acid on the Expression of mir-155-5p in Human Glial Cells

Author

Mandana Azarmehr and Atoosa Moradzadegan

Subjects

sialic acid, mir-155 microrna, real-time pcr, glial cell, Medicine, Medicine (General), R5-920

Abstract

Background: Sialic acid is a 9-carbon monosaccharide that is predominantly expressed by the central nervous system and is involved in many physiological and pathological events like cancer and autoimmune diseases. miR155-5p is one of the microRNAs playing an active role in hematopoietic, inflammatory, and immune related responses and in inflammatory responses its expression increases in glial cells. Therefore, the present study was performed to investigate the effect of sialic acid on altering the expression of miR-155-5p in glial cells to identify the signaling pathways involved in inflammation.Methods: Glial cells were treated with different concentrations of sialic acid and IC-50 cells were examined by MTT assay. Then cell RNA was extracted and cDNA synthesis was performed for real-time PCR.Findings: The results from data analysis show that miR-155-5p had higher rate of expression at different concentrations compared to the control state.Conclusion: Considering that sialic acid increases the expression of miR-155-5p gene and results in a weaker defense against inflammation, the significance of miR-155-5p in inflammation and the role of sialic acid in stimulating inflammation is brought to attention, and extensive study into the knowledge of these pathways could pave the way for further research on the therapeutic goals of neuro-inflammatory diseases.

Published

2022

42. Central nervous system regeneration: the roles of glial cells in the potential molecular mechanism underlying remyelination

Author

Lili Quan, Akiko Uyeda, and Rieko Muramatsu

Subjects

Central nervous system, Glial cell, Remyelination, Systemic factors, Multiple sclerosis, Pathology, RB1-214

Abstract

Abstract Glial cells play crucial roles in brain homeostasis and pathogenesis of central nervous system (CNS) injuries and diseases. However, the roles of these cells and the molecular mechanisms toward regeneration in the CNS have not been fully understood, especially the capacity of them toward demyelinating diseases. Therefore, there are still very limited therapeutic strategies to restore the function of adult CNS in diseases such as multiple sclerosis (MS). Remyelination, a spontaneous regeneration process in the CNS, requires the involvement of multiple cellular and extracellular components. Promoting remyelination by therapeutic interventions is a promising novel approach to restore the CNS function. Herein, we review the role of glial cells in CNS diseases and injuries. Particularly, we discuss the roles of glia and their functional interactions and regulatory mechanisms in remyelination, as well as the current therapeutic strategies for MS.

Published

2022

43. A review on the consequences of molecular and genomic alterations following exposure to electromagnetic fields: Remodeling of neuronal network and cognitive changes.

Author

Abtin, Shima, Seyedaghamiri, Fatemehsadat, Aalidaeijavadi, Zahra, Farrokhi, Amir Mohammad, Moshrefi, Fazel, Ziveh, Tayebeh, Zibaii, Mohammad Ismail, Aliakbarian, Hadi, Rezaei-Tavirani, Mostafa, and Haghparast, Abbas

Subjects

*CENTRAL nervous system, *NEURAL circuitry, *GENETIC regulation, *ELECTROMAGNETIC fields, *COGNITIVE neuroscience, *SYNAPSES, *EPIGENOMICS

Abstract

The use of electromagnetic fields (EMFs) is essential in daily life. Since 1970, concerns have grown about potential health hazards from EMF. Exposure to EMF can stimulate nerves and affect the central nervous system, leading to neurological and cognitive changes. However, current research results are often vague and contradictory. These effects include changes in memory and learning through changes in neuronal plasticity in the hippocampus, synapses and hippocampal neuritis, and changes in metabolism and neurotransmitter levels. Prenatal exposure to EMFs has negative effects on memory and learning, as well as changes in hippocampal neuron density and histomorphology of hippocampus. EMF exposure also affects the structure and function of glial cells, affecting gate dynamics, ion conduction, membrane concentration, and protein expression. EMF exposure affects gene expression and may change epigenetic regulation through effects on DNA methylation, histone modification, and microRNA biogenesis, and potentially leading to biological changes. Therefore, exposure to EMFs possibly leads to changes in cellular and molecular mechanisms in central nervous system and alter cognitive function. • Electromagnetic field (EMF) exposure alters neurogenesis and apoptosis. • EMF exposure affects epigenetic and non-epigenetic regulation of gene expression. • Exposure to EMF modifies the expression, function, and structure of ion channels. • EMF exposure changes synaptic transmission and glial function. • EMF exposure causes the neuronal network remodeling and behavioral consequences. [ABSTRACT FROM AUTHOR]

