Your search keyword '"trigeminal ganglion"' showing total 7,597 results

1. Ageing‐Related Macrophage Polarisation in the Trigeminal Ganglion Enhances Incisional Intraoral Pain.

Author

Urata, Kentaro, Oto, Tatsuki, Hayashi, Yoshinori, Hitomi, Suzuro, Ikeda, Takayuki, Iwata, Koichi, Iinuma, Toshimitsu, and Shinoda, Masamichi

Subjects

*MACROPHAGES, *MUCOUS membranes, *GANGLIA, *REFLEXES, *IMMUNOGLOBULINS, *OROFACIAL pain

Abstract

ABSTRACT Objective Materials and Methods Results Conclusions Although macrophage polarisation in the trigeminal ganglion (TG) is crucial in orofacial pain hypersensitivity, the effect of ageing‐related changes and their involvement in intra‐oral nociception remains unclear. We assessed the effect of ageing‐related macrophage polarisation in TG on intra‐oral mechanical pain hypersensitivity following palatal mucosal incision using senescence‐accelerated mice (SAM)‐prone8 (SAMP8) and SAM‐resistant 1 (SAMR1).Mechanical head‐withdrawal reflex threshold (MHWRT) of the palatal mucosa was measured for 21 days after palatal mucosal incision. On days 3 and 14, the abundance of Iba‐1‐immunoreactive (IR) cells, CD11c‐IR cells (pro‐inflammatory macrophages (M1)), C‐C motif chemokine ligand 2 (CCL2)‐IR M1‐macrophages, CD206‐IR cells (anti‐inflammatory macrophages (M2)) and transforming growth factor‐β (TGF‐β)‐IR M2‐macrophages in the TG was analysed. The effect of continuous intra‐TG administration of CCL2‐neutralising antibody or recombinant‐CCL2 on MHWRT was examined.Incision‐induced decrease in MHWRT was enhanced in SAMP8 compared with that in SAMR1. On days 3 and 14, the number of CCL2‐IR M1‐macrophages in TG was increased in SAMP8 compared with that in SAMR1. CCL2‐neutralising antibody suppressed, whereas recombinant‐CCL2 increased pain hypersensitivity in SAMP8.Mechanical pain hypersensitivity after oral mucosal injury is potentiated and sustained by age‐related enhancement of CCL2 signalling via M1‐macrophage hyperactivation in TG. [ABSTRACT FROM AUTHOR]

Published

2024

2. The Trigeminal Sensory System and Orofacial Pain.

Author

Kim, Hyung Kyu, Chung, Ki-myung, Xing, Juping, Kim, Hee Young, and Youn, Dong-ho

Subjects

*BURNING mouth syndrome, *OROFACIAL pain, *TRIGEMINAL neuralgia, *TRIGEMINAL nerve, *NEURAL transmission

Abstract

The trigeminal sensory system consists of the trigeminal nerve, the trigeminal ganglion, and the trigeminal sensory nuclei (the mesencephalic nucleus, the principal nucleus, the spinal trigeminal nucleus, and several smaller nuclei). Various sensory signals carried by the trigeminal nerve from the orofacial area travel into the trigeminal sensory system, where they are processed into integrated sensory information that is relayed to higher sensory brain areas. Thus, knowledge of the trigeminal sensory system is essential for comprehending orofacial pain. This review elucidates the individual nuclei that comprise the trigeminal sensory system and their synaptic transmission. Additionally, it discusses four types of orofacial pain and their relationship to the system. Consequently, this review aims to enhance the understanding of the mechanisms underlying orofacial pain. [ABSTRACT FROM AUTHOR]

Published

2024

3. Gender-different effect of Src family kinases antagonism on photophobia and trigeminal ganglion activity.

Author

Huang, Zhuoan, Yao, Junyu, Nie, Lingdi, Nie, Xinchen, Xiong, Xuechunhui, Kõks, Sulev, Quinn, John P., Kanhere, Aditi, and Wang, Minyan

Subjects

*VISION disorders, *RESEARCH funding, *ENZYME-linked immunosorbent assay, *POLYMERASE chain reaction, *HYPOTHALAMUS, *MICE, *RNA, *SENSORY ganglia, *GENE expression profiling, *ANIMAL experimentation, *NEUROPEPTIDES, *TRANSFERASES, *MIGRAINE, *SEQUENCE analysis

Abstract

Background: Src family kinases (SFKs) contribute to migraine pathogenesis, yet its role in regulating photophobia behaviour, one of the most common forms of migraine, remains unknown. Here, we addressed whether SFKs antagonism alleviates photophobia behavior and explored the underlying mechanism involving hypothalamus and trigeminal ganglion activity, as measured by the alteration of neuropeptide levels and transcriptome respectively. Methods: A rapid-onset and injury-free mouse model of photophobia was developed following intranasal injection of the TRPA1 activator, umbellulone. The role of SFKs antagonism on light aversion was assessed by the total time the mouse stays in the light and transition times between the dark and light compartments. To gain insight to the preventive mechanism of SFKs antagonism, hypothalamic neuropeptides levels were assessed using enzyme linked immunofluorescent assay and trigeminal ganglion activity were assessed using RNA-sequencing and qPCR analysis. Results: SFKs antagonism by a clinically relevant SFKs inhibitor saracatinib reduced the total time in light and transition times in male mice, but not in females, suggesting SFKs play a crucial role in photophobia progressing and exhibit a male-only effect. SFKs antagonism had no effect on hypothalamic calcitonin gene-related peptide and pituitary adenylate cyclase-activating polypeptide levels of all mice investigated, suggesting the gender-different effect of saracatinib on light aversion appears to be independent of these hypothalamic neuropeptide levels. In trigeminal ganglion of male mice, photophobia is associated with profound alteration of differentially expressed genes, part of which were reversed by SFKs antagonism. Subsequent qPCR analysis showed SFKs antagonism displayed gender-different modulation of expression in some candidate genes, particularly noteworthy those encoding ion channels (trpm3, Scn8a), ATPase signaling (crebbp, Atp5α1) and kinase receptors (Zmynd8, Akt1). Conclusions: In conclusion, our data revealed that SFKs antagonism reduced photophobia processing in male mice and exhibited gender-different modulation of trigeminal ganglion activity, primarily manifesting as alterations in the transcriptome profile. These findings underscore the potential of SFKs antagonism for allieving photophobia in males, highlighting its value in the emerging field of precision medicine. [ABSTRACT FROM AUTHOR]

