Your search keyword '"schwann cell"' showing total 10,240 results

1. Schwann Cell‐Mediated M2‐Like Macrophage Polarization in Rhabdomyosarcoma.

Author

Feng, Guanying, Guo, Yibo, Chen, Mingtao, Zhang, Yu, Liu, Zheqi, Sun, Chen, Hu, Xin, Lin, Chengzhong, Liu, Yu, Wu, Yue, Wu, Hao, Yang, Xi, Wang, Yang, Ye, Jinhai, Liu, Jiannan, Wang, Xu, Ji, Tong, and Zhang, Chenping

Abstract

ABSTRACT Objective Methods Results Conclusions To investigate the cellular components and immunological characteristics of the head and neck rhabdomyosarcoma (RMS) microenvironment.We conducted single‐cell transcriptomics to analyze the cellular components of the RMS microenvironment. CellChat was utilized for analyzing intercellular interactions. The cancer genome atlas database was used for validation. CIBERSORT was applied for immune infiltration profiling. Functional enrichment analyses were performed using the Kyoto Encyclopedia of Genes and Genomes. Gene set scores were calculated using single‐sample gene set enrichment analysis. Subcutaneous allograft models and bulk RNA sequencing were used for validation. Flow cytometry and immunohistochemistry were used to identify M2‐like macrophages.Our findings revealed an extremely low presence of neutrophils in RMS samples compared with normal sample. RMS sample with high Schwann cell infiltration exhibited an increase in M2‐like macrophage infiltration. Receptor‐ligand pairs, specifically MIF‐CD74 and PTN‐SDC3, were identified between Schwann cells and M2‐like macrophages. In the RMS sample characterized by significant Schwann cell infiltration, M2‐like macrophages demonstrate robust expression of axon guidance factors and are enriched in the axon guidance pathway.Our study provides valuable insights into the microenvironment and immunological characteristics of RMS, offering crucial information for further research and potential therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2024

2. Tau Isoform-Regulated Schwann Cell Proliferation and Migration Improve Peripheral Nerve Regeneration After Injury.

Author

Li, Shiying, Zhang, Fuqian, Wang, Guifang, Liu, Qianyan, Wang, Xinghui, Chen, Qianqian, and Chu, Dandan

Subjects

*ALTERNATIVE RNA splicing, *PERIPHERAL nerve injuries, *SCIATIC nerve injuries, *CENTRAL nervous system diseases, *SCIATIC nerve

Abstract

Tau is a microtubule-associated protein that plays a vital role in the mammalian nervous system. Alternative splicing of the MAPT gene leads to the formation of tau isoforms with varying N-terminal inserts and microtubule-binding repeats. Dysregulation of tau alternative splicing has been linked to diseases in the central nervous system, but the roles of tau isoforms in the peripheral nervous system remain unclear. Here, we investigated the alternative splicing of tau exons 4A and 10 in the sciatic nerve and Schwann cells during development and following injury. We discovered that low-molecular-weight (LMW) tau, resulting from the exclusion of exon 4A, and 3R tau, generated by the exclusion of exon 10, diminishes with aging in rat sciatic nerve and Schwann cells. High-molecular-weight (HMW) tau and 3R tau increase in the adult sciatic nerve post-injury. We constructed viruses that expressed HMW−4R, LMW−4R, HMW−3R, and LMW−3R and introduced them into cultured cells or the distal part of the injured sciatic nerve to assess their effects on Schwann cell migration and proliferation. We also examined the effects of the four isoforms on axon growth and debris clearance after sciatic nerve injury. Our results demonstrated that tau isoforms inhibit Schwann cell proliferation while promoting Schwann cell migration and sciatic nerve regeneration. Specifically, the 3R−tau isoforms were more effective than the 4R−tau isoforms in promoting nerve regeneration. In conclusion, our study reveals the roles of tau isoforms in the peripheral nervous system and provides insights into the development of new therapeutic strategies for peripheral nerve injuries. [ABSTRACT FROM AUTHOR]

Published

2024

3. FGF21 inhibits ferroptosis caused by mitochondrial damage to promote the repair of peripheral nerve injury.

Author

Yan, Yao, Ran, Xinyu, Zhou, Zihan, Gu, Yuting, Wang, Rendu, Qiu, Chuanqi, Sun, Yinuo, Wang, Jifeng, Xiao, Jian, Lu, Yingfeng, and Wang, Jian

Subjects

PERIPHERAL nerve injuries, FIBROBLAST growth factors, SCIATIC nerve injuries, UNSATURATED fatty acids, SCHWANN cells

Abstract

Introduction: Ferroptosis is a new type of cell death characterized by lipid peroxidation and iron dependency, representing an emerging disease regulation mechanism. The limited understanding of ferroptosis in peripheral nerve injury (PNI) complicates the management of such injuries. Mitochondrial dysfunction, which contributes to ferroptosis, further exacerbates the challenges of peripheral nerve repair Methods: In this study, we established an in vitro model of Schwann cells model treated with TBHP and an in vivo sciatic nerve crush injury model in rats. These models were used to investigate the effects of fibroblast growth factor 21 (FGF21) on PNI, both in vitro and in vivo, and to explore the potential mechanisms linking injury-induced ferroptosis and mitochondrial dysfunction. Results: Our findings reveal that PNI triggers abnormal accumulation of lipid reactive oxygen species (ROS) and inactivates mitochondrial respiratory chain complex III, leading to mitochondrial dysfunction. This dysfunction catalyzes the oxidation of excessive polyunsaturated fatty acids, resulting in antioxidant imbalance and loss of ferroptosis suppressor protein 1 (FSP1), which drives lipid peroxidation. Additionally, irregular iron metabolism, defective mitophagy, and other factors contribute to the induction of ferroptosis. Importantly, we found that FGF21 attenuates the abnormal accumulation of lipid ROS, restores mitochondrial function, and suppresses ferroptosis, thus promoting PNI repair. Notably, glutathione peroxidase 4 (GPX4), a downstream target of nuclear factor E2-related factor 2 (Nrf2), and the ERK/Nrf2 pathway are involved in the regulation of ferroptosis by FGF21. Conclusion: FGF21 promotes peripheral nerve repair by inhibiting ferroptosis caused by mitochondrial dysfunction. Therefore, targeting mitochondria and ferroptosis represents a promising therapeutic strategy for effective PNI repair. [ABSTRACT FROM AUTHOR]

Published

2024

4. Development of a ZRS Reporter System for the Newt (Cynops pyrrhogaster) During Terrestrial Limb Regeneration.

Author

Casco-Robles, Martin Miguel, Ikeda, Ryosuke, Maruo, Fumiaki, and Chiba, Chikafumi

Subjects

SCHWANN cells, NEWTS, REGENERATIVE medicine, BINDING sites, PROTEIN expression

Abstract

Background: Newts, a type of urodele amphibian, offer remarkable insights into regenerative medicine due to their extraordinary tissue regeneration capabilities—a challenging feat in humans. During limb regeneration of adult newts, fascinating cellular and molecular processes are revealed, including scarless healing, de-differentiation of mature cells, and regeneration of limbs and digits. Sonic hedgehog (Shh), crucial for vertebrate limb development, is regulated by the zone of polarizing activity regulatory sequence (ZRS) in the limb bud zone of polarizing activity (ZPA). The metamorphosed (terrestrial) newt can reactivate Shh during regeneration, facilitating proper limb patterning. Cell types capable of regulating the ZRS in metamorphosed newts remain unknown. The identification of such cell types provides invaluable insight into novel regenerative mechanisms. Objective: In this study, we developed the first newt ZRS reporter. Methods: We isolated and characterized the newt ZRS enhancer (nZRS), identifying conserved DNA binding sites. Several binding sites with medical relevance were conserved in the newt ZRS. In functional analysis, we developed a system composed of a transgenic nZRS reporter newt and a new newt anti-Shh antibody, which allowed Shh monitoring during limb regeneration. Results: We identified a group of Schwann cells capable of ZRS reporter and Shh protein expression during terrestrial limb regeneration. Conclusions: This system provides a valuable in vivo approach for future genetic studies of patterning during limb regeneration. [ABSTRACT FROM AUTHOR]

Published

2024

5. The Protective Role of Caffeine against Histological and Ultrastructural Changes of Peripheral Nerve in Type 2 Diabetic Rats.

Author

Othman, Manal A., Potu, Bhagath Kumar, Rashid, Aisha, Fatima, Ayesha, and El-Din, Wael Amin Nasr

Abstract

Type 2 diabetes mellitus (T2DM) is linked to injuries to many organs including the nervous system. Diabetic peripheral neuropathy (DPN) is a common complication of diabetes; it can result in disruption of Schwann cells (SCs) function, degeneration of nerve axons and demyelination. SCs provide trophic support to neurons and myelin formation and their role in nerve injury and regeneration is very crucial. Caffeine, a psychoactive beverage, was found to reduce the risk of many disorders including nervous system degeneration. The purpose of this study was to address the role of caffeine in peripheral nerve degeneration in a rat model of T2DM. Wistar rats were fed with a high caloric diet and injected with a single low dose of streptozotocin (STZ). Caffeine was administered to the rats orally for 5 weeks and was given one week before injection of STZ. The rats were sacrificed, then sciatic nerves were harvested, and processed for histological and electron microscopic evaluations. Immunohistochemistry was also done using the primary antibodies: anti S-100 (Schwann cell marker), anti-MBP (myelin basic protein) and anti-VEGF-A (vascular endothelial growth factor A). Examination of the sciatic nerve of diabetic rats revealed degeneration of SCs and axons, myelin, and connective tissue coverings. There was decrease in immunostaining of S-100 and MBP and increase in VEGFA, in diabetic rats. Administration of caffeine to diabetic rats resulted in improvement of histological and ultrastructural changes and upregulation of S-100, MBP, and downregulation of VEGFA. There were degenerative changes of the sciatic nerve of diabetic rats that were ameliorated by the administration of caffeine. [ABSTRACT FROM AUTHOR]

Published

2024

6. Novel SOX10 indel mutations drive schwannomas through impaired transactivation of myelination gene programs

Author

Williams, Erik A, Ravindranathan, Ajay, Gupta, Rohit, Stevers, Nicholas O, Suwala, Abigail K, Hong, Chibo, Kim, Somang, Yuan, Jimmy Bo, Wu, Jasper, Barreto, Jairo, Lucas, Calixto-Hope G, Chan, Emily, Pekmezci, Melike, LeBoit, Philip E, Mully, Thaddeus, Perry, Arie, Bollen, Andrew, Van Ziffle, Jessica, Devine, W Patrick, Reddy, Alyssa T, Gupta, Nalin, Basnet, Kristen M, Macaulay, Robert JB, Malafronte, Patrick, Lee, Han, Yong, William H, Williams, Kevin Jon, Juratli, Tareq A, Mata, Douglas A, Huang, Richard SP, Hiemenz, Matthew C, Pavlick, Dean C, Frampton, Garrett M, Janovitz, Tyler, Ross, Jeffrey S, Chang, Susan M, Berger, Mitchel S, Jacques, Line, Song, Jun S, Costello, Joseph F, and Solomon, David A

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Pediatric, Cancer, Human Genome, Neurosciences, Biotechnology, Genetics, Rare Diseases, Aetiology, 2.1 Biological and endogenous factors, Humans, INDEL Mutation, Transcriptional Activation, Neurilemmoma, Neuroma, Acoustic, Mutation, Nerve Sheath Neoplasms, SOXE Transcription Factors, myelination, PMP2, Schwann cell, schwannoma, SOX10, Oncology and Carcinogenesis, Oncology & Carcinogenesis, Oncology and carcinogenesis

Abstract

BackgroundSchwannomas are common peripheral nerve sheath tumors that can cause severe morbidity given their stereotypic intracranial and paraspinal locations. Similar to many solid tumors, schwannomas and other nerve sheath tumors are primarily thought to arise due to aberrant hyperactivation of the RAS growth factor signaling pathway. Here, we sought to further define the molecular pathogenesis of schwannomas.MethodsWe performed comprehensive genomic profiling on a cohort of 96 human schwannomas, as well as DNA methylation profiling on a subset. Functional studies including RNA sequencing, chromatin immunoprecipitation-DNA sequencing, electrophoretic mobility shift assay, and luciferase reporter assays were performed in a fetal glial cell model following transduction with wildtype and tumor-derived mutant isoforms of SOX10.ResultsWe identified that nearly one-third of sporadic schwannomas lack alterations in known nerve sheath tumor genes and instead harbor novel recurrent in-frame insertion/deletion mutations in SOX10, which encodes a transcription factor responsible for controlling Schwann cell differentiation and myelination. SOX10 indel mutations were highly enriched in schwannomas arising from nonvestibular cranial nerves (eg facial, trigeminal, vagus) and were absent from vestibular nerve schwannomas driven by NF2 mutation. Functional studies revealed these SOX10 indel mutations have retained DNA binding capacity but impaired transactivation of glial differentiation and myelination gene programs.ConclusionsWe thus speculate that SOX10 indel mutations drive a unique subtype of schwannomas by impeding proper differentiation of immature Schwann cells.