Published

2024

44. Spinal lipocalin 2 as a factor in the development of central post-stroke pain.

Author

Nakamoto, Kazuo and Tokuyama, Shogo

Subjects

*LIPOCALIN-2, *LIPOCALINS, *NEUROGLIA, *INTRATHECAL injections, *SPINAL cord, *PROTHROMBIN, *IMMUNOGLOBULINS

Abstract

[Display omitted] • Central poststroke pain (CPSP) is a type of central neuropathic pain whose mechanisms remain unknown. • We hypothesized that spinal glial cell-derived molecules promoted the development of CPSP. • We used a bilateral common carotid occlusion (BCAO)-induced CPSP mouse model. • BCAO mice showed hypersensitivity to mechanical stimuli and astrocyte activation in the spinal cord. • Lipocalin 2 (LCN2) in the spinal cord of BCAO mice were identified as a responsible factor for CPSP. Central poststroke pain (CPSP) is a type of central neuropathic pain whose mechanisms remain unknown. Recently, we showed that activated astrocytes and microglial cells are present in the spinal cord of CPSP model mice. Activated glial cells exacerbate cerebral ischemic pathology by increasing the expression of inflammatory factors. However, the involvement of spinal glial cells in CPSP remains unknown. We hypothesized that spinal glial cell-derived molecules cause hyperexcitability or promoted the development of CPSP. In this study, we identified glial cell-derived factors involved in the development of CPSP using a bilateral common carotid occlusion (BCAO)-induced CPSP mouse model. Male ddY mice were subjected to BCAO for 30 min. The von Frey test assessed mechanical hypersensitivity in the right hind paw of mice. BCAO mice showed hypersensitivity to mechanical stimuli and astrocyte activation in the spinal cord 3 days after treatment. DNA microarray analysis revealed a significant increase in lipocalin 2 (LCN2), is known as neutrophil gelatinase-associated lipocalin, in the superficial dorsal horns of BCAO-induced CPSP model mice. LCN2 colocalized with GFAP, an astrocyte marker. Spinal GFAP-positive cells in BCAO mice co-expressed signal transducer and activator of transcription 3 (STAT3). The increase in the fluorescence intensity of LCN2 and GFAP in BCAO mice was suppressed by intrathecal injection of AG490, an inhibitor of JAK2 and downstream STAT3 activation, or anti-LCN2 antibody. Our findings indicated that LCN2 in spinal astrocytes may be a key molecule and may be partly involved in the development of CPSP. [ABSTRACT FROM AUTHOR]

Published

2024

45. Neurotoxic mechanisms of mycotoxins: Focus on aflatoxin B1 and T-2 toxin.

Author

Song, Chao, Wang, Zixu, Cao, Jing, Dong, Yulan, and Chen, Yaoxing

Subjects

ANIMAL health, NEUROGLIA, BLOOD-brain barrier, ENCEPHALITIS, REACTIVE oxygen species, NEURAL transmission

Abstract

Aflatoxin B1 (AFB1) and T-2 toxin are commonly found in animal feed and stored grain, posing a serious threat to human and animal health. Mycotoxins can penetrate brain tissue by compromising the blood-brain barrier, triggering oxidative stress and neuroinflammation, and leading to oxidative damage and apoptosis of brain cells. The potential neurotoxic mechanisms of AFB1 and T-2 toxin were discussed by summarizing the relevant research reports from the past ten years. AFB1 and T-2 toxin cause neuronal damage in the cerebral cortex and hippocampus, leading to synaptic transmission dysfunction, ultimately impairing the nervous system function of the body. The toxic mechanism is related to excessive reactive oxygen species (ROS), oxidative stress, mitochondrial dysfunction, apoptosis, autophagy, and an exaggerated inflammatory response. After passing through the blood-brain barrier, toxins can directly affect glial cells, alter the activation state of microglia and astrocytes, thereby promoting brain inflammation, disrupting the blood-brain barrier, and influencing the synaptic transmission process. We discussed the diverse effects of various concentrations of toxins and different modes of exposure on neurotoxicity. In addition, toxins can also cross the placental barrier, causing neurotoxic symptoms in offspring, as demonstrated in various species. Our goal is to uncover the underlying mechanisms of the neurotoxicity of AFB1 and T-2 toxin and to provide insights for future research, including investigating the impact of mycotoxins on interactions between microglia and astrocytes. [Display omitted] • The neurotoxic symptoms caused by aflatoxin B1 and T-2 toxin in various species was reviewed. • The effects of various doses and methods of administration on neurotoxicity induced by toxins were discussed. • The effects of aflatoxins B1 and T-2 toxin on glial cells were reviewed. • Four potential interventions for neurotoxicity induced by aflatoxin B1 and T-2 toxin are proposed. [ABSTRACT FROM AUTHOR]