Published

2024

4. Neuroimmune interactions in the development and chronification of migraine headache.

Author

Zhang, Jintao, Simoes, Roli, Guo, Tingting, and Cao, Yu-Qing

Subjects

*REGULATORY T cells, *IMMUNOCOMPETENT cells, *MIGRAINE, *GENOME-wide association studies, *NEUROGLIA

Abstract

Large-scale genome-wide association analyses have identified loci of migraine risk that encode inflammation-related genes. Other lines of evidence in humans have further implicated immune dysregulation in migraine, including measurements of peripheral proinflammatory factors and neuroimaging studies. Studies in rodents point to immune dysregulation along the trigeminovascular pathway as a major contributor to migraine's pathophysiology. Reciprocal modulation between the immune cells and the meningeal afferent neurons regulates peripheral and central sensitization, leading to persistent headache and its chronification. Microglia–neuron interactions in the trigeminocervical complex may play an important role in the transition from episodic to chronic migraine. Emerging evidence suggests that regulatory T cells participate in the resolution of migraine headaches. Targeting regulatory T cells may restore the balance between immune activation and suppression to reverse chronic headaches. Migraine is highly prevalent and debilitating. The persistent headaches in this condition are thought to arise from the activation and sensitization of the trigeminovascular pathway. Both clinical and animal model studies have suggested that neuroimmune interactions contribute to the pathophysiology of migraine headache. In this review, we first summarize the findings from human studies implicating the dysregulation of the immune system in migraine, including genetic analyses, measurement of circulatory factors, and neuroimaging data. We next discuss recent advances from rodent studies aimed at elucidating the neuroimmune interactions that manifest at various levels of the trigeminovascular pathway and lead to the recruitment of innate and adaptive immune cells as well as immunocompetent glial cells. These cells reciprocally modulate neuronal activity via multiple pro- and anti-inflammatory mediators, thereby regulating peripheral and central sensitization. Throughout the discussions, we highlight the potential clinical and translational implications of the findings. [ABSTRACT FROM AUTHOR]

Published

2024

5. Changes of Trigeminal Ganglion Neurons Innervating the Temporomandibular Joint in Chronic Pain Rat Model.

Author

Liu, Wen, Jiang, Henghua, Ke, Jin, Liu, Xin, Feng, Yaping, Hou, Jinsong, Long, Xing, and Kao, Chia Tze

Subjects

LABORATORY rats, JOINT pain, TEMPOROMANDIBULAR joint, PHENOTYPIC plasticity, INTRACELLULAR calcium, TEMPOROMANDIBULAR disorders

Abstract

Background: Phenotype alterations of nociceptive neurons have been shown to be a key step in the pathogenesis of many pain‐related diseases. However, it is unclear if the characteristic changes of temporomandibular joint (TMJ) primary afferent neurons are related to the pathogenesis of temporomandibular joint osteoarthritis (TMJOA) chronic pain. This study aimed to determine the morphological and neurochemical changes in trigeminal ganglion (TG) neurons innervating the TMJ in TMJOA chronic pain rats. Materials and Methods: Monosodium iodoacetate (MIA)‐induced TMJOA chronic pain rat model was established (n = 6), and saline was injected in rats of the control group (n = 6). TMJ primary afferent neurons were labeled with retrograde tracing (Dil). The spatial distribution and the expression of calcitonin gene‐related peptide (CGRP), isolectin B4 (IB4), and neurofilament 200 (NF200) of TMJ primary afferent neurons in TG were investigated using immunofluorescence. Intracellular calcium signaling was recorded by calcium imaging (n = 20). Results: TMJ primary afferent neurons were located only in the V3 region of the TG from both saline‐ and MIA‐injected rats. The number of TG neurons innervating the TMJ was increased in MIA‐injected rats. Elevated number and intracellular calcium concentration of small‐ and medium‐sized instead of large‐sized Dil+ TG neurons were found in MIA‐injected rats. The upregulated expression of CGRP and IB4, but not NF200, in TG neurons innervating the rat TMJs was accompanied by TMJOA chronic pain. Conclusion: This study suggests that sensitization of small‐ to medium‐sized Dil+ TG neurons and CGRP‐ and IB4‐positive Dil+ TG neurons might contribute to the development of TMJOA chronic pain in rats. This will provide valuable information for more efficient control of TMJOA chronic pain. [ABSTRACT FROM AUTHOR]

Published

2024

6. A Quadruple Gene-Deleted Live BoHV-1 Subunit RVFV Vaccine Vector Reactivates from Latency and Replicates in the TG Neurons of Calves but Is Not Transported to and Shed from Nasal Mucosa.

Author

Pavulraj, Selvaraj, Stout, Rhett W., Paulsen, Daniel B., and Chowdhury, Shafiqul I.