Published

2023

7. Nuclear Magnetic Resonance Treatment Induces ßNGF Release from Schwann Cells and Enhances the Neurite Growth of Dorsal Root Ganglion Neurons In Vitro.

Author

Rad, Anda, Weigl, Lukas, Steinecker-Frohnwieser, Bibiane, Stadlmayr, Sarah, Millesi, Flavia, Haertinger, Maximilian, Borger, Anton, Supper, Paul, Semmler, Lorenz, Wolf, Sonja, Naghilou, Aida, Weiss, Tamara, Kress, Hans G., and Radtke, Christine

Subjects

*DORSAL root ganglia, *TRPV cation channels, *NUCLEAR magnetic resonance, *NOCICEPTORS, *PERIPHERAL nervous system

Abstract

Peripheral nerve regeneration depends on close interaction between neurons and Schwann cells (SCs). After nerve injury, SCs produce growth factors and cytokines that are crucial for axon re-growth. Previous studies revealed the supernatant of SCs exposed to nuclear magnetic resonance therapy (NMRT) treatment to increase survival and neurite formation of rat dorsal root ganglion (DRG) neurons in vitro. The aim of this study was to identify factors involved in transferring the observed NMRT-induced effects to SCs and consequently to DRG neurons. Conditioned media of NMRT-treated (CM NMRT) and untreated SCs (CM CTRL) were tested by beta-nerve growth factor (ßNGF) ELISA and multiplex cytokine panels to profile secreted factors. The expression of nociceptive transient receptor potential vanilloid 1 (TRPV1) channels was assessed and the intracellular calcium response in DRG neurons to high-potassium solution, capsaicin or adenosine triphosphate was measured mimicking noxious stimuli. NMRT induced the secretion of ßNGF and pro-regenerative-signaling factors. Blocking antibody experiments confirmed ßNGF as the main factor responsible for neurotrophic/neuritogenic effects of CM NMRT. The TRPV1 expression or sensitivity to specific stimuli was not altered, whereas the viability of cultured DRG neurons was increased. Positive effects of CM NMRT supernatant on DRG neurons are primarily mediated by increased ßNGF levels. [ABSTRACT FROM AUTHOR]

Published

2024

8. 施万细胞促进头颈癌增殖、侵袭机制的研究进展.

Author

蔡永鹏, 苟黎明, and 李 勇

Abstract

There is extensive peripheral nerve infiltration and tumor innervation in head and neck cancer, which promotes tumor progress and brings worse prognosis. Schwann cells (SCs) are a type of glial cells that are widely distributed in the peripheral nervous system and are involved in nerve injury repair. In recent years, more and more studies have shown that SCs play an important role in the tumor microenvironment (TME). Reprogrammed SCs promote peripheral nerve infiltration and tumor innervation through signal interaction with tumor and nerves on the one hand, and directly act on TME components and promote tumor progression on the other hand. This paper mainly discusses the cross-talk patterns of SCs and cancer-nerve signals, as well as the mechanism of action of SCS-related signals in TME, and explore potential targets for therapeutic intervention in SCS-related head and neck cancer. [ABSTRACT FROM AUTHOR]

Published

2024

9. Enhancement of Heme-Oxygenase 1 in the Injured Peripheral Nerve Following Sulforaphane Administration Fosters Regeneration via Proliferation and Maintenance of Repair Schwann Cells.

Author

Szepanowski, Fabian, Zipfel, Jaqueline, Szepanowski, Rebecca D., Eggert, Bianca, Güner, Nail-Mert, Szepanowski, Leon-Phillip, Kleinschnitz, Christoph, Mausberg, Anne K., and Stettner, Mark

Subjects

SCHWANN cells, SCIATIC nerve injuries, SCIATIC nerve, CRUSH syndrome, HEME oxygenase

Abstract

Nuclear erythroid 2-related factor 2 (Nrf2) and its downstream effector heme oxygenase 1 (HO-1) are commonly activated in response to cellular stresses. The elevated expression of HO-1 has been associated with markedly accelerated peripheral nerve regeneration. This study aimed to evaluate the impact of a naturally occurring dietary Nrf2/HO-1 activator—sulforaphane (SFN)—on regeneration in a murine sciatic nerve crush model. The beneficial safety profile of SFN has been thoroughly investigated and confirmed several times. Here, SFN was administered daily, starting immediately after C57BL/6 mice were subjected to sciatic nerve crush injury. Injured sciatic nerves were excised at various time points post injury for molecular, immunohistochemical and morphometric analyses. Moreover, functional assessment was performed by grip strength analysis and electrophysiology. Following SFN treatment, the early response to injury includes a modulation of autophagic pathways and marked upregulation of Nrf2/HO-1 expression. This enhancement of HO-1 expression was maintained throughout the regeneration phase and accompanied by a significant increase in repair Schwann cells. In these cells, elevated proliferation rates were observed. Significant improvements in grip strength test performance, nerve conduction velocity and remyelination were also noted following SFN treatment. Collectively, SFN modulates cytoprotective and autophagic pathways in the injured nerve, increasing the number of repair Schwann cells and contributing to effective nerve regeneration. Given the availability of SFN as a nutritional supplement, this compound might constitute a novel regenerative approach with broad patient accessibility and further studies on this topic are warranted. [ABSTRACT FROM AUTHOR]

Published

2024

10. TFEB/3 Govern Repair Schwann Cell Generation and Function Following Peripheral Nerve Injury.

Author

Patel, Akash A., Kim, Hyukmin, Ramesh, Raghu, Marquez, Anthony, Faraj, Moler M., Antikainen, Henri, Lee, Andrew S., Torres, Adriana, Khawaja, Imran M., Heffernan, Corey, Bonder, Edward M., Maurel, Patrice, Svaren, John, Son, Young-Jin, Dobrowolski, Radek, and Kim, Haesun A.

Subjects

*SCHWANN cells, *SCIATIC nerve injuries, *PERIPHERAL nerve injuries, *KNOCKOUT mice, *GENETIC regulation, *NERVOUS system regeneration

Abstract

TFEB and TFE3 (TFEB/3), key regulators of lysosomal biogenesis and autophagy, play diverse roles depending on cell type. This study highlights a hitherto unrecognized role of TFEB/3 crucial for peripheral nerve repair. Specifically, they promote the generation of progenitor-like repair Schwann cells after axonal injury. In Schwann cell-specific TFEB/3 double knock-out mice of either sex, the TFEB/3 loss disrupts the transcriptomic reprogramming that is essential for the formation of repair Schwann cells. Consequently, mutant mice fail to populate the injured nerve with repair Schwann cells and exhibit defects in axon regrowth, target reinnervation, and functional recovery. TFEB/3 deficiency inhibits the expression of injury-responsive repair Schwann cell genes, despite the continued expression of c-jun, a previously identified regulator of repair Schwann cell function. TFEB/3 binding motifs are enriched in the enhancer regions of injury-responsive genes, suggesting their role in repair gene activation. Autophagy-dependent myelin breakdown is not impaired despite TFEB/3 deficiency. These findings underscore a unique role of TFEB/3 in adult Schwann cells that is required for proper peripheral nerve regeneration. [ABSTRACT FROM AUTHOR]

Published

2024

11. Schwann Cell-Derived Exosomes Induced Axon Growth after Spinal Cord Injury by Decreasing PTP-σ Activation on CSPGs via the Rho/ROCK Pathway.

Author

Zhu, Shibo, Ma, Hongpeng, Hou, Mengfan, Li, Hailiang, and Ning, Guangzhi

Subjects

*SPINAL cord injuries, *EXOSOMES, *SCARS, *CHONDROITIN sulfates, *NEUROLOGICAL disorders

Abstract

Spinal cord injury (SCI) is a severe neurological condition that involves a lengthy pathological process. This process leads to the upregulation of chondroitin sulfate proteoglycans (CSPGs) by reactive glia, which impedes repair and regeneration in the spinal cord. The role of the CSPG-specific receptor protein tyrosine phosphatase-sigma (PTP-σ) in post-SCI remains largely unexplored. Exosomes have great potential in the diagnosis, prognosis, and treatment of SCI due to their ability to easily cross the blood‒brain barrier. Schwann cell-derived exosomes (SCDEs) promote functional recovery in mice post-SCI by decreasing CSPG deposition. However, the mechanism by which SCDEs decrease CSPGs after SCI remains unknown. Herein, we observed elevated levels of PTP-σ and increased CSPG deposition during glial scar formation after SCI in vivo. After SCDEs were injected into SCI mice, CSPG deposition decreased in scar tissue at the injury site, the expression of PTP-σ increased during axonal growth around the injury site, and motor function subsequently recovered. Additionally, we demonstrated that the use of both Rho/ROCK inhibitors and SCDEs inhibited the reparative effects of SCDEs on scar tissue after SCI. In conclusion, our study revealed that treatment with SCDEs targeting the Rho/ROCK signaling pathway reduced PTP-σ activation in the CSPG post-SCI, which inhibited scar tissue formation. [ABSTRACT FROM AUTHOR]

Published

2024

12. (+)-Catechin Alleviates CCI-Induced Neuropathic Pain in Rats by Modulating the IL34/CSFIR Axis and Attenuating the Schwann Cell-Macrophage Cascade Response in the DRG.

Author

Jing, Bei, Chen, Zhen-ni, Si, Wai-mei, Zhao, Jia-ji, Zhao, Guo-ping, and Zhang, Di

Abstract

The aim of this study was to investigate the potential therapeutic applications of (+)-catechin in the treatment of neuropathic pain. In vivo study, 32 SD rats were randomly divided into four groups: sham group, chronic constriction injury (CCI) group, CCI + ibuprofen group and CCI+ (+)-catechin group. They were subjected to behavioural tests, ELISA, immunohistochemistry and Western blotting. The mechanisms involved were investigated using specific inhibitors in cell experiments. Results of in vivo experiments showed that (+)-catechin could reduce the cold sensitivity pain in a rat model of CCI; ELISA and immunohistochemistry results showed that (+)-catechin could decrease the levels of IL-8, IL-6, TNF-α, CCL2 and CCL5 in serum and the expression levels of nNOS, COX2, IL6, TNF-α, IBA-1 and CSF1R in DRG of CCI rats. Finally, western blot confirmed that (+)-catechin could diminish the levels of IL-34/CSF1R/JAK2/STAT3 signalling pathway in DRG of CCI rats. In vitro studies showed that (+)-catechin reduced IL-34 secretion in LPS-induced RSC96 cells. Meanwhile, (+)-catechin administration in LPS-induced Schwann cell–conditioned medium (L-CM) significantly inhibited the proliferation and migration of RAW264.7 cells; in addition, L-CM+(+)-catechin reduced the activation of the CSF1R/JAK2/STAT3 signalling pathway. (+)-Catechin attenuated the Schwann cell-macrophage cascade response in the DRG by modulating the IL34/CSFIR axis and inhibiting activation of the JAK2/STAT3 pathway, thereby attenuating CCI-induced neuropathic pain in rats. [ABSTRACT FROM AUTHOR]

Published

2024

13. Adenosine A2A receptor as a potential regulator of Mycobacterium leprae survival mechanisms: new insights into leprosy neural damage.