Published

2024

46. MCT1-dependent energetic failure and neuroinflammation underlie optic nerve degeneration in Wolfram syndrome mice

Author

Greta Rossi, Gabriele Ordazzo, Niccolò N Vanni, Valerio Castoldi, Angelo Iannielli, Dario Di Silvestre, Edoardo Bellini, Letizia Bernardo, Serena G Giannelli, Mirko Luoni, Sharon Muggeo, Letizia Leocani, PierLuigi Mauri, and Vania Broccoli

Subjects

eye, retinal development, glial cell, astrocytes, Medicine, Science, Biology (General), QH301-705.5

Abstract

Wolfram syndrome 1 (WS1) is a rare genetic disorder caused by mutations in the WFS1 gene leading to a wide spectrum of clinical dysfunctions, among which blindness, diabetes, and neurological deficits are the most prominent. WFS1 encodes for the endoplasmic reticulum (ER) resident transmembrane protein wolframin with multiple functions in ER processes. However, the WFS1-dependent etiopathology in retinal cells is unknown. Herein, we showed that Wfs1 mutant mice developed early retinal electrophysiological impairments followed by marked visual loss. Interestingly, axons and myelin disruption in the optic nerve preceded the degeneration of the retinal ganglion cell bodies in the retina. Transcriptomics at pre-degenerative stage revealed the STAT3-dependent activation of proinflammatory glial markers with reduction of the homeostatic and pro-survival factors glutamine synthetase and BDNF. Furthermore, label-free comparative proteomics identified a significant reduction of the monocarboxylate transport isoform 1 (MCT1) and its partner basigin that are highly enriched on retinal glia and myelin-forming oligodendrocytes in optic nerve together with wolframin. Loss of MCT1 caused a failure in lactate transfer from glial to neuronal cell bodies and axons leading to a chronic hypometabolic state. Thus, this bioenergetic impairment is occurring concurrently both within the axonal regions and cell bodies of the retinal ganglion cells, selectively endangering their survival while impacting less on other retinal cells. This metabolic dysfunction occurs months before the frank RGC degeneration suggesting an extended time-window for intervening with new therapeutic strategies focused on boosting retinal and optic nerve bioenergetics in WS1.

Published

2023

47. Evaluating the Glucantime Concentration for the ex vivo Glial Cell Model of Antimony-resistant Leishmania tropica Amastigotes

Author

Orçun Zorbozan, Vedat Evren, Mehmet Harman, Ahmet Özbilgin, Özlem Alkan Yılmaz, and Nevin Turgay

Subjects

leishmania tropica, ex vivo, glial cell, amastigote, antimony resistance, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

Objective:Because the protocols used in the treatment of leishmaniasis can be toxic and have many limitations, such as the development of resistance against such protocols, new treatment options are needed, especially against resistant patients. Ex vivo models may be a good source for evaluating new drug options for patients with antimony-resistant parasites. This study aimed to evaluate the Glucantime concentration for our ex vivo glial cell amastigote model we had defined in previous work.Methods:We prepared the astroglial cell culture from brains of 2 to 3 day old neonatal Sprague-Dawley rats under sterile conditions by modifying McCarthy’s method. Four plates of cells were infected with antimony-resistant Leishmania tropica promastigotes. After 24 h of incubation, we added Glucantime to 3 plates with different concentrations. After 72 h, we removed the supernatant and then dried, fixed, and stained the plates with Giemsa to count the amastigotes in the glial cells.Results:We observed the amastigotes in glial cells in the control flask. Glial cells were ruined in flasks, which include 75 μg/mL and 37.5 μg/mL Glucantime. The number of amastigotes per 100 glial cells was 116 for the flask with 7.5 μg/mL Glucantime concentration, while 487 for the control flask.Conclusion:We found that while high concentrations of Glucantime were toxic for glial cells, 7.5 μg/mL Glucantime concentration managed to reduce the number of Leishmania tropica amastigotes in glial cells.

Published

2021

48. Multilineage-differentiating stress-enduring cells alleviate atopic dermatitis-associated behaviors in mice

Author

WenDi Fei, JunLin Wu, MengDie Gao, Qian Wang, Ya Yu Zhao, ChunLi Shan, Yu Shen, and Gang Chen

Subjects

Muse cells, Pruritus, DNFB, Spinal cord, Atopic dermatitis, Glial cell, Medicine (General), R5-920, Biochemistry, QD415-436