Subjects

*RIFT Valley fever, *ANIMAL herds, *VIRAL shedding, *VACCINE effectiveness, *NERVE endings

Abstract

Bovine herpesvirus type 1 (BoHV-1) establishes lifelong latency in trigeminal ganglionic (TG) neurons following intranasal and ocular infection in cattle. Periodically, the latent virus reactivates in the TG due to stress and is transported anterogradely to nerve endings in the nasal epithelium, where the virus replicates and sheds. Consequently, BoHV-1 is transmitted to susceptible animals and maintained in the cattle population. Modified live BoHV-1 vaccine strains (BoHV-1 MLV) also have a similar latency reactivation. Therefore, they circulate and are maintained in cattle herds. Additionally, they can regain virulence and cause vaccine outbreaks because they mutate and recombine with other circulating field wild-type (wt) strains. Recently, we constructed a BoHV-1 quadruple mutant virus (BoHV-1qmv) that lacks immune evasive properties due to UL49.5 and glycoprotein G (gG) deletions. In addition, it also lacks the gE cytoplasmic tail (gE CT) and Us9 gene sequences designed to make it safe, increase its vaccine efficacy against BoHV-1, and restrict its anterograde neuronal transport noted above. Further, we engineered the BoHV-1qmv-vector to serve as a subunit vaccine against the Rift Valley fever virus (BoHV-1qmv Sub-RVFV) (doi: 10.3390/v15112183). In this study, we determined the latency reactivation and nasal virus shedding properties of BoHV-1qmv (vector) and BoHV-1qmv-vectored subunit RVFV (BoHV-1qmv sub-RVFV) vaccine virus in calves in comparison to the BoHV-1 wild-type (wt) following intranasal inoculation. The real-time PCR results showed that BoHV-1 wt- but not the BoHV-1qmv vector- and BoHV-1qmv Sub-RVFV-inoculated calves shed virus in the nose following dexamethasone-induced latency reactivation; however, like the BoHV-1 wt, both the BoHV-1qmv vector and BoHV-1qmv Sub-RVFV viruses established latency, were reactivated, and replicated in the TG neurons. These results are consistent with the anterograde neurotransport function of the gE CT and Us9 sequences, which are deleted in the BoHV-1qmv and BoHV-1qmv Sub-RVFV. [ABSTRACT FROM AUTHOR]

Published

2024

7. Non-neuronal cells act as crucial players in neuropathic orofacial pain.

Author

Iwata, Koichi, Hayashi, Yoshinori, Hitomi, Suzuro, Tsuboi, Yoshiyuki, and Shinoda, Masamichi

Abstract

Following peripheral nerve damage, various non-neuronal cells are activated, triggering accumulation in the peripheral and central nervous systems, and communicate with neurons. Evidence suggest that neuronal and non-neuronal cell communication is a critical mechanism of neuropathic pain; however, its detailed mechanisms in contributing to neuropathic orofacial pain development remain unclear. Neuronal and non-neuronal cell communication in the trigeminal ganglion (TG) is believed to cause neuronal hyperactivation following trigeminal nerve damage, resulting in neuropathic orofacial pain. Trigeminal nerve damage activates and accumulates non-neuronal cells, such as satellite cells and macrophages in the TG and microglia, astrocytes, and oligodendrocytes in the trigeminal spinal subnucleus caudalis (Vc) and upper cervical spinal cord (C1–C2). These non-neuronal cells release various molecules, contributing to the hyperactivation of TG, Vc, and C1–C2 nociceptive neurons. These hyperactive nociceptive neurons release molecules that enhance non-neuronal cell activation. This neuron and non-neuronal cell crosstalk causes hyperactivation of nociceptive neurons in the TG, Vc, and C1–C2. Here, we addressed previous and recent data on the contribution of neuronal and non-neuronal cell communication and its involvement in neuropathic orofacial pain development. Previous and recent data suggest that neuronal and non-neuronal cell communication in the TG, Vc, and C1–C2 is a key mechanism that causes neuropathic orofacial pain associated with trigeminal nerve damage. [ABSTRACT FROM AUTHOR]

Published

2024

8. Cytoarchitecture and intercellular interactions in the trigeminal ganglion: Associations with neuropathic pain in the orofacial region.

Author

Goto, Tetsuya, Kuramoto, Eriko, Iwai, Haruki, and Yamanaka, Atsushi

Abstract

Disorders of the trigeminal nerve, a sensory nerve of the orofacial region, often lead to complications in dental practice, including neuropathic pain, allodynia, and ectopic pain. Management of these complications requires an understanding of the cytoarchitecture of the trigeminal ganglion, where the cell bodies of the trigeminal nerve are located, and the mechanisms of cell-cell interactions. In the trigeminal ganglion, ganglion, satellite, Schwann, and immune cells coexist and interact. Cell-cell interactions are complex and occur through direct contact via gap junctions or through mediators such as adenosine triphosphate, nitric oxide, peptides, and cytokines. Interactions between the nervous and immune systems within the trigeminal ganglion may have neuroprotective effects during nerve injury or may exacerbate inflammation and produce chronic pain. Under pathological conditions of the trigeminal nerve, cell-cell interactions can cause allodynia and ectopic pain. Although cell-cell interactions that occur via mediators can act at some distance, they are more effective when the cells are close together. Therefore, information on the three-dimensional topography of trigeminal ganglion cells is essential for understanding the pathophysiology of ectopic pain. A three-dimensional map of the somatotopic localization of trigeminal ganglion neurons revealed that ganglion cells innervating distant orofacial regions are often apposed to each other, interacting with and potentially contributing to ectopic pain. Elucidation of the complex network of mediators and their receptors responsible for intercellular communication within the trigeminal ganglion is essential for understanding ectopic pain. • The trigeminal ganglion contains nervous system cells and immune system cells. • Cells in the trigeminal ganglion interact via gap junctions and mediators. • 3D topography of trigeminal ganglion is essential for clarifying ectopic pain. • The neuro-immune axis may have neuroinflammatory or neuroprotective effects. • Control of the neuro-immune axis leads to the solution of ectopic pain. [ABSTRACT FROM AUTHOR]

Published

2024

9. Sex differences in expression of CGRP family of receptors and ligands in the rat trigeminal system

Author

Aida Maddahi, Jacob C. A. Edvinsson, and Lars Edvinsson

Subjects

Trigeminal ganglion, CGRP, Adrenomedullin, Amylin, Calcitonin, Receptors, Medicine