Author

Freire dos Santos, Plinio Marcos, Díaz Acosta, Chyntia Carolina, Silveira Andrezo Rosa, Thabatta Leal, Harumi Ishiba, Michelle, Alves Dias, André, Rodrigues Pereira, Antonio Marcos, Domingos Gutierres, Luísa, Pontes Pereira, Melissa, da Silva Rocha, Matheus, Sammarco Rosa, Patrícia, Bertoluci, Daniele F. F., Roberto Meyer-Fernandes, José, Ramalho Costa, Fabricio da Mota, Marques, Maria Angela M., Belisle, John T., Olmo Pinheiro, Roberta, Silva Rodrigues, Luciana, Vidal Pessolani, Maria Cristina, and Berrêdo-Pinho, Marcia

Subjects

ADENOSINES, PURINERGIC receptors, MYCOBACTERIUM leprae, HANSEN'S disease, TRANSCRIPTION factors, SCHWANN cells, PERIPHERAL nervous system

Abstract

Background: Leprosy is a chronic infectious disease caused by Mycobacterium leprae, which can lead to a disabling neurodegenerative condition. M. leprae preferentially infects skin macrophages and Schwann cells-glial cells of the peripheral nervous system. The infection modifies the host cell lipid metabolism, subverting it in favor of the formation of cholesterol-rich lipid droplets (LD) that are essential for bacterial survival. Although researchers have made progress in understanding leprosy pathogenesis, many aspects of the molecular and cellular mechanisms of host-pathogen interaction still require clarification. The purinergic system utilizes extracellular ATP and adenosine as critical signalingmolecules and plays several roles in pathophysiological processes. Furthermore, nucleoside surface receptors such as the adenosine receptor A2AR involved in neuroimmune response, lipid metabolism, and neuron-glia interaction are targets for the treatment of different diseases. Despite the importance of this system, nothing has been described about its role in leprosy, particularly adenosinergic signaling (AdoS) during M. leprae-Schwann cell interaction. Methods: M. leprae was purified from the hind footpad of athymic nu/nu mice. ST88-14 human cells were infected with M. leprae in the presence or absence of specific agonists or antagonists of AdoS. Enzymatic activity assays, fluorescence microscopy, Western blotting, and RT-qPCR analysis were performed. M. leprae viability was investigated by RT-qPCR, and cytokines were evaluated by enzymelinked immunosorbent assay. Results: We demonstrated that M. leprae-infected Schwann cells upregulated CD73 and ADA and downregulated A2AR expression and the phosphorylation of the transcription factor CREB (p-CREB). On the other hand, activation of A2AR with its selective agonist, CGS21680, resulted in: 1) reduced lipid droplets accumulation and pro-lipogenic gene expression; 2) reduced production of IL-6 and IL-8; 3) reduced intracellular M. leprae viability; 4) increased levels of p-CREB. Conclusion: These findings suggest the involvement of the AdoS in leprosy neuropathogenesis and support the idea that M. leprae, by downmodulating the expression and activity of A2AR in Schwann cells, decreases A2AR downstream signaling, contributing to the maintenance of LD accumulation and intracellular viability of the bacillus. [ABSTRACT FROM AUTHOR]

Published

2024

14. Role of Piezo2 in Schwann Cell Volume Regulation and Its Impact on Neurotrophic Release Regulation.

Author

Chawapun Suttinont, Katsuyuki Maeno, Mamiko Yano, Kaori Sato-Numata, Tomohiro Numata, and Moe Tsutsumi

Subjects

*CELLULAR control mechanisms, *CELL size, *SCHWANN cells, *MERKEL cells, *NERVE fibers, *TRP channels

Abstract

Background/Aims: Tactile perception relies on mechanoreceptors and nerve fibers, including c-fibers, Aβ-fibers and Aδ-fibers. Schwann cells (SCs) play a crucial role in supporting nerve fibers, with non-myelinating SCs enwrapping c-fibers and myelinating SCs ensheathing Aβ and Aδ fibers. Recent research has unveiled new functions for cutaneous sensory SCs, highlighting the involvement of nociceptive SCs in pain perception and Meissner corpuscle SCs in tactile sensation. Furthermore, Piezo2, previously associated with Merkel cell tactile sensitivity, has been identified in SCs. The goal of this study was to investigate the channels implicated in SC mechanosensitivity and the release process of neurotrophic factor secretion. Methods: Immortalized IFRS1 SCs and human primary SCs generated two distinct subtypes of SCs: undifferentiated and differentiated SCs. Quantitative PCR was employed to evaluate the expression of differentiation markers and mechanosensitive channels, including TRP channels (TRPV4, TRPM7 and TRPA1) and Piezo channels (Piezo1 and Piezo2). To validate the functionality of specific mechanosensitive channels, Ca2+ imaging and electronic cell sizing experiments were conducted under hypotonic conditions, and inhibitors and siRNAs were used. Protein expression was assessed by Western blotting and immunostaining. Additionally, secretome analysis was performed to evaluate the release of neurotrophic factors in response to hypotonic stimulation, with BDNF, a representative trophic factor, quantified using ELISA. Results: Induction of differentiation increased Piezo2 mRNA expression levels both in IFRS1 and in human primary SCs. Both cell types were responsive to hypotonic solutions, with differentiated SCs displaying a more pronounced response. Gd3+ and FM1-43 effectively inhibited hypotonicity-induced Ca2+ transients in differentiated SCs, implicating Piezo2 channels. Conversely, inhibitors of Piezo1 and TRPM7 (Dooku1 and NS8593, respectively) had no discernible impact. Moreover, Piezo2 in differentiated SCs appeared to participate in regulatory volume decreases (RVD) after cell swelling induced by hypotonic stimulation. A Piezo2 deficiency correlated with reduced RVD and prolonged cell swelling, leading to heightened release of the neurotrophic factor BDNF by upregulating the function of endogenously expressed Ca2+-permeable TRPV4. Conclusion: Our study unveils the mechanosensitivity of SCs and implicates Piezo2 channels in the release of neurotrophic factors from SCs. These results suggest that Piezo2 may contribute to RVD, thereby maintaining cellular homeostasis, and may also serve as a negative regulator of neurotrophic factor release. These findings underscore the need for further investigation into the role of Piezo2 in SC function and neurotrophic regulation. [ABSTRACT FROM AUTHOR]

Published

2024

15. Regeneration of Propriospinal Axons in Rat Transected Spinal Cord Injury through a Growth-Promoting Pathway Constructed by Schwann Cells Overexpressing GDNF.

Author

Du, Xiaolong, Zhang, Shengqi, Khabbaz, Aytak, Cohen, Kristen Lynn, Zhang, Yihong, Chakraborty, Samhita, Smith, George M., Wang, Hongxing, Yadav, Amol P., Liu, Naikui, and Deng, Lingxiao

Subjects

*GLIAL fibrillary acidic protein, *SCHWANN cells, *SPINAL cord injuries, *SPINAL cord, *GROWTH factors, *AXONS

Abstract

Unsuccessful axonal regeneration in transected spinal cord injury (SCI) is mainly attributed to shortage of growth factors, inhibitory glial scar, and low intrinsic regenerating capacity of severely injured neurons. Previously, we constructed an axonal growth permissive pathway in a thoracic hemisected injury by transplantation of Schwann cells overexpressing glial-cell-derived neurotrophic factor (SCs-GDNF) into the lesion gap as well as the caudal cord and proved that this novel permissive bridge promoted the regeneration of descending propriospinal tract (dPST) axons across and beyond the lesion. In the current study, we subjected rats to complete thoracic (T11) spinal cord transections and examined whether these combinatorial treatments can support dPST axons' regeneration beyond the transected injury. The results indicated that GDNF significantly improved graft–host interface by promoting integration between SCs and astrocytes, especially the migration of reactive astrocyte into SCs-GDNF territory. The glial response in the caudal graft area has been significantly attenuated. The astrocytes inside the grafted area were morphologically characterized by elongated and slim process and bipolar orientation accompanied by dramatically reduced expression of glial fibrillary acidic protein. Tremendous dPST axons have been found to regenerate across the lesion and back to the caudal spinal cord which were otherwise difficult to see in control groups. The caudal synaptic connections were formed, and regenerated axons were remyelinated. The hindlimb locomotor function has been improved. [ABSTRACT FROM AUTHOR]

Published

2024

16. An in vitro model for postoperative cranial nerve dysfunction and a proposed method of rehabilitation with N-acetylcysteine microparticles.

Author

Kita, Ashley, Kedeshian, Katherine, Hong, Michelle, and Hoffman, Larry

Subjects

*CRANIAL nerves, *SCHWANN cells, *ACETYLCYSTEINE, *NERVOUS system injuries, *OXIDATIVE stress

Abstract

Purpose: When operating near cranial motor nerves, transient postoperative weakness of target muscles lasting weeks to months is often observed. As nerves are typically intact at a procedure's completion, paresis is hypothesized to result from a combination of neurapraxia and axonotmesis. As both neurapraxia and axonotmesis involve Schwann cell injury and require remyelination, we developed an in vitro RSC96 Schwann cell model of injury using hydrogen peroxide (H2O2) to induce oxidative stress and investigated the efficacy of candidate therapeutic agents to promote RSC96 viability. As a first step in developing a long-term local administration strategy, the most promising of these agents was incorporated into sustained-release microparticles and investigated for bioactivity using this assay. Methods: The concentration of H2O2 which reduced viability by 50% was determined to establish a standard for inducing oxidative stress in RSC96 cultures. Fresh cultures were then co-dosed with H2O2 and the potential therapeutics melatonin, N-acetylcysteine, resveratrol, and 4-aminopyridine. Schwann cell viability was evaluated and the most efficacious agent, N-acetylcysteine, was encapsulated into microparticles. Eluted samples of N-acetylcysteine from microparticles was evaluated for retained bioactivity. Results: 100 µM N-acetylcysteine improved the viability of Schwann cells dosed with H2O2. 100 µM Microparticle-eluted N-acetylcysteine also enhanced Schwann cell viability. Conclusion: We developed a Schwann cell culture model of iatrogenic nerve injury and used this to identify N-acetylcysteine as an agent to promote recovery. N-acetylcysteine was packaged into microparticles and demonstrated promise as a locally administrable agent to reduce oxidative stress in Schwann cells. [ABSTRACT FROM AUTHOR]

Published

2024

17. Hybrid construction of tissue-engineered nerve graft using skin derived precursors induced neurons and Schwann cells to enhance peripheral neuroregeneration

Author

Qi Guo, Hui Zhu, Xi Xu, Tianyi Huang, Yulin Pan, Xiaosong Gu, Shusen Cui, and Chengbin Xue

Subjects

Skin derived precursor, Neuroregeneration, Tissue engineered nerve graft, Peripheral nerve injury, Schwann cell, Neuron, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Peripheral nerve injury is a major challenge in clinical treatment due to the limited intrinsic capacity for nerve regeneration. Tissue engineering approaches offer promising solutions by providing biomimetic scaffolds and cell sources to promote nerve regeneration. In the present work, we investigated the potential role of skin-derived progenitors (SKPs), which are induced into neurons and Schwann cells (SCs), and their extracellular matrix in tissue-engineered nerve grafts (TENGs) to enhance peripheral neuroregeneration. SKPs were induced to differentiate into neurons and SCs in vitro and incorporated into nerve grafts composed of a biocompatible scaffold including chitosan neural conduit and silk fibroin filaments. In vivo experiments using a rat model of peripheral nerve injury showed that TENGs significantly enhanced nerve regeneration compared to the scaffold control group, catching up with the autograft group. Histological analysis showed improved axonal regrowth, myelination and functional recovery in animals treated with these TENGs. In addition, immunohistochemical staining confirmed the presence of induced neurons and SCs within the regenerated nerve tissue. Our results suggest that SKP-induced neurons and SCs in tissue-engineered nerve grafts have great potential for promoting peripheral nerve regeneration and represent a promising approach for clinical translation in the treatment of peripheral nerve injury. Further optimization and characterization of these engineered constructs is warranted to improve their clinical applicability and efficacy.