Abstract

Abstract Background Pruritus is a recurring, long-lasting skin disease with few effective treatments. Many patients have unsatisfactory responses to currently available antipruritic treatments, and effective therapeutics are urgently needed to relieve symptoms. A previous study reported that mesenchymal stem cell (MSC)-mediated immune regulation could be used to treat skin inflammatory diseases. Multilineage-differentiating stress-enduring (Muse) cells are a new type of pluripotent stem cell that may also have the potential to treat inflammatory skin diseases. Methods Muse cells were isolated from human bone marrow-derived MSCs (BMSCs) via the 8-h longterm trypsin incubation (LTT) method. Repeated use of 2,4-dinitrofluorobenzene (DNFB) induced atopic dermatitis (AD) in a mouse model. Immunofluorescence, behavior recording, and image analysis were used to evaluate the therapeutic effect of subcutaneous Muse cell injection. Real-time quantitative polymerase chain reaction (qPCR) was used to measure the expression of inflammatory factors. In vitro, wound healing and cell proliferation experiments were used to examine the effect of Muse cell supernatant on keratinocytes. Results Our results showed that subcutaneous injection of Muse cells after AD model induction significantly alleviated scratching behavior in mice. The evaluation of dermatitis and photos of damaged skin on the back of the neck revealed that Muse cells reduced dermatitis, playing an active role in healing the damaged skin. The activation of spinal glial cells and scratching behavior were also reduced by Muse cell injection. In addition, we also showed that the expression levels of the inflammatory factors interleukin (IL)-6, IL-17α, and IL-33 in both the spinal cord and skin were suppressed by Muse cells. Furthermore, Muse cells not only exerted anti-inflammatory effects on lipopolysaccharide (LPS)-induced human HaCat cells but also promoted wound healing and keratinocyte proliferation. Conclusions In vivo, Muse cells could alleviate scratching symptoms, reduce epidermal inflammation, and promote wound healing. In vitro, Muse cells could also promote the migration and proliferation of keratinocytes. In summary, Muse cells may become a new therapeutic agent for the treatment of AD.

Published

2021

49. m6A epitranscriptomic modification regulates neural progenitor-to-glial cell transition in the retina

Author

Yanling Xin, Qinghai He, Huilin Liang, Ke Zhang, Jingyi Guo, Qi Zhong, Dan Chen, Jinyan Li, Yizhi Liu, and Shuyi Chen

Subjects

retinal development, glial cell, m6A, Medicine, Science, Biology (General), QH301-705.5

Abstract

N 6-methyladenosine (m6A) is the most prevalent mRNA internal modification and has been shown to regulate the development, physiology, and pathology of various tissues. However, the functions of the m6A epitranscriptome in the visual system remain unclear. In this study, using a retina-specific conditional knockout mouse model, we show that retinas deficient in Mettl3, the core component of the m6A methyltransferase complex, exhibit structural and functional abnormalities beginning at the end of retinogenesis. Immunohistological and single-cell RNA sequencing (scRNA-seq) analyses of retinogenesis processes reveal that retinal progenitor cells (RPCs) and Müller glial cells are the two cell types primarily affected by Mettl3 deficiency. Integrative analyses of scRNA-seq and MeRIP-seq data suggest that m6A fine-tunes the transcriptomic transition from RPCs to Müller cells by promoting the degradation of RPC transcripts, the disruption of which leads to abnormalities in late retinogenesis and likely compromises the glial functions of Müller cells. Overexpression of m6A-regulated RPC transcripts in late RPCs partially recapitulates the Mettl3-deficient retinal phenotype. Collectively, our study reveals an epitranscriptomic mechanism governing progenitor-to-glial cell transition during late retinogenesis, which is essential for the homeostasis of the mature retina. The mechanism revealed in this study might also apply to other nervous systems.

Published

2022

50. Heterogeneity and Molecular Markers for CNS Glial Cells Revealed by Single-Cell Transcriptomics.

Author

Sun, Junjie, Song, Yixing, Chen, Zhiheng, Qiu, Jiaying, Zhu, Shunxing, Wu, Liucheng, and Xing, Lingyan

Subjects

*SPINAL cord diseases, *ALZHEIMER'S disease, *HETEROGENEITY, *SPINAL cord injuries, *NEUROGLIA, *NEUROLOGICAL disorders, *OLIGODENDROGLIA

Abstract

Glial cells, including astrocytes, oligodendrocytes, and microglia, are the major components in the central nervous system (CNS). Studies have revealed the heterogeneity of each glial cell type and that they each may play distinct roles in physiological processes and/or neurological diseases. Single-cell sequencing (scRNA-seq) technology developed in recent years has extended our understanding of glial cell heterogeneity from the perspective of transcriptome profiling. This review summarizes the marker genes of major glial cells in the CNS and reveals their heterogeneity in different species, CNS regions, developmental stages, and pathological states (Alzheimer's disease and spinal cord injury), expanding our knowledge of glial cell heterogeneity on both molecular and functional levels. [ABSTRACT FROM AUTHOR]

Published

2022