Abstract

Abstract Background Calcitonin gene-related peptide (CGRP) is part of the calcitonin peptide family, which includes calcitonin (CT), amylin (AMY), and adrenomedullin (ADM). CGRP and its receptor are highly present in the trigeminovascular system (TVS). Recent research suggests that other members of the calcitonin family could be feasible therapeutic targets in the treatment of migraine. The present study aims to elucidate the distribution of ADM, AMY, CT, and their receptors in the rat TVS, and to explore potential sex differences in their expression. Methods Trigeminal ganglia (TG) were dissected from male and female adult rats. Protein and gene expression were assessed through immunohistochemistry and RT-qPCR. Additionally, the dura mater was isolated for further investigation of protein expression and fiber localization using immunohistochemistry. Results Quantitative gene expression analysis revealed the presence of all genes in male and female TGs, except for calcitonin receptor (CTR). Notably, CGRP mRNA levels in TG were several folds higher than those of other genes. The receptor activity-modifying protein-1 (RAMP1) mRNA levels were significantly higher in female compared to male. No AMY or CT immunoreactivity was observed in the TVS. In contrast, immunoreactivity for ADM, CGRP, RAMP1, CTR, and calcitonin-like receptor (CLR) were observed in the cytoplasm of TG neurons. Immunoreactive Aδ-fibers storing RAMP1, ADM and CLR were also identified. RAMP2 and RAMP3 were expressed in nucleus of TG neurons and in satellite glial cells. Furthermore, RAMP1 and CLR were co-localized with CASPR in the nodes of Ranvier located in Aδ-fibers. Conclusions This study provides valuable insights into the distribution of the CGRP family of peptides and their receptors in the TVS. CGRP mRNA levels in the TG were markedly higher than those of other genes, demonstrating the key role of CGRP. The co-localization of CLR and RAMP1 on Aδ-fibers with CASPR suggests a potential role for this receptor in modulating trigeminal nerve function and neuronal excitability, with implications for migraine pathophysiology. Additionally, RAMP1 mRNA levels were significantly higher in female TG compared to males, indicating sex-specific differences in gene expression. These findings underscore the need for further research into the functional significance of gender-related variations.

Published

2024

10. Gender-different effect of Src family kinases antagonism on photophobia and trigeminal ganglion activity

Author

Zhuoan Huang, Junyu Yao, Lingdi Nie, Xinchen Nie, Xuechunhui Xiong, Sulev Kõks, John P. Quinn, Aditi Kanhere, and Minyan Wang

Subjects

Src family kinases, Transient receptor potential ankyrin 1, Light aversion, Migraine, Trigeminal ganglion, Gender, Medicine

Abstract

Abstract Background Src family kinases (SFKs) contribute to migraine pathogenesis, yet its role in regulating photophobia behaviour, one of the most common forms of migraine, remains unknown. Here, we addressed whether SFKs antagonism alleviates photophobia behavior and explored the underlying mechanism involving hypothalamus and trigeminal ganglion activity, as measured by the alteration of neuropeptide levels and transcriptome respectively. Methods A rapid-onset and injury-free mouse model of photophobia was developed following intranasal injection of the TRPA1 activator, umbellulone. The role of SFKs antagonism on light aversion was assessed by the total time the mouse stays in the light and transition times between the dark and light compartments. To gain insight to the preventive mechanism of SFKs antagonism, hypothalamic neuropeptides levels were assessed using enzyme linked immunofluorescent assay and trigeminal ganglion activity were assessed using RNA-sequencing and qPCR analysis. Results SFKs antagonism by a clinically relevant SFKs inhibitor saracatinib reduced the total time in light and transition times in male mice, but not in females, suggesting SFKs play a crucial role in photophobia progressing and exhibit a male-only effect. SFKs antagonism had no effect on hypothalamic calcitonin gene-related peptide and pituitary adenylate cyclase-activating polypeptide levels of all mice investigated, suggesting the gender-different effect of saracatinib on light aversion appears to be independent of these hypothalamic neuropeptide levels. In trigeminal ganglion of male mice, photophobia is associated with profound alteration of differentially expressed genes, part of which were reversed by SFKs antagonism. Subsequent qPCR analysis showed SFKs antagonism displayed gender-different modulation of expression in some candidate genes, particularly noteworthy those encoding ion channels (trpm3, Scn8a), ATPase signaling (crebbp, Atp5α1) and kinase receptors (Zmynd8, Akt1). Conclusions In conclusion, our data revealed that SFKs antagonism reduced photophobia processing in male mice and exhibited gender-different modulation of trigeminal ganglion activity, primarily manifesting as alterations in the transcriptome profile. These findings underscore the potential of SFKs antagonism for allieving photophobia in males, highlighting its value in the emerging field of precision medicine.

Published

2024

11. Morphometric and morphological characteristics of the trigeminal ganglion of rats in an experimental model of aseptic inflammation and introduced cryopreserved placenta

Author

O.D. Danyliv, V.I. Shepitko, Ye.V. Stetsuk, and N.V. Boruta

Subjects

trigeminal ganglion, inflammation, cryopreserved placenta, biologically active substances, macrophages, lymphocytes, mast cells, rats, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Background. Diseases of the peripheral nervous system account for more than 50 % of all outpatient neurological pathology, and since inflammatory diseases are one of the main problems of medicine, it is important now to develop new methods of anti-inflammatory therapy based on the action of biologically active substances contained in natural products, as well as in many mammalian tissues, particularly in the placental tissue, which is an endocrine gland during pregnancy. Therefore, the issue of using cryopreserved placenta preparations is of great practical importance in the treatment of inflammatory processes and requires further research. The purpose of the work was to investigate the morphometric and morphological features of the trigeminal ganglion of rats in the experimental model of aseptic inflammation and the introduction of cryopreserved placenta. Materials and methods. The work was carried out on 50 sexually mature male rats. The control group consisted of 5 animals who received a single injection of physiological saline solution. Using standard research methods, paraffin blocks were made from which a series of semi-thin sections were cut and stained with hematoxylin and eosin. Histological sections were studied in a light Biorex 3 microscope with a digi­tal camera using software adapted for research. Statistical data processing was performed using Microsoft Office Excel. Results. The morphometric study of rats from the control group revealed that the cytoplasm volume of the bodies of the trigeminal ganglion neurons was 3489.89 ± 37.59 μm3, the volume of the nucleus was 247.68 ± 4.30 μm3. In the experimental model of inflammation and introduction of cryopreserved placenta, destructive phenomena are observed until the seventh day, with marked swelling of the stroma, disruption in the structure of neurons with signs of cytoplasmic swelling, which is confirmed by the data of a morphometric study, namely a reliable increase in the cytoplasm volume by 30.78 % compared to the control group of animals (p

Published

2024

12. Aging is associated with sex-specific alteration in the expression of genes encoding for neuroestradiol synthesis and signaling proteins in the mouse trigeminal somatosensory input.