Published

2024

18. Cimifugin Alleviates Chronic Constriction Injury of the Sciatic Nerve by Suppressing Inflammatory Response and Schwann Cell Apoptosis

Author

Zhang, Qijuan, Zhang, Xiaoli, He, Qing, Tian, Yu, and Liu, Zhengmao

Published

2024

19. The Protective Role of Caffeine against Histological and Ultrastructural Changes of Peripheral Nerve in Type 2 Diabetic Rats

Author

Manal A. Othman, Bhagath Kumar Potu, Aisha Rashid, Ayesha Fatima, and Wael Amin Nasr El-Din

Published

2024

20. Interruptible demyelination in avian riboflavin deficient neuropathy

Author

Zhao Cai

Subjects

Riboflavin, Demyelination, Remyelination, Teased nerve fibre, Schwann cell, Biotechnology, TP248.13-248.65, Biology (General), QH301-705.5, Biochemistry, QD415-436

Abstract

Abstract Background and aims The evolution of demyelination in individual internodes remains unclear although it has been noticed the paranodal demyelination precedes internodal demyelination in neuropathies with diverse aetiologies. For therapeutic purpose, it is fundamental to know whether the demyelinating procedure in affected internodes can be interrupted. This study aimed to delineate the development of demyelination in individual internodes in avian riboflavin deficient neuropathy. Methods Newborn broiler meat chickens were maintained either on a routine diet containing 5.0 mg/kg riboflavin, a riboflavin deficient diet containing 1.8 mg/kg riboflavin, or initially a riboflavin deficient diet for 11 days and then routine diet plus riboflavin repletion from day 12. Evolution of demyelination in individual internodes was analyzed by teased nerve fibre studies from day 11 to 21. Results In riboflavin deficient chickens, demyelination was the predominant feature: it was mainly confined to the paranodal region at day 11; extended into internodal region, but less than half of the internodal length in most affected internodes at day 16; involved more than half or whole internode at day 21. In the internode undergoing demyelination, myelin degeneration of varying degrees was noticed in the cytoplasm of the Schwann cell wrapping the internode. Two days after riboflavin repletion, co-existence of remyelination and active demyelination within individual internodes was noticed. Remyelination together with preserved short original internodes was the characteristic feature 4 and 9 days after riboflavin repletion. Conclusion Riboflavin repletion interrupts the progression from paranodal to internodal demyelination in riboflavin deficient chickens and promotes remyelination before complete internodal demyelination.

Published

2024

21. Bone Marrow Stem Cells Derived from Nerves Have Neurogenic Properties and Potential Utility for Regenerative Therapy

Author

Ott, Leah C, Han, Christopher Y, Mueller, Jessica L, Rahman, Ahmed A, Hotta, Ryo, Goldstein, Allan M, and Stavely, Rhian

Subjects

Biochemistry and Cell Biology, Biological Sciences, Medicinal and Biomolecular Chemistry, Chemical Sciences, Microbiology, Pediatric, Stem Cell Research - Embryonic - Non-Human, Stem Cell Research - Nonembryonic - Non-Human, Stem Cell Research - Nonembryonic - Human, Neurosciences, Transplantation, Regenerative Medicine, Stem Cell Research, Underpinning research, Development of treatments and therapeutic interventions, 1.1 Normal biological development and functioning, 5.2 Cellular and gene therapies, Neurological, Female, Pregnancy, Humans, Endothelial Cells, Neurogenesis, Cell Differentiation, Neural Stem Cells, Schwann Cells, Bone Marrow Cells, Neural Crest, Schwann cell, bone marrow, enteric nervous system, neural crest, neural crest stem cell, neural stem cell, neurovascular, stem cell, Other Chemical Sciences, Genetics, Other Biological Sciences, Chemical Physics, Biochemistry and cell biology, Medicinal and biomolecular chemistry

Abstract

Neurons and glia of the peripheral nervous system are derived from progenitor cell populations, originating from embryonic neural crest. The neural crest and vasculature are intimately associated during embryonic development and in the mature central nervous system, in which they form a neurovascular unit comprised of neurons, glia, pericytes, and vascular endothelial cells that play important roles in health and disease. Our group and others have previously reported that postnatal populations of stem cells originating from glia or Schwann cells possess neural stem cell qualities, including rapid proliferation and differentiation into mature glia and neurons. Bone marrow receives sensory and sympathetic innervation from the peripheral nervous system and is known to contain myelinating and unmyelinating Schwann cells. Herein, we describe a population of neural crest-derived Schwann cells residing in a neurovascular niche of bone marrow in association with nerve fibers. These Schwann cells can be isolated and expanded. They demonstrate plasticity in vitro, generating neural stem cells that exhibit neurogenic potential and form neural networks within the enteric nervous system in vivo following transplantation to the intestine. These cells represent a novel source of autologous neural stem cells for the treatment of neurointestinal disorders.

Published

2023

22. Role of secretomes in cell-free therapeutic strategies in regenerative medicine.

Author

Karimian, Aida, Khoshnazar, Seyedeh Mahdieh, Kazemi, Tahmineh, Asadi, Asadollah, and Abdolmaleki, Arash

Abstract

After an injury, peripheral nervous system neurons have the potential to rebuild their axons by generating a complicated activation response. Signals from the damaged axon are required for this genetic transition to occur. Schwann cells (SCs) near a damaged nerve's distal stump also play a role in the local modulation of axonal programs, not only via cell-to-cell contacts but also through secreted signals (the secretome). The secretome is made up of all the proteins that the cell produces, such as cytokines, growth factors, and extracellular vesicles. The released vesicles may carry signaling proteins as well as coding and regulatory RNAs, allowing for multilayer communication. The secretome of SCs is now well understood as being critical for both orchestrating Wallerian degeneration and maintaining axonal regeneration. As a consequence, secretome has emerged as a feasible tissue regeneration alternative to cell therapy. Separate SC secretome components have been used extensively in the lab to promote peripheral nerve regeneration after injury. However, in neurological therapies, the secretome generated by mesenchymal (MSC) or other derived stem cells has been the most often used. In fact, the advantages of cell treatment have been connected to the release of bioactive chemicals and extracellular vesicles, which make up MSCs' secretome. [ABSTRACT FROM AUTHOR]

Published

2024

23. Enhancing intraneural revascularization following peripheral nerve injury through hypoxic Schwann-cell-derived exosomes: an insight into endothelial glycolysis.

Author

Sun, Jun, Zeng, Qiuhua, Wu, Zhimin, Li, Zhangyu, Gao, Qun, Liao, Zhi, Li, Hao, Ling, Cong, Chen, Chuan, Wang, Hui, and Zhang, Baoyu

Subjects

*PERIPHERAL nerve injuries, *NERVOUS system regeneration, *GLYCOLYSIS, *OXYGEN consumption, *EXOSOMES, *OXIDATIVE phosphorylation, *PERIPHERAL nervous system, *GENE expression

Abstract

Background: Endothelial cell (EC)-driven intraneural revascularization (INRV) and Schwann cells-derived exosomes (SCs-Exos) both play crucial roles in peripheral nerve injury (PNI). However, the interplay between them remains unclear. We aimed to elucidate the effects and underlying mechanisms of SCs-Exos on INRV following PNI. Results: We found that GW4869 inhibited INRV, as well as that normoxic SCs-Exos (N-SCs-Exos) exhibited significant pro-INRV effects in vivo and in vitro that were potentiated by hypoxic SCs-Exos (H-SCs-Exos). Upregulation of glycolysis emerged as a pivotal factor for INRV after PNI, as evidenced by the observation that 3PO administration, a glycolytic inhibitor, inhibited the INRV process in vivo and in vitro. H-SCs-Exos more significantly enhanced extracellular acidification rate/oxygen consumption rate ratio, lactate production, and glycolytic gene expression while simultaneously suppressing acetyl-CoA production and pyruvate dehydrogenase E1 subunit alpha (PDH-E1α) expression than N-SCs-Exos both in vivo and in vitro. Furthermore, we determined that H-SCs-Exos were more enriched with miR-21-5p than N-SCs-Exos. Knockdown of miR-21-5p significantly attenuated the pro-glycolysis and pro-INRV effects of H-SCs-Exos. Mechanistically, miR-21-5p orchestrated EC metabolism in favor of glycolysis by targeting von Hippel-Lindau/hypoxia-inducible factor-1α and PDH-E1α, thereby enhancing hypoxia-inducible factor-1α-mediated glycolysis and inhibiting PDH-E1α-mediated oxidative phosphorylation. Conclusion: This study unveiled a novel intrinsic mechanism of pro-INRV after PNI, providing a promising therapeutic target for post-injury peripheral nerve regeneration and repair. [ABSTRACT FROM AUTHOR]

Published

2024

24. Interruptible demyelination in avian riboflavin deficient neuropathy.

Author

Cai, Zhao

Subjects

*VITAMIN B2, *DEMYELINATION, *NEUROPATHY, *MALNUTRITION, *SCHWANN cells, *BROILER chickens

Abstract

Background and aims: The evolution of demyelination in individual internodes remains unclear although it has been noticed the paranodal demyelination precedes internodal demyelination in neuropathies with diverse aetiologies. For therapeutic purpose, it is fundamental to know whether the demyelinating procedure in affected internodes can be interrupted. This study aimed to delineate the development of demyelination in individual internodes in avian riboflavin deficient neuropathy. Methods: Newborn broiler meat chickens were maintained either on a routine diet containing 5.0 mg/kg riboflavin, a riboflavin deficient diet containing 1.8 mg/kg riboflavin, or initially a riboflavin deficient diet for 11 days and then routine diet plus riboflavin repletion from day 12. Evolution of demyelination in individual internodes was analyzed by teased nerve fibre studies from day 11 to 21. Results: In riboflavin deficient chickens, demyelination was the predominant feature: it was mainly confined to the paranodal region at day 11; extended into internodal region, but less than half of the internodal length in most affected internodes at day 16; involved more than half or whole internode at day 21. In the internode undergoing demyelination, myelin degeneration of varying degrees was noticed in the cytoplasm of the Schwann cell wrapping the internode. Two days after riboflavin repletion, co-existence of remyelination and active demyelination within individual internodes was noticed. Remyelination together with preserved short original internodes was the characteristic feature 4 and 9 days after riboflavin repletion. Conclusion: Riboflavin repletion interrupts the progression from paranodal to internodal demyelination in riboflavin deficient chickens and promotes remyelination before complete internodal demyelination. [ABSTRACT FROM AUTHOR]

Published

2024

25. FGF21 inhibits ferroptosis caused by mitochondrial damage to promote the repair of peripheral nerve injury

Author

Yao Yan, Xinyu Ran, Zihan Zhou, Yuting Gu, Rendu Wang, Chuanqi Qiu, Yinuo Sun, Jifeng Wang, Jian Xiao, Yingfeng Lu, and Jian Wang

Subjects

peripheral nerve injury, ferroptosis, mitochondria, fibroblast growth factor 21 (FGF21), schwann cell, ROS, Therapeutics. Pharmacology, RM1-950

Abstract

Introduction Ferroptosis is a new type of cell death characterized by lipid peroxidation and iron dependency, representing an emerging disease regulation mechanism. The limited understanding of ferroptosis in peripheral nerve injury (PNI) complicates the management of such injuries. Mitochondrial dysfunction, which contributes to ferroptosis, further exacerbates the challenges of peripheral nerve repairMethodsIn this study, we established an in vitro model of Schwann cells model treated with TBHP and an in vivo sciatic nerve crush injury model in rats. These models were used to investigate the effects of fibroblast growth factor 21 (FGF21) on PNI, both in vitro and in vivo, and to explore the potential mechanisms linking injury-induced ferroptosis and mitochondrial dysfunction.Results Our findings reveal that PNI triggers abnormal accumulation of lipid reactive oxygen species (ROS) and inactivates mitochondrial respiratory chain complex III, leading to mitochondrial dysfunction. This dysfunction catalyzes the oxidation of excessive polyunsaturated fatty acids, resulting in antioxidant imbalance and loss of ferroptosis suppressor protein 1 (FSP1), which drives lipid peroxidation. Additionally, irregular iron metabolism, defective mitophagy, and other factors contribute to the induction of ferroptosis. Importantly, we found that FGF21 attenuates the abnormal accumulation of lipid ROS, restores mitochondrial function, and suppresses ferroptosis, thus promoting PNI repair. Notably, glutathione peroxidase 4 (GPX4), a downstream target of nuclear factor E2-related factor 2 (Nrf2), and the ERK/Nrf2 pathway are involved in the regulation of ferroptosis by FGF21.ConclusionFGF21 promotes peripheral nerve repair by inhibiting ferroptosis caused by mitochondrial dysfunction. Therefore, targeting mitochondria and ferroptosis represents a promising therapeutic strategy for effective PNI repair.