Author

Bautista-Abad, Álvaro, García-Magro, Nuria, Pinto-Benito, Daniel, Cáceres-Pajuelo, Julio Eduardo, Alises, Carlos Vicente, Ganchala, Danny, Lagunas, Natalia, Negredo, Pilar, García-Segura, Luis Miguel, Arevalo, Maria-Angeles, and Grassi, Daniela

Subjects

ANDROGEN receptors, ESTROGEN receptors, SENSORY ganglia, DORSAL root ganglia, AGE differences, PAIN perception

Abstract

Pain perception is influenced by sex and aging, with previous studies indicating the involvement of aromatase, the estradiol synthase enzyme, in regulating pain perception. Previous research has established the presence of aromatase in dorsal root ganglia sensory neurons and its role in modulating pain perception. The present study aims to explore the implications of aging and sex on the expression of aromatase and estrogen receptors in the trigeminal ganglion. The study examined mRNA levels of aromatase, ERs, and the androgen receptor (AR) in the trigeminal ganglion of 3-month-old and 27-month-old male and female mice, as well as 3-month-old mice from the four-core genotype (FCG) transgenic model. The latter facilitates the assessment of gonadal hormone and sex chromosome implications for sex-specific traits. Aromatase localization in the ganglion was further assessed through immunohistochemistry. Aromatase immunoreactivity was observed for the first time in sensory neurons within the trigeminal ganglion. Trigeminal ganglion gene expressions were detected for aromatase, ERs, and AR in both sexes. Aromatase, ERβ, and GPER gene expressions were higher in young males versus young females. Analyses of the FCG model indicated that sex differences depended solely on gonadal sex. The aging process induced an enhancement in the expression of aromatase, ERs, and AR genes across both sexes, culminating in a reversal of the previously observed gender-based differences. the potential impact of estrogen synthesis and signaling in the trigeminal ganglion on age and sex differences warrants consideration, particularly in relation to trigeminal sensory functions and pain perception. Age and gonadal sex influence ERs, AR, and ARO levels in the trigeminal ganglion. Although somatosensory perception shows a decline in the elderly, the incidence of trigeminal neuralgia intensifies in aged adults and is predominantly prevalent in women relative to men. The increased expression of aromatase and estrogen receptors in aged female animals suggests that the modulatory influence that neuroestradiol exerts over the trigeminal somatosensory input, inclusive of pain, undergoes changes in elderly male and female individuals in a sex-specific manner. [ABSTRACT FROM AUTHOR]

Published

2024

13. The extracapsular capsule phenomenon of percutaneous balloon compression provides adequate compression of the third branch of the trigeminal nerve: a retrospective study.

Author

Fu, Lijun, Liu, Zuying, Bu, Huilian, Lu, Zhongyuan, Kong, Cunlong, Wang, Tao, Ma, Letian, Wen, Yuanyuan, Liu, Qingying, Wang, Zhongyu, Wang, Jian, and Fan, Xiaochong

Subjects

*TRIGEMINAL neuralgia, *MANDIBULAR nerve, *TRIGEMINAL nerve, *POSTOPERATIVE period, *NEURALGIA

Abstract

Background: Percutaneous balloon compression (PBC) is an effective, low-cost, and simple treatment for primary trigeminal neuralgia (TN). However, PBC has poor efficacy and no better solution for the third branch (V3) of TN. Methods: Clinical data of 52 patients with trigeminal neuralgia treated with PBC were retrospectively analyzed. Postoperative numbness of the patient was evaluated by facial numbness at the Barrow Neurological Institute (BNI-N). The main observation was the incidence of higher numbness in the V3 than in the other two branches or equally strong numbness in the three branches in the immediate postoperative period. Results: The efficacy values in the pear-shaped balloon group at the first postoperative day (T1), the first month (T2), in the third month (T3), and the sixth month (T4) were 96.7%, 93.3%, 93.3%, and 90%, respectively, and 1 patient (3.3%) had recurrence. The efficacy value for the extracapsular capsule group was 95.5% at all times and there were no patients with recurrence within 6 months after surgery. In the immediate postoperative period, the effective compression rate of V3 in the pear-shaped balloon group was 43.3%, and 86.4% in the extracapsular capsule group (P = 0.020). At six months of follow-up, the effective compression rate of V3 was higher in the extracapsular capsule group than in the pear-shaped balloon group. Conclusions: The riveted structure of the extracapsular capsule can effectively compress V3, thus performing PBC with a balloon shaped as an extracapsular capsule is a new, effective, and safe treatment option for TN V3. Trial registration: ClinicalTrials.gov ChiCTR2300067313. [ABSTRACT FROM AUTHOR]

Published

2024

14. Analysis of factors selectively related to herpes zoster involving peripheral sensory ganglia: Retrospective study.

Author

Liu, Jing, Wang, Cihan, Li, Xin, Guan, Jingjing, Song, Xiaowei, Song, Yinghao, and Wang, Cunjin

Subjects

DORSAL root ganglia, SENSORY neurons, POSTHERPETIC neuralgia, SENSORY ganglia, PERCUTANEOUS coronary intervention, HERPES zoster

Abstract

Herpes zoster (HZ), resulting from the reactivation of the varicella‐zoster virus, is a significant disease. This study aimed to explore the factors influencing sensory neuron involvement in HZ at different locations and its association with postherpetic neuralgia (PHN). A total of 3143 cases were retrieved from an electronic medical record system, including 2676 cases of HZ and 467 cases of PHN. Gender, age, site of onset, past surgical history, and comorbidities were analyzed using a multifactorial logistic regression model. The results revealed correlations between age, gender, comorbidities (diabetes, coronary heart disease, percutaneous coronary intervention [PCI]), and sensory neuron involvement in HZ. Specifically, older age, female gender, and comorbid conditions such as diabetes/coronary heart disease were associated with sacral dorsal root ganglion (DRG) involvement, while PCI history was associated with lumbar DRG involvement. Additionally, sensory neuron involvement at different locations by HZ was linked to PHN. Furthermore, independent risk factors for PHN included thoracic DRG involvement, older age, and comorbidities (diabetes, surgical history, malignancy). It is crucial to prevent damage to the DRG, especially in individuals with comorbidities, through activities avoidance and active treatment, to minimize the occurrence of PHN. [ABSTRACT FROM AUTHOR]

Published

2024

15. Морфометричні та морфологічні особливості трійчастого вузла щурів при експериментальній моделі асептичного запалення і введенні кріоконсервованої плаценти.

Author

О. Д., Данилів, В. І., Шепітько, Є. В., Стецук, and Н. В., Борута

Subjects

PERIPHERAL neuropathy, LABORATORY rats, MAST cells, ENDOCRINE glands, SALINE injections

Abstract

Background. Diseases of the peripheral nervous system account for more than 50 % of all outpatient neurological pathology, and since inflammatory diseases are one of the main problems of medicine, it is important now to develop new methods of anti-inflammatory therapy based on the action of biologically active substances contained in natural products, as well as in many mammalian tissues, particularly in the placental tissue, which is an endocrine gland during pregnancy. Therefore, the issue of using cryopreserved placenta preparations is of great practical importance in the treatment of inflammatory processes and requires further research. The purpose of the work was to investigate the morphometric and morphological features of the trigeminal ganglion of rats in the experimental model of aseptic inflammation and the introduction of cryopreserved placenta. Materials and methods. The work was carried out on 50 sexually mature male rats. The control group consisted of 5 animals who received a single injection of physiological saline solution. Using standard research methods, paraffin blocks were made from which a series of semi-thin sections were cut and stained with hematoxylin and eosin. Histological sections were studied in a light Biorex 3 microscope with a digital camera using software adapted for research. Statistical data processing was performed using Microsoft Office Excel. Results. The morphometric study of rats from the control group revealed that the cytoplasm volume of the bodies of the trigeminal ganglion neurons was 3489.89 ± 37.59 μm3, the volume of the nucleus was 247.68 ± 4.30 μm3. In the experimental model of inflammation and introduction of cryopreserved placenta, destructive phenomena are observed until the seventh day, with marked swelling of the stroma, disruption in the structure of neurons with signs of cytoplasmic swelling, which is confirmed by the data of a morphometric study, namely a reliable increase in the cytoplasm volume by 30.78 % compared to the control group of animals (p < 0.05). After the seventh day of observation, the stimulating effect of components of the fetoplacental complex led to the acceleration of intracellular reparative processes. The change in the number of lymphoid cells had a wave-like nature, with a significant increase in the number of macrophages until the fifth day, which was 8.07 times higher than in the control group (p < 0.05) that indicated the activation of the humoral link of the immune response accelerated by the introduction of cryopreserved placenta. Conclusions. An increase in the number of mast cells was observed until the fifth day of observation, with a significant increase in their average number, which is associated with enhanced regulation of the state of the intercellular substance in response to an alterative factor. By the end of the experiment, there was a significant decrease in the average number of mast cells due to an increased regulatory effect of components of the fetoplacental complex of cryopreserved placenta. [ABSTRACT FROM AUTHOR]

Published

2024

16. Neuronavigated percutaneous gasserian radiofrequency thermorhizotomy for trigeminal neuralgia: how I do it.

Author

Rizzi, Michele, Castelli, Nicolò, Martino, Donato, and Nazzi, Vittoria

Subjects

*TRIGEMINAL neuralgia, *RADIO frequency, *TREATMENT effectiveness, *TRIGEMINAL nerve, *CATHETERIZATION

Abstract

Background: Radiofrequency thermorhizotomy (TRZ) is an established treatment for trigeminal neuralgia (TN). TRZ can result risky and painful in a consistent subset of patients, due to the need to perform multiple trajectories, before a successful foramen ovale cannulation. Moreover, intraoperative x-rays are required. Method: TRZ has been performed by using a neuronavigated stylet, before trajectory planning on a dedicated workstation. Conclusion: Navigated-TRZ (N-TRZ) meets the expectations of a safer and more tolerable procedure due to the use of a single trajectory, avoiding critical structures. Moreover, N-TRZ is x-ray free. Efficacy outcomes are similar to those reported in literature. [ABSTRACT FROM AUTHOR]

Published

2024

17. An experimental model for primary neuropathic corneal pain induced by long ciliary nerve ligation in rats.

Author

Jinhong Wu, Tianjie Yuan, Danyun Fu, Rui Xu, Wenna Zhang, Shuangshuang Li, Jiahui Ding, Lili Feng, Ying Xi, Jijiang Wang, Wenxian Li, and Yuan Han

Subjects

*NEURALGIA, *CALCITONIN gene-related peptide, *NERVE endings, *RATS, *NERVES, *CORNEAL dystrophies