Published

2024

26. Targeting PI3K/Akt/mTOR signaling in rodent models of PMP22 gene-dosage diseases

Author

Doris Krauter, Daniela Stausberg, Timon J Hartmann, Stefan Volkmann, Theresa Kungl, David A Rasche, Gesine Saher, Robert Fledrich, Ruth M Stassart, Klaus-Armin Nave, Sandra Goebbels, David Ewers, and Michael W Sereda

Subjects

Charcot–Marie–Tooth Neuropathies, Peripheral Myelin Protein of 22 kDa, Myelin, Schwann Cell, PI3K/Akt/mTOR Signaling, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Haplo-insufficiency of the gene encoding the myelin protein PMP22 leads to focal myelin overgrowth in the peripheral nervous system and hereditary neuropathy with liability to pressure palsies (HNPP). Conversely, duplication of PMP22 causes Charcot-Marie-Tooth disease type 1A (CMT1A), characterized by hypomyelination of medium to large caliber axons. The molecular mechanisms of abnormal myelin growth regulation by PMP22 have remained obscure. Here, we show in rodent models of HNPP and CMT1A that the PI3K/Akt/mTOR-pathway inhibiting phosphatase PTEN is correlated in abundance with PMP22 in peripheral nerves, without evidence for direct protein interactions. Indeed, treating DRG neuron/Schwann cell co-cultures from HNPP mice with PI3K/Akt/mTOR pathway inhibitors reduced focal hypermyelination. When we treated HNPP mice in vivo with the mTOR inhibitor Rapamycin, motor functions were improved, compound muscle amplitudes were increased and pathological tomacula in sciatic nerves were reduced. In contrast, we found Schwann cell dedifferentiation in CMT1A uncoupled from PI3K/Akt/mTOR, leaving partial PTEN ablation insufficient for disease amelioration. For HNPP, the development of PI3K/Akt/mTOR pathway inhibitors may be considered as the first treatment option for pressure palsies.

Published

2024

27. The physiological role of the unfolded protein response in the nervous system

Author

Shuangchan Wu and Wensheng Lin

Subjects

myelin, neuron, oligodendrocyte, schwann cell, unfolded protein response, Neurology. Diseases of the nervous system, RC346-429

Abstract

The unfolded protein response (UPR) is a cellular stress response pathway activated when the endoplasmic reticulum, a crucial organelle for protein folding and modification, encounters an accumulation of unfolded or misfolded proteins. The UPR aims to restore endoplasmic reticulum homeostasis by enhancing protein folding capacity, reducing protein biosynthesis, and promoting protein degradation. It also plays a pivotal role in coordinating signaling cascades to determine cell fate and function in response to endoplasmic reticulum stress. Recent research has highlighted the significance of the UPR not only in maintaining endoplasmic reticulum homeostasis but also in influencing various physiological processes in the nervous system. Here, we provide an overview of recent findings that underscore the UPR’s involvement in preserving the function and viability of neuronal and myelinating cells under physiological conditions, and highlight the critical role of the UPR in brain development, memory storage, retinal cone development, myelination, and maintenance of myelin thickness.

Published

2024

28. Role of transforming growth factor-β in peripheral nerve regeneration

Author

Zihan Ding, Maorong Jiang, Jiaxi Qian, Dandan Gu, Huiyuan Bai, Min Cai, and Dengbing Yao

Subjects

myelination, nerve repair and regeneration, neurite, neuroinflammation, peripheral nerve injury, schwann cell, transforming growth factor-β, wallerian degeneration, Neurology. Diseases of the nervous system, RC346-429

Abstract

Injuries caused by trauma and neurodegenerative diseases can damage the peripheral nervous system and cause functional deficits. Unlike in the central nervous system, damaged axons in peripheral nerves can be induced to regenerate in response to intrinsic cues after reprogramming or in a growth-promoting microenvironment created by Schwann cells. However, axon regeneration and repair do not automatically result in the restoration of function, which is the ultimate therapeutic goal but also a major clinical challenge. Transforming growth factor (TGF) is a multifunctional cytokine that regulates various biological processes including tissue repair, embryo development, and cell growth and differentiation. There is accumulating evidence that TGF-β family proteins participate in peripheral nerve repair through various factors and signaling pathways by regulating the growth and transformation of Schwann cells; recruiting specific immune cells; controlling the permeability of the blood-nerve barrier, thereby stimulating axon growth; and inhibiting remyelination of regenerated axons. TGF-β has been applied to the treatment of peripheral nerve injury in animal models. In this context, we review the functions of TGF-β in peripheral nerve regeneration and potential clinical applications.

Published

2024

29. Development of a ZRS Reporter System for the Newt (Cynops pyrrhogaster) During Terrestrial Limb Regeneration

Author

Martin Miguel Casco-Robles, Ryosuke Ikeda, Fumiaki Maruo, and Chikafumi Chiba

Subjects

newt, limb regeneration, Shh, Schwann cell, pattern formation, ZPA, Biology (General), QH301-705.5

Abstract

Background: Newts, a type of urodele amphibian, offer remarkable insights into regenerative medicine due to their extraordinary tissue regeneration capabilities—a challenging feat in humans. During limb regeneration of adult newts, fascinating cellular and molecular processes are revealed, including scarless healing, de-differentiation of mature cells, and regeneration of limbs and digits. Sonic hedgehog (Shh), crucial for vertebrate limb development, is regulated by the zone of polarizing activity regulatory sequence (ZRS) in the limb bud zone of polarizing activity (ZPA). The metamorphosed (terrestrial) newt can reactivate Shh during regeneration, facilitating proper limb patterning. Cell types capable of regulating the ZRS in metamorphosed newts remain unknown. The identification of such cell types provides invaluable insight into novel regenerative mechanisms. Objective: In this study, we developed the first newt ZRS reporter. Methods: We isolated and characterized the newt ZRS enhancer (nZRS), identifying conserved DNA binding sites. Several binding sites with medical relevance were conserved in the newt ZRS. In functional analysis, we developed a system composed of a transgenic nZRS reporter newt and a new newt anti-Shh antibody, which allowed Shh monitoring during limb regeneration. Results: We identified a group of Schwann cells capable of ZRS reporter and Shh protein expression during terrestrial limb regeneration. Conclusions: This system provides a valuable in vivo approach for future genetic studies of patterning during limb regeneration.

Published

2024

30. Targeting PI3K/Akt/mTOR signaling in rodent models of PMP22 gene-dosage diseases.

Author

Krauter, Doris, Stausberg, Daniela, Hartmann, Timon J, Volkmann, Stefan, Kungl, Theresa, Rasche, David A, Saher, Gesine, Fledrich, Robert, Stassart, Ruth M, Nave, Klaus-Armin, Goebbels, Sandra, Ewers, David, and Sereda, Michael W

Abstract

Haplo-insufficiency of the gene encoding the myelin protein PMP22 leads to focal myelin overgrowth in the peripheral nervous system and hereditary neuropathy with liability to pressure palsies (HNPP). Conversely, duplication of PMP22 causes Charcot-Marie-Tooth disease type 1A (CMT1A), characterized by hypomyelination of medium to large caliber axons. The molecular mechanisms of abnormal myelin growth regulation by PMP22 have remained obscure. Here, we show in rodent models of HNPP and CMT1A that the PI3K/Akt/mTOR-pathway inhibiting phosphatase PTEN is correlated in abundance with PMP22 in peripheral nerves, without evidence for direct protein interactions. Indeed, treating DRG neuron/Schwann cell co-cultures from HNPP mice with PI3K/Akt/mTOR pathway inhibitors reduced focal hypermyelination. When we treated HNPP mice in vivo with the mTOR inhibitor Rapamycin, motor functions were improved, compound muscle amplitudes were increased and pathological tomacula in sciatic nerves were reduced. In contrast, we found Schwann cell dedifferentiation in CMT1A uncoupled from PI3K/Akt/mTOR, leaving partial PTEN ablation insufficient for disease amelioration. For HNPP, the development of PI3K/Akt/mTOR pathway inhibitors may be considered as the first treatment option for pressure palsies. Synopsis: Genetic and pharmacologic targeting of the PTEN/PI3K/Akt/mTOR signaling pathway was used as a potential therapeutic strategy in the peripheral neuropathies Hereditary Neuropathy with Liability to Pressure Palsies (HNPP) and Charcot Marie Tooth disease type 1A (CMT1A). Abundance of PTEN as the major inhibitor of the PI3K/Akt/mTOR signaling pathway is decreased in HNPP and increased in CMT1A rodent models. Inhibiting mTOR downstream of PTEN improves the behavioral, electrophysiological and histological disease phenotype in a mouse model of HNPP. Genetic targeting of PTEN in Schwann cells only transiently increased myelin growth in CMT1A model mice due to a differentiation defect, which is not present in HNPP nerves. Genetic and pharmacologic targeting of the PTEN/PI3K/AKT/mTOR signaling pathway was used as a potential therapeutic strategy in the peripheral neuropathies Hereditary Neuropathy with Liability to Pressure Palsies (HNPP) and Charcot Marie Tooth disease type 1A (CMT1A). [ABSTRACT FROM AUTHOR]

Published

2024

31. 1% 富血小板血浆联合骨髓间充质干细胞促进周围神经损伤的修复.