Abstract

Neuropathic corneal pain (NCP) is a new and ill-defined disease characterized by pain, discomfort, aching, burning sensation, irritation, dryness, and grittiness. However, the mechanism underlying NCP remain unclear. Here, we reported a novel rat model of primary NCP induced by long ciliary nerve (LCN) ligation. After sustained LCN ligation, the rats developed increased corneal mechanical and chemical sensitivity, spontaneous blinking, and photophobia, which were ameliorated by intraperitoneal injection of morphine or gabapentin. However, neither tear reduction nor corneal injury was observed in LCN-ligated rats. Furthermore, after LCN ligation, the rats displayed a significant reduction in corneal nerve density, as well as increased tortuosity and beading nerve ending. Long ciliary nerve ligation also notably elevated corneal responsiveness under resting or menthol-stimulated conditions. At a cellular level, we observed that LCN ligation increased calcitonin gene-related peptide (neuropeptide)-positive cells in the trigeminal ganglion (TG). At a molecular level, upregulated mRNA levels of ion channels Piezo2, TRPM8, and TRPV1, as well as inflammatory factors TNF-α, IL-1 β, and IL-6, were also detected in the TG after LCN ligation. Meanwhile, consecutive oral gabapentin attenuated LCN ligation-induced corneal hyperalgesia and increased levels of ion channels and inflammation factors in TG. This study provides a reliable primary NCP model induced by LCN ligation in rats using a simple, minimally invasive surgery technique, which may help shed light on the underlying cellular and molecular bases of NCP and aid in developing a new treatment for the disease. [ABSTRACT FROM AUTHOR]

Published

2024

18. Thermosensation and TRP Channels

Author

Tominaga, Makoto, Kashio, Makiko, Crusio, Wim E., Series Editor, Dong, Haidong, Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, Steinlein, Ortrud, Series Editor, Xiao, Junjie, Series Editor, Rosenhouse-Dantsker, Avia, Editorial Board Member, Tominaga, Makoto, editor, and Takagi, Masahiro, editor

Published

2024

19. Enhancement of allyl isothiocyanate-evoked responses of mouse trigeminal ganglion cells by the kokumi substance γ-glutamyl-valyl-glycine (γ-EVG) through activation of the calcium-sensing receptor (CaSR)

Author

Akiyama, Tasuku, Curtis, Eric, Carstens, M Iodi, and Carstens, E

Subjects

Medical Physiology, Biomedical and Clinical Sciences, Neurosciences, Mice, Animals, Receptors, Calcium-Sensing, Capsaicin, Trigeminal Ganglion, Glutathione, TRPA1 Cation Channel, Calcium-sensing receptor (CasR), Calcium imaging, Immunohistochemistry, TRPA1, TRPV1, Kokumi substance, Trigeminal ganglion cell, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Behavioral Science & Comparative Psychology, Biological sciences, Biomedical and clinical sciences, Psychology

Abstract

Some γ-glutamyl peptides including glutathione (γ-Glu-Cys-Gly) and γ-glutamyl-valyl-glycine (γ-Glu-Val-Gly= γ-EVG) are reported to increase the intensity of basic tastes, such as salty, sweet, and umami, although they have no taste themselves at tested concentrations. The mechanism of action of γ-glutamyl peptides is not clearly understood, but the calcium sensing receptor (CaSR) may be involved. Glutathione and γ-EVG enhance the pungency of some spices, and the present study investigated the effects of γ-EVG on the responses of trigeminal ganglion (TG) cells to thermosensitiveTRP channel agonists. Single-cell RT-PCR revealed that most CaSR-expressing cells co-expressed TRPV1 (sensitive to capsaicin) and TRPA1 (sensitive to allyl isothiocyanate= AITC). Intracellular Ca2+ imaging showed that pretreatment with γ-EVG excited 7% of trigeminal ganglion (TG) cells and increased the amplitude of their responses to AITC, but not to capsaicin or menthol. The enhancing effect of γ-EVG was prevented by a CaSR inhibitor. The results indicate that γ-EVG increases AITC pungency by activating a subset of trigeminal ganglion cells that co-express CaSR and TRPA1.

Published

2023

20. A novel indicator to predict the outcome of percutaneous stereotactic radiofrequency rhizotomy for trigeminal neuralgia patients: diffusivity metrics of MR-DTI

Author

Xu Su, Zhengming Wang, Zhijia Wang, Min Cheng, Chao Du, and Yu Tian

Subjects

Diffusion tensor imaging, Trigeminal neuralgia, Abnormal ganglion, Trigeminal ganglion, Percutaneous stereotactic radiofrequency rhizotomy, Medicine, Science

Abstract

Abstract Magnetic resonance-diffusion tensor imaging (MR-DTI) has been used in the microvascular decompression and gamma knife radiosurgery in trigeminal neuralgia (TN) patients; however, use of percutaneous stereotactic radiofrequency rhizotomy (PSR) to target an abnormal trigeminal ganglion (ab-TG) is unreported. Fractional anisotropy (FA), mean and radial diffusivity (MD and RD, respectively), and axial diffusivity (AD) of the trigeminal nerve (CNV) were measured in 20 TN patients and 40 healthy control participants immediately post PSR, at 6-months, and at 1 year. Longitudinal alteration of the diffusivity metrics and any correlation with treatment effects, or prognoses, were analyzed. In the TN group, either low FA (value 17% defined an ab-TG. Two-to-three days post PSR, all 15 patients reported decreased pain scores with increased FA at the ab-TG (P

Published

2024

21. LncRNA Anxa10-203 enhances Mc1r mRNA stability to promote neuropathic pain by recruiting DHX30 in the trigeminal ganglion

Author

YaJing Liu, Fei Liu, YiKe Li, YueLing Li, YuHeng Feng, JiaShuo Zhao, Cheng Zhou, ChunJie Li, JieFei Shen, and YanYan Zhang

Subjects

Trigeminal ganglion, Long non-coding RNA, Neuropathic pain, RNA-binding proteins, DExH-box helicase 30, Melanocortin 1 receptor, Medicine