Author

冯睿钦, 韩 娜, 张 蒙, 谷馨怡, and 张丰识

Subjects

*STEM cell culture, *MESENCHYMAL stem cells, *SCIATIC nerve injuries, *PERIPHERAL nerve injuries, *CELL morphology, *PLATELET-rich plasma, *BONE marrow

Abstract

BACKGROUND: Platelet-rich plasma has been shown to enhance the viability and the pro-angiogenesis capacity of mesenchymal stem cells. Extracellular vesicles are one of the key mediators for mesenchymal stem cells to exert their effects, but currently, it is unclear whether platelet-rich plasma affects the functions of extracellular vesicles. OBJECTIVE: To investigate the effects of platelet-rich plasma on the function of extracellular vesicles from bone marrow mesenchymal stem cells, verify whether platelet-rich plasma can be used as an adjuvant to enhance the healing effects of bone marrow mesenchymal stem cells on repairing the peripheral nerve injury. METHODS: For in vitro study, bone marrow mesenchymal stem cells were cultured under normal conditions and with 1% platelet-rich plasma. The ultracentrifugation was used to extract the extracellular vesicles produced by bone marrow mesenchymal stem cells cultured under normal conditions (EVs-nor) or the condition supplemented with 1% platelet-rich plasma (EVs-prp). Extracellular vesicles were used to incubate with Schwann cells. The EdU assay, western blot assay, qPCR and light microscopy photography were performed to examine the effects of EVs-nor and EVs-prp on Schwann cell reprogramming, which was characterized by cell proliferation, c-Jun expression, reprogramming-associated gene expression and cell morphology. For in vivo study, the model of sciatic nerve injury in rats was established. Bone marrow mesenchymal stem cells were grafted with or without 1% platelet-rich plasma into the injured rat sciatic nerve using a chitin nerve conduit. Eight weeks after the surgery, the recovery was assessed by histological and functional indexes, including regenerated nerve fiber density, gastrocnemius wet weight ratio and sciatic function index. RESULTS AND CONCLUSION: (1) Compared with EVs-nor, EVs-prp was stronger in promoting Schwann cell proliferation. The gene expressions of c-Jun and GDNF were significantly upregulated in EVs-prp treated Schwann cells. The morphology of Schwann cells was significantly longer in EVs-prp group than that in EVs-nor group, indicating that EVs-prp had a stronger ability to stimulate Schwann cell reprogramming than EVs-nor. (2) Sciatic nerve injury animal experiment results revealed that grafting mesenchymal stem cells along with platelet-rich plasma into the injured sciatic nerve showed the best recovery compared with grafting mesenchymal stem cells or platelet-rich plasma alone, demonstrated by the significantly improved density of nerve fibers, gastrocnemius wet weight ratio, and sciatic function index. (3) These results suggested that platelet-rich plasma improved the function of bone marrow mesenchymal stem cell-derived extracellular vesicles and could be served as a practical and feasible preparation to synergize with bone marrow mesenchymal stem cells to improve peripheral nerve repair. [ABSTRACT FROM AUTHOR]

Published

2024

32. Dihydromyricetin reverses capecitabine‐induced peripheral myelin dysfunction through modulation of oxidative stress.

Author

Fang, Jie, Lou, Shuyi, Zhou, Xinyi, Lou, Dayong, Zhou, Liqin, and Bian, Rong

Abstract

Previous clinical reports have shown that capecitabine, an oral prodrug of 5‐fluorouracil (5‐Fu), can induce peripheral neuropathy, resulting in numbness, paresthesia and hypoesthesia. However, the mechanism through which capecitabine causes peripheral nerve injury remains unclear. Here, we demonstrate that systemic administration of capecitabine leads to myelin abnormalities in the peripheral nerves of mice, which are possibly attributed to the death of Schwann cells, the myelinating cells in the peripheral nervous system. Furthermore, our results show that 5‐Fu induces significant oxidative stress in Schwann cells by inhibiting the expression of the anti‐oxidative protein DJ‐1, leading to a decrease in Schwann cell markers. We found that the anti‐oxidant dihydromyricetin (DMY) reverses 5‐Fu‐induced Schwann cell death and oxidative stress and alleviates capecitabine‐induced myelin abnormalities. Taken together, our data indicate that capecitabine induces peripheral myelin dysfunction by regulating DJ‐1‐mediated oxidative stress in Schwann cells and reveal DMY as a potential therapeutic strategy for capecitabine‐induced peripheral neuropathy. [ABSTRACT FROM AUTHOR]

Published

2024

33. Schwann cells acquire a repair phenotype after assembling into spheroids and show enhanced in vivo therapeutic potential for promoting peripheral nerve repair.

Author

Shih-Heng Chen, Hsin-Wen Wang, Pei-Ching Yang, Shih-Shien Chen, Chia-Hsin Ho, Ying-Chi Kao, Shao-Wen Liu, Han Chiu, Yu-Jie Lin, Er-Yuan Chuang, Jen-Huang Huang, Huang-Kai Kao, and Chieh-Cheng Huang

Subjects

*NERVOUS system regeneration, *PERIPHERAL nervous system, *SCHWANN cells, *SUPERIOR colliculus, *MYELIN sheath, *DORSAL root ganglia, *SCIATIC nerve, *PHENOTYPES

Abstract

The prognosis for postinjury peripheral nerve regeneration remains suboptimal. Although transplantation of exogenous Schwann cells (SCs) has been considered a promising treatment to promote nerve repair, this strategy has been hampered in practice by the limited availability of SC sources and an insufficient postengraftment cell retention rate. In this study, to address these challenges, SCs were aggregated into spheroids before being delivered to an injured rat sciatic nerve. We found that the three-dimensional aggregation of SCs induced their acquisition of a repair phenotype, as indicated by enhanced levels of c-Jun expression/activation and decreased expression of myelin sheath protein. Furthermore, our in vitro results demonstrated the superior potential of the SC spheroid-derived secretome in promoting neurite outgrowth of dorsal root ganglion neurons, enhancing the proliferation and migration of endogenous SCs, and recruiting macrophages. Moreover, transplantation of SC spheroids into rats after sciatic nerve transection effectively increased the postinjury nerve structure restoration and motor functional recovery rates, demonstrating the therapeutic potential of SC spheroids. In summary, transplantation of preassembled SC spheroids may hold great potential for enhancing the cell delivery efficiency and the resultant therapeutic outcome, thereby improving SC-based transplantation approaches for promoting peripheral nerve regeneration. [ABSTRACT FROM AUTHOR]

Published

2024

34. Role of catecholamine synthases in the maintenance of cancer stem‐like cells in malignant peripheral nerve sheath tumors.

Author

Katayama, Haruyoshi, Fujimura, Atsushi, Huang, Rongsheng, Otani, Yusuke, Itano, Takuto, Fujiwara, Tomohiro, Kunisada, Toshiyuki, Nakata, Eiji, and Ozaki, Toshifumi

Abstract

Malignant peripheral nerve sheath tumors (MPNSTs) are malignant tumors that are derived from Schwann cell lineage around peripheral nerves. As in many other cancer types, cancer stem cells (CSCs) have been identified in MPNSTs, and they are considered the cause of treatment resistance, recurrence, and metastasis. As an element defining the cancer stemness of MPNSTs, we previously reported a molecular mechanism by which exogenous adrenaline activates a core cancer stemness factor, YAP/TAZ, through β2 adrenoceptor (ADRB2). In this study, we found that MPNST cells express catecholamine synthases and that these enzymes are essential for maintaining cancer stemness, such as the ability to self‐renew and maintain an undifferentiated state. Through gene knockdown and inhibition of these enzymes, we confirmed that catecholamines are indeed synthesized in MPNST cells. The results confirmed that catecholamine synthase knockdown in MPNST cells reduces the activity of YAP/TAZ. These data suggest that a mechanism of YAP/TAZ activation by de novo synthesized adrenaline, as well as exogenous adrenaline, may exist in the maintenance of cancer stemness of MPNST cells. This mechanism not only helps to understand the pathology of MPNST, but could also contribute to the development of therapeutic strategies for MPNST. [ABSTRACT FROM AUTHOR]

Published

2024

35. Age-related structural and functional changes of the intracardiac nervous system.

Author

Sassu, Eliza, Tumlinson, Gavin, Stefanovska, Dragana, Fernández, Marbely C., Iaconianni, Pia, Madl, Josef, Brennan, Tomás A., Koch, Manuel, Cameron, Breanne A., Preissl, Sebastian, Ravens, Ursula, Schneider-Warme, Franziska, Kohl, Peter, Zgierski-Johnston, Callum M., and Hortells, Luis

Subjects

*HEART, *ATRIOVENTRICULAR node, *NERVOUS system, *MUSCARINIC receptors, *HEART conduction system, *CHONDROITIN sulfate proteoglycan, *MUSCARINIC acetylcholine receptors, *PERIPHERAL nervous system

Abstract

Although aging is known to be associated with an increased incidence of both atrial and ventricular arrhythmias, there is limited knowledge about how Schwann cells (SC) and the intracardiac nervous system (iCNS) remodel with age. Here we investigate the differences in cardiac SC, parasympathetic nerve fibers, and muscarinic acetylcholine receptor M2 (M2R) expression in young and old mice. Additionally, we examine age-related changes in cardiac responses to sympathomimetic and parasympathomimetic drugs. Lower SC density, lower SC proliferation and fewer parasympathetic nerve fibers were observed in cardiac and, as a control sciatic nerves from old (20–24 months) compared to young mice (2–3 months). In old mice, chondroitin sulfate proteoglycan 4 (CSPG4) was increased in sciatic but not cardiac nerves. Expression of M2R was lower in ventricular myocardium and ventricular conduction system from old mice compared to young mice, while no significant difference was seen in M2R expression in sino-atrial or atrio-ventricular node pacemaker tissue. Heart rate was slower and PQ intervals were longer in Langendorff-perfused hearts from old mice. Ventricular tachycardia and fibrillation were more frequently observed in response to carbachol administration in hearts from old mice versus those from young mice. On the background of reduced presence of SC and parasympathetic nerve fibers, and of lower M2R expression in ventricular cardiomyocytes and conduction system of aged hearts, the propensity of ventricular arrhythmogenesis upon parasympathomimetic drug application is increased. Whether this is caused by an increase in heterogeneity of iCNS structure and function remains to be elucidated. [Display omitted] • Reduced Schwann cell density and proliferation are observed in aged intracardiac and peripheral nervous systems. • Deposits of acidic polysaccharides, for example CSPG4, can be found in sciatic nerves from old but not young mice. • Less parasympathetic nerve fibers are detected in aged peripheral nerves and cardiac nerves. • Less muscarininc acetylcholine receptor M2 expression is found in aged ventricular cardiomyocytes and conduction system. • Langendorff-perfused hearts from old mice are more prone to ventricular arrhythmias upon carbachol stimulation. [ABSTRACT FROM AUTHOR]

Published

2024

36. X-linked Charcot Marie Tooth mutations alter CO2 sensitivity of connexin32 hemichannels.

Author

Butler, Jack and Dale, Nicholas

Subjects

SCHWANN cells, DENTAL pathology, GENETIC mutation, CARBON dioxide, EXTRACELLULAR space

Abstract

Connexin32 (Cx32) is expressed in myelinating Schwann cells. It forms both reflexive gap junctions, to facilitate transfer of molecules from the outer to the inner myelin layers and hemichannels at the paranode to permit action potential-evoked release of ATP into the extracellular space. Loss of function mutations in Cx32 cause X-linked Charcot Marie Tooth disease (CMTX), a slowly developing peripheral neuropathy. The mechanistic links between Cx32 mutations and CMTX are not well understood. As Cx32 hemichannels can be opened by increases in PCO2, we have examined whether CMTX mutations alter this CO2 sensitivity. By using Ca2+ imaging, dye loading and genetically encoded ATP sensors to measure ATP release, we have found 5 CMTX mutations that abolish the CO2 sensitivity of Cx32 hemichannels (A88D, 111–116 Del, C179Y, E102G, V139M). Others cause a partial loss (L56F, R220Stop, and R15W). Some CMTX mutations have no apparent effect on CO2 sensitivity (R15Q, L9F, G12S, V13L, V84I, W133R). The mutation R15W alters multiple additional aspects of hemichannel function including Ca2+ and ATP permeability. The mutations that abolish CO2 sensitivity are transdominant and abolish CO2 sensitivity of co-expressed Cx32WT. We have shown that Schwannoma RT4 D6P2T cells can release ATP in response to elevated PCO2 via the opening of Cx32. This is consistent with the hypothesis that the CO2 sensitivity of Cx32 may be important for maintenance of healthy myelin. Our data, showing a transdominant effect of certain CMTX mutations on CO2 sensitivity, may need to be taken into account in any future gene therapies for this condition. [ABSTRACT FROM AUTHOR]

Published

2024

37. Investigating neuroectodermal transdifferentiation : how do CNS progenitors form Schwann cells?

Author

Chen, Civia, Arthur-Farraj, Peter, and Franklin, Robin

Subjects

Central nervous system, Myelin, oligodendrocyte progenitor cell, remyelination, Schwann cell

Abstract

Myelin sheaths provide trophic support to axons, allow rapid nerve impulse conduction and are critical for neuronal function. Under homeostatic conditions, axons of the central nervous system (CNS) are myelinated by oligodendrocytes. However, in response to demyelination, Schwann cells (SCs), the myelinating glia of the peripheral nervous system (PNS), can contribute to CNS remyelination. Although CNS-resident SCs were previously thought to have migrated into the CNS from peripheral sources, lineage tracing studies demonstrated that adult CNS progenitors, oligodendrocyte progenitor cells (OPCs), can produce SCs in vivo. The mechanisms underlying this damage-induced plasticity of OPC fate choice remain incompletely understood. Therefore, in this thesis I sought to understand how changes in the lesion environment alter the differentiation trajectories of individual OPCs, and to determine how these factors affect the transcriptional control of OPC fate choices. Using single-cell RNA-sequencing I identified a subpopulation of OPCs within the demyelinating lesion that co-express SC markers. Within this SC primed group, differential gene analysis revealed a significant upregulation of genes involved in integrin signalling and with bone morphogenetic protein (BMP) activation. I showed that recapitulating the lesion environment by exposing cultured OPCs to vitronectin and BMP4 is sufficient to induce a SC fate within one week of induction. OPC-derived SCs morphologically and transcriptionally resemble primary SCs, and when transplanted into the CNS can survive and myelinate host CNS axons with peripheral type myelin. Subsequently, I found that these external pathways can directly interact with Olig2 and Sox10, which are critical regulators of cell fate in oligodendroglial cells and SCs. I then showed that OPCs can be directly reprogrammed toward a SC fate by manipulating the expression levels of Olig2 and Sox10. To further characterise the molecular changes that accompany the phenotypic conversion, I used single-cell RNA-sequencing to identify the core biological processes required for SC differentiation, and to show that successfully converted OPC-derived SCs express a number of transcriptional hallmarks of peripheral SCs. Together, these findings indicate that injury-related changes in the environment can destabilise oligodendroglial transcription factor networks, which enable alternative OPC fate choices, and reveal deeper insights into the mechanisms underlying OPC cell fate decisions during CNS remyelination.

Published

2022

38. Adenosine A2A receptor as a potential regulator of Mycobacterium leprae survival mechanisms: new insights into leprosy neural damage

Author

Plinio Marcos Freire dos Santos, Chyntia Carolina Díaz Acosta, Thabatta Leal Silveira Andrezo Rosa, Michelle Harumi Ishiba, André Alves Dias, Antonio Marcos Rodrigues Pereira, Luísa Domingos Gutierres, Melissa Pontes Pereira, Matheus da Silva Rocha, Patrícia Sammarco Rosa, Daniele F. F. Bertoluci, José Roberto Meyer-Fernandes, Fabricio da Mota Ramalho Costa, Maria Angela M. Marques, John T. Belisle, Roberta Olmo Pinheiro, Luciana Silva Rodrigues, Maria Cristina Vidal Pessolani, and Marcia Berrêdo-Pinho

Subjects

Leprosy, schwann cell, M. leprae, adenosinergic system, A2A receptor, lipid droplet, Therapeutics. Pharmacology, RM1-950

Abstract

BackgroundLeprosy is a chronic infectious disease caused by Mycobacterium leprae, which can lead to a disabling neurodegenerative condition. M. leprae preferentially infects skin macrophages and Schwann cells–glial cells of the peripheral nervous system. The infection modifies the host cell lipid metabolism, subverting it in favor of the formation of cholesterol-rich lipid droplets (LD) that are essential for bacterial survival. Although researchers have made progress in understanding leprosy pathogenesis, many aspects of the molecular and cellular mechanisms of host–pathogen interaction still require clarification. The purinergic system utilizes extracellular ATP and adenosine as critical signaling molecules and plays several roles in pathophysiological processes. Furthermore, nucleoside surface receptors such as the adenosine receptor A2AR involved in neuroimmune response, lipid metabolism, and neuron–glia interaction are targets for the treatment of different diseases. Despite the importance of this system, nothing has been described about its role in leprosy, particularly adenosinergic signaling (AdoS) during M. leprae–Schwann cell interaction.MethodsM. leprae was purified from the hind footpad of athymic nu/nu mice. ST88-14 human cells were infected with M. leprae in the presence or absence of specific agonists or antagonists of AdoS. Enzymatic activity assays, fluorescence microscopy, Western blotting, and RT-qPCR analysis were performed. M. leprae viability was investigated by RT-qPCR, and cytokines were evaluated by enzyme-linked immunosorbent assay.ResultsWe demonstrated that M. leprae-infected Schwann cells upregulated CD73 and ADA and downregulated A2AR expression and the phosphorylation of the transcription factor CREB (p-CREB). On the other hand, activation of A2AR with its selective agonist, CGS21680, resulted in: 1) reduced lipid droplets accumulation and pro-lipogenic gene expression; 2) reduced production of IL-6 and IL-8; 3) reduced intracellular M. leprae viability; 4) increased levels of p-CREB.ConclusionThese findings suggest the involvement of the AdoS in leprosy neuropathogenesis and support the idea that M. leprae, by downmodulating the expression and activity of A2AR in Schwann cells, decreases A2AR downstream signaling, contributing to the maintenance of LD accumulation and intracellular viability of the bacillus.

Published

2024

39. The role of dynamic interplay exists between sympathetic and parasympathetic nerve in gastric tumorigenesis

Author

Diqun Chen, Xunjun Li, Yiyun Wang, Xinxin Li, Hongxia Zhang, Lina Zhang, Jia Yang, Haoyang Tan, Yingxin Xie, Yingyi Liuzhou, Jiayun Qiu, Miao Shi, Feiran Zhang, Wu Zhong, Kexing Xi, Chuanfa Fang, Alpha Ibrahima Balde, Jiang Yu, and Tao Chen

Subjects

bioinformatics, gastric precancerous lesion, immunohistochemistry, parasympathetic nerve, Schwann cell, sympathetic nerve, Medical technology, R855-855.5, Biotechnology, TP248.13-248.65

Abstract

Abstract Recent research underscores the significance of the nervous system in tumor progression. Nonetheless, understanding the intricate roles of nerves in gastric tumorigenesis remains limited. Our study aims to elucidate nerve alterations, associated key genes, and signaling pathways during gastric tumorigenesis. We enroll 257 patients with gastric precancerous lesions (GPLs) from four national cohorts. Utilizing immunohistochemistry and digital analysis, we quantified the densities of sympathetic and parasympathetic nerves, as well as Schwann cells in patient slides. We collected three mRNA expression profiles of GPL samples from the gene expression omnibus database and assessed them for nerve expression signatures, differentially expressed genes, enriched pathways, and the immune microenvironment. Parasympathetic nerve and Schwann cell densities display a progressive increase, while sympathetic nerve exhibits an inverse trend along the precancerous spectrums. Notably, CD8+ T cells, natural killer cells, and antigen‐presenting cells (APC) co‐inhibition decrease, while epithelial‐mesenchymal transition increases significantly from early to late premalignancy. Several key nerve‐regulating genes (NTRK3, MYBL2, NRP1, BCL2, CCND1, VEGFA, PLXNA2, ADRB2), and pathways (mitogen‐activated protein kinase [MAPK]/ERK, PI3K/AKT, Wnt) emerge as potential contributors to precancerous progression. Our study reveals a dynamic relationship between sympathetic and parasympathetic nerves, characterized by a gradual increase in parasympathetic nerve and Schwann cell density, contrasting with an inverse trend in sympathetic nerve across precancerous spectrums. Targeting the interaction between tumor cells and nerves, including sympathetic and parasympathetic nerves, has emerged as a promising strategy for the prevention and treatment of gastric cancer.

Published

2024

40. Chondroitinase ABC combined with Schwann cell transplantation enhances restoration of neural connection and functional recovery following acute and chronic spinal cord injury

Author

Wenrui Qu, Xiangbing Wu, Wei Wu, Ying Wang, Yan Sun, Lingxiao Deng, Melissa Walker, Chen Chen, Heqiao Dai, Qi Han, Ying Ding, Yongzhi Xia, George Smith, Rui Li, Nai-Kui Liu, and Xiao-Ming Xu

Subjects

axonal regrowth, bladder function, chondroitinase abc, functional recovery, glial scar, lentivirus, migration, schwann cell, spinal cord injury, transplantation, Neurology. Diseases of the nervous system, RC346-429

Abstract

Schwann cell transplantation is considered one of the most promising cell-based therapy to repair injured spinal cord due to its unique growth-promoting and myelin-forming properties. A the Food and Drug Administration-approved Phase I clinical trial has been conducted to evaluate the safety of transplanted human autologous Schwann cells to treat patients with spinal cord injury. A major challenge for Schwann cell transplantation is that grafted Schwann cells are confined within the lesion cavity, and they do not migrate into the host environment due to the inhibitory barrier formed by injury-induced glial scar, thus limiting axonal reentry into the host spinal cord. Here we introduce a combinatorial strategy by suppressing the inhibitory extracellular environment with injection of lentivirus-mediated transfection of chondroitinase ABC gene at the rostral and caudal borders of the lesion site and simultaneously leveraging the repair capacity of transplanted Schwann cells in adult rats following a mid-thoracic contusive spinal cord injury. We report that when the glial scar was degraded by chondroitinase ABC at the rostral and caudal lesion borders, Schwann cells migrated for considerable distances in both rostral and caudal directions. Such Schwann cell migration led to enhanced axonal regrowth, including the serotonergic and dopaminergic axons originating from supraspinal regions, and promoted recovery of locomotor and urinary bladder functions. Importantly, the Schwann cell survival and axonal regrowth persisted up to 6 months after the injury, even when treatment was delayed for 3 months to mimic chronic spinal cord injury. These findings collectively show promising evidence for a combinatorial strategy with chondroitinase ABC and Schwann cells in promoting remodeling and recovery of function following spinal cord injury.

Published

2025

41. Treating amyotrophic lateral sclerosis with allogeneic Schwann cell–derived exosomal vesicles: a case report

Author

Pascal J. Goldschmidt-Clermont, Aisha Khan, George Jimsheleishvili, Patricia Graham, Adriana Brooks, Risset Silvera, Alexander J.P. Goldschmidt, Damien D. Pearse, W. Dalton Dietrich, Allan D. Levi, and James D. Guest

Subjects

allogeneic, amyotrophic lateral sclerosis, exosomes, infusion, neuromuscular junction, schwann cell, Neurology. Diseases of the nervous system, RC346-429

Abstract

Schwann cells are essential for the maintenance and function of motor neurons, axonal networks, and the neuromuscular junction. In amyotrophic lateral sclerosis, where motor neuron function is progressively lost, Schwann cell function may also be impaired. Recently, important signaling and potential trophic activities of Schwann cell-derived exosomal vesicles have been reported. This case report describes the treatment of a patient with advanced amyotrophic lateral sclerosis using serial intravenous infusions of allogeneic Schwann cell-derived exosomal vesicles, marking, to our knowledge, the first instance of such treatment. An 81-year-old male patient presented with a 1.5-year history of rapidly progressive amyotrophic lateral sclerosis. After initial diagnosis, the patient underwent a combination of generic riluzole, sodium phenylbutyrate for the treatment of amyotrophic lateral sclerosis, and taurursodiol. The patient volunteered to participate in an FDA-approved single-patient expanded access treatment and received weekly intravenous infusions of allogeneic Schwann cell-derived exosomal vesicles to potentially restore impaired Schwann cell and motor neuron function. We confirmed that cultured Schwann cells obtained from the amyotrophic lateral sclerosis patient via sural nerve biopsy appeared impaired (senescent) and that exposure of the patient’s Schwann cells to allogeneic Schwann cell-derived exosomal vesicles, cultured expanded from a cadaver donor improved their growth capacity in vitro. After a period of observation lasting 10 weeks, during which amyotrophic lateral sclerosis Functional Rating Scale-Revised and pulmonary function were regularly monitored, the patient received weekly consecutive infusions of 1.54 × 1012 (×2), and then consecutive infusions of 7.5 × 1012 (×6) allogeneic Schwann cell-derived exosomal vesicles diluted in 40 mL of Dulbecco’s phosphate-buffered saline. None of the infusions were associated with adverse events such as infusion reactions (allergic or otherwise) or changes in vital signs. Clinical lab serum neurofilament and cytokine levels measured prior to each infusion varied somewhat without a clear trend. A more sensitive in-house assay suggested possible inflammasome activation during the disease course. A trend for clinical stabilization was observed during the infusion period. Our study provides a novel approach to address impaired Schwann cells and possibly motor neuron function in patients with amyotrophic lateral sclerosis using allogeneic Schwann cell-derived exosomal vesicles. Initial findings suggest that this approach is safe.

Published

2025

42. THE ROLE OF SCHWANN CELLS IN THE PATHOLOGY OF THE HUMAN APPENDIX IN CHILDREN

Author

M. KAPITONOVA, I.B. BROHI, S. GUPALO, A.V. SMIRNOV, V.S. PETRENYUK, and A. AHMAD

Subjects

appendix, schwann cell, s100 protein, pcna, appendicitis, chronic abdominal syndrome., Public aspects of medicine, RA1-1270

Abstract

Objective: To compare the immunohistochemical (IHC) characteristics of appendices removed from children with acute appendicitis and chronic pain syndrome (CP) in the right lower quadrant of the abdomen (RLQA), as well as to define clinical and morphological correlations. Methods: The structure of fifty-one appendices of children aged 5-14 years who underwent appendectomy for chronic appendicitis/CP in the RLQA (24 patients, Group 1) and acute appendicitis (27 patients, Group 2) was assessed. Image analysis of histological sections stained with hematoxylin-eosin and immunohistochemically for S100 protein and proliferating cell nuclear antigen (PCNA) was performed. Results: Image analysis showed the presence of a significantly higher volume density (VD) and numerical density (ND) (p

Published

2023

43. What happens when Schwann cells are exposed to Mycobacterium leprae – A systematic review

Author

Lara Machado de Oliveira Brügger, Marina Monnerat Lemos dos Santos, Flavio Alves Lara, and Bruno Siqueira Mietto

Subjects

Host-pathogen interaction, Leprosy neuropathy, Mycobacterium leprae, Peripheral nervous system, Schwann cell, Systematic review, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Mycobacterium leprae, the pathogen that causes human leprosy, has a unique affinity for infecting and persisting inside Schwann cells, the principal glia of the peripheral nervous system. Several studies have focused on this intricate host-pathogen interaction as an attempt to advance the current knowledge of the mechanisms governing nerve destruction and disease progression. However, during the chronic course of leprosy neuropathy, Schwann cells can respond to and internalize both live and dead M. leprae and bacilli-derived antigens, and this may result in divergent cellular pathobiological responses. This may also distinctly contribute to tissue degeneration, failure to repair, inflammatory reactions, and nerve fibrosis, hallmarks of the disease. Therefore, the present study systematically searched for published studies on M. leprae-Schwann cell interaction in vitro to summarize the findings and provide a focused discussion of Schwann cell dynamics following challenge with leprosy bacilli.

Published

2023

44. Senescent Schwann cells induced by aging and chronic denervation impair axonal regeneration following peripheral nerve injury

Author

Andrés Fuentes‐Flores, Cristian Geronimo‐Olvera, Karina Girardi, David Necuñir‐Ibarra, Sandip Kumar Patel, Joanna Bons, Megan C Wright, Daniel Geschwind, Ahmet Hoke, Jose A Gomez‐Sanchez, Birgit Schilling, Daniela L Rebolledo, Judith Campisi, and Felipe A Court

Subjects

aging, chronic denervation, nerve regeneration, Schwann cell, senescence, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Following peripheral nerve injury, successful axonal growth and functional recovery require Schwann cell (SC) reprogramming into a reparative phenotype, a process dependent upon c‐Jun transcription factor activation. Unfortunately, axonal regeneration is greatly impaired in aged organisms and following chronic denervation, which can lead to poor clinical outcomes. While diminished c‐Jun expression in SCs has been associated with regenerative failure, it is unclear whether the inability to maintain a repair state is associated with the transition into an axonal growth inhibition phenotype. We here find that reparative SCs transition into a senescent phenotype, characterized by diminished c‐Jun expression and secretion of inhibitory factors for axonal regeneration in aging and chronic denervation. In both conditions, the elimination of senescent SCs by systemic senolytic drug treatment or genetic targeting improved nerve regeneration and functional recovery, increased c‐Jun expression and decreased nerve inflammation. This work provides the first characterization of senescent SCs and their influence on axonal regeneration in aging and chronic denervation, opening new avenues for enhancing regeneration and functional recovery after peripheral nerve injuries.

Published

2023

45. Ferroptosis involves in Schwann cell death in diabetic peripheral neuropathy

Author

Wu Kai-yan, Deng Fei, Mao Xin-yu, Zhou Dan, and Shen Wei-gan

Subjects

ferroptosis, diabetic peripheral neuropathy, schwann cell, nrf2 signaling pathway, Medicine

Abstract

Accumulating evidence shows that Schwann cells’ (SCs) death caused by high glucose (HG) is involved in the pathological process of diabetic peripheral neuropathy (DPN). Ferroptosis is a novel form of regulatory cell death driven by iron-dependent lipid peroxidation. However, it is not clear whether ferroptosis is involved in the death process of SCs induced by HG. The expression of ferroptosis-related indicators in the serum of DPN patients was detected by ELISA. Subsequently, using cell counting kit‑8, western blot, real-time PCR, and Ki-67 staining, we investigated the effects of HG on the ferroptosis of SCs and initially explored the underlying mechanism. The results showed that the serum levels of glutathione peroxidase 4 (GPX4) and glutathione in patients with DPN decreased, while malondialdehyde levels increased significantly. Then, we observed that erastin and HG induced ferroptosis in SCs, resulting in the decrease in cell activity and the expression level of GPX4 and SLC7A11, which could be effectively reversed by the ferroptosis inhibitor Fer-1. Mechanistically, HG induced ferroptosis in SCs by inhibiting the NRF2 signaling pathway. Our results showed that ferroptosis was involved in the death process of SCs induced by HG. Inhibition of ferroptosis in SCs might create a new avenue for the treatment of DPN.

Published

2023

46. Nuclear Magnetic Resonance Treatment Induces ßNGF Release from Schwann Cells and Enhances the Neurite Growth of Dorsal Root Ganglion Neurons In Vitro

Author

Anda Rad, Lukas Weigl, Bibiane Steinecker-Frohnwieser, Sarah Stadlmayr, Flavia Millesi, Maximilian Haertinger, Anton Borger, Paul Supper, Lorenz Semmler, Sonja Wolf, Aida Naghilou, Tamara Weiss, Hans G. Kress, and Christine Radtke

Subjects

peripheral nerve regeneration, low nuclear magnetic resonance therapy, Schwann cell, DRG neuron, cytokines, neurite outgrowth, Cytology, QH573-671

Abstract

Peripheral nerve regeneration depends on close interaction between neurons and Schwann cells (SCs). After nerve injury, SCs produce growth factors and cytokines that are crucial for axon re-growth. Previous studies revealed the supernatant of SCs exposed to nuclear magnetic resonance therapy (NMRT) treatment to increase survival and neurite formation of rat dorsal root ganglion (DRG) neurons in vitro. The aim of this study was to identify factors involved in transferring the observed NMRT-induced effects to SCs and consequently to DRG neurons. Conditioned media of NMRT-treated (CM NMRT) and untreated SCs (CM CTRL) were tested by beta-nerve growth factor (ßNGF) ELISA and multiplex cytokine panels to profile secreted factors. The expression of nociceptive transient receptor potential vanilloid 1 (TRPV1) channels was assessed and the intracellular calcium response in DRG neurons to high-potassium solution, capsaicin or adenosine triphosphate was measured mimicking noxious stimuli. NMRT induced the secretion of ßNGF and pro-regenerative-signaling factors. Blocking antibody experiments confirmed ßNGF as the main factor responsible for neurotrophic/neuritogenic effects of CM NMRT. The TRPV1 expression or sensitivity to specific stimuli was not altered, whereas the viability of cultured DRG neurons was increased. Positive effects of CM NMRT supernatant on DRG neurons are primarily mediated by increased ßNGF levels.

Published

2024

47. Regeneration of Propriospinal Axons in Rat Transected Spinal Cord Injury through a Growth-Promoting Pathway Constructed by Schwann Cells Overexpressing GDNF

Author

Xiaolong Du, Shengqi Zhang, Aytak Khabbaz, Kristen Lynn Cohen, Yihong Zhang, Samhita Chakraborty, George M. Smith, Hongxing Wang, Amol P. Yadav, Naikui Liu, and Lingxiao Deng

Subjects

descending propriospinal axon, spinal transection, Schwann cell, glial-cell-derived neurotrophic factor, transplantation, regeneration, Cytology, QH573-671

Abstract

Unsuccessful axonal regeneration in transected spinal cord injury (SCI) is mainly attributed to shortage of growth factors, inhibitory glial scar, and low intrinsic regenerating capacity of severely injured neurons. Previously, we constructed an axonal growth permissive pathway in a thoracic hemisected injury by transplantation of Schwann cells overexpressing glial-cell-derived neurotrophic factor (SCs-GDNF) into the lesion gap as well as the caudal cord and proved that this novel permissive bridge promoted the regeneration of descending propriospinal tract (dPST) axons across and beyond the lesion. In the current study, we subjected rats to complete thoracic (T11) spinal cord transections and examined whether these combinatorial treatments can support dPST axons’ regeneration beyond the transected injury. The results indicated that GDNF significantly improved graft–host interface by promoting integration between SCs and astrocytes, especially the migration of reactive astrocyte into SCs-GDNF territory. The glial response in the caudal graft area has been significantly attenuated. The astrocytes inside the grafted area were morphologically characterized by elongated and slim process and bipolar orientation accompanied by dramatically reduced expression of glial fibrillary acidic protein. Tremendous dPST axons have been found to regenerate across the lesion and back to the caudal spinal cord which were otherwise difficult to see in control groups. The caudal synaptic connections were formed, and regenerated axons were remyelinated. The hindlimb locomotor function has been improved.

Published

2024

48. Nervous System Interactions with Nonimmune Elements in Cancer Microenvironment: A Missing Piece?

Author

Çifcibaşı, Kaan, Mota Reyes, Carmen, Istvanffy, Rouzanna, Demir, Ihsan Ekin, Amit, Moran, editor, and Scheff, Nicole N., editor

Published

2023

49. The Fundamentals of Schwann Cell Biology

Author

Abd Razak, Nurul Husna, Zainey, Amiza Shahira, Idris, Jalilah, Daud, Muhammad Fauzi, Ismail, Azman, editor, Nur Zulkipli, Fatin, editor, Jaafar, Jimisiah, editor, and Öchsner, Andreas, editor

Published

2023

50. Combination of Engineered Expression of Polysialic Acid on Transplanted Schwann Cells and in Injured Rat Spinal Cord Promotes Significant Axonal Growth and Functional Recovery

Author

Fangyou Gao, Yi Zhang, Dongsheng Wu, Juan Luo, Svetlana Gushchina, and Xuenong Bo

Subjects

spinal cord injury, polysialic acid, Schwann cell, transplantation, corticospinal axon, axonal regeneration, Neurology. Diseases of the nervous system, RC346-429

Abstract

Providing cellular support and modifying the glial scar around the lesion are two key strategies for promoting axonal regeneration after spinal cord injury. We showed previously that over-expressing polysialic acid (PSA) on Schwann cells (SCs) by lentiviral vector (LV)-mediated expression of polysialyltransferase (PST) facilitated their integration and migration in the injured spinal cord. We also showed that PSA over-expression in the injured spinal cord modified the glial scar and promoted the growth of ascending sensory axons. In this study, we combined the PST/SC transplantation with LV/PST injection in spinal cords after dorsal column transection and found the combined treatments led to faster and more profound locomotor functional recovery compared with animals receiving combined GFP/SC transplantation with LV/GFP injection. Histological examination showed significantly more injured corticospinal axons growing close to the lesion/transplant borders and into the caudal spinal cord in the PST group than in the GFP group. We also found over -expressing PSA around the lesion site did not cause allodynia and hyperalgesia in our injury model. These results demonstrate the promising therapeutic benefit of over-expressing PSA in transplanted SCs and spinal cord in promoting axonal growth and restoring motor function.

Published

2023