Abstract

Abstract Background Trigeminal nerve injury is one of the most serious complications in oral clinics, and the subsequent chronic orofacial pain is a consumptive disease. Increasing evidence demonstrates long non-coding RNAs (lncRNAs) play an important role in the pathological process of neuropathic pain. This study aims to explore the function and mechanism of LncRNA Anxa10-203 in the development of orofacial neuropathic pain. Methods A mouse model of orofacial neuropathic pain was established by chronic constriction injury of the infraorbital nerve (CCI-ION). The Von Frey test was applied to evaluate hypersensitivity of mice. RT-qPCR and/or Western Blot were performed to analyze the expression of Anxa10-203, DHX30, and MC1R. Cellular localization of target genes was verified by immunofluorescence and RNA fluorescence in situ hybridization. RNA pull-down and RNA immunoprecipitation were used to detect the interaction between the target molecules. Electrophysiology was employed to assess the intrinsic excitability of TG neurons (TGNs) in vitro. Results Anxa10-203 was upregulated in the TG of CCI-ION mice, and knockdown of Anxa10-203 relieved neuropathic pain. Structurally, Anxa10-203 was located in the cytoplasm of TGNs. Mechanistically, Mc1r expression was positively correlated with Anxa10-203 and was identified as the functional target of Anxa10-203. Besides, Anxa10-203 recruited RNA binding protein DHX30 and formed the Anxa10-203/DHX30 complex to enhance the stability of Mc1r mRNA, resulting in the upregulation of MC1R, which contributed to the enhancement of the intrinsic activity of TGNs in vitro and orofacial neuropathic pain in vivo. Conclusions LncRNA Anxa10-203 in the TG played an important role in orofacial neuropathic pain and mediated mechanical allodynia in CCI-ION mice by binding with DHX30 to upregulate MC1R expression. Graphical Abstract The up-regulated lncRNA Anxa10-203 in the trigeminal ganglion of CCI-ION mice interacts with DHX30 to contribute to the excitability of TG neurons and orofacial pain by enhancing Mc1r mRNA stability.

Published

2024

22. The cellular basis of mechanosensation in mammalian tongue.

Author

Moayedi, Yalda, Xu, Shan, Obayashi, Sophie, Hoffman, Benjamin, Gerling, Gregory, and Lumpkin, Ellen

Subjects

CP: Neuroscience, calcium imaging, clustering analysis, functional classification, lingual innervation, mechanosensation, peripheral nervous system, somatosensation, tongue, trigeminal ganglia, Mice, Animals, Sensory Receptor Cells, Tongue, Trigeminal Ganglion, Touch, Mammals

Abstract

Mechanosensory neurons that innervate the tongue provide essential information to guide feeding, speech, and social grooming. We use in vivo calcium imaging of mouse trigeminal ganglion neurons to identify functional groups of mechanosensory neurons innervating the anterior tongue. These sensory neurons respond to thermal and mechanical stimulation. Analysis of neuronal activity patterns reveal that most mechanosensory trigeminal neurons are tuned to detect moving stimuli across the tongue. Using an unbiased, multilayer hierarchical clustering approach to classify pressure-evoked activity based on temporal response dynamics, we identify five functional classes of mechanosensory neurons with distinct force-response relations and adaptation profiles. These populations are tuned to detect different features of touch. Molecular markers of functionally distinct clusters are identified by analyzing cluster representation in genetically marked neuronal subsets. Collectively, these studies provide a platform for defining the contributions of functionally distinct mechanosensory neurons to oral behaviors crucial for survival in mammals.

Published

2023

23. PACAP38/mast-cell-specific receptor axis mediates repetitive stress-induced headache in mice.

Author

Son, Hyeonwi, Zhang, Yan, Shannonhouse, John, Gomez, Ruben, and Kim, Yu Shin

Subjects

*HOMEOSTASIS, *HEADACHE, *NEURONS, *ENZYME-linked immunosorbent assay, *TRIGEMINAL nerve, *IN vivo studies, *CELLULAR signal transduction, *FLUORESCENT antibody technique, *DESCRIPTIVE statistics, *MAST cells, *MICE, *PSYCHOLOGICAL stress, *ANIMAL experimentation, *SENSORY receptors, *TUMOR necrosis factors, MIGRAINE complications

Abstract

Background: Pain, an evolutionarily conserved warning system, lets us recognize threats and motivates us to adapt to those threats. Headache pain from migraine affects approximately 15% of the global population. However, the identity of any putative threat that migraine or headache warns us to avoid is unknown because migraine pathogenesis is poorly understood. Here, we show that a stress-induced increase in pituitary adenylate cyclase-activating polypeptide-38 (PACAP38), known as an initiator of allosteric load inducing unbalanced homeostasis, causes headache-like behaviour in male mice via mas-related G protein-coupled receptor B2 (MrgprB2) in mast cells. Methods: The repetitive stress model and dural injection of PACAP38 were performed to induce headache behaviours. We assessed headache behaviours using the facial von Frey test and the grimace scale in wild-type and MrgprB2-deficient mice. We further examined the activities of trigeminal ganglion neurons using in vivo Pirt-GCaMP Ca2+ imaging of intact trigeminal ganglion (TG). Results: Repetitive stress and dural injection of PACAP38 induced MrgprB2-dependent headache behaviours. Blood levels of PACAP38 were increased after repetitive stress. PACAP38/MrgprB2-induced mast cell degranulation sensitizes the trigeminovascular system in dura mater. Moreover, using in vivo intact TG Pirt-GCaMP Ca2+ imaging, we show that stress or/and elevation of PACAP38 sensitized the TG neurons via MrgprB2. MrgprB2-deficient mice showed no sensitization of TG neurons or mast cell activation. We found that repetitive stress and dural injection of PACAP38 induced headache behaviour through TNF-a and TRPV1 pathways. Conclusions: Our findings highlight the PACAP38-MrgprB2 pathway as a new target for the treatment of stress-related migraine headache. Furthermore, our results pertaining to stress interoception via the MrgprB2/PACAP38 axis suggests that migraine headache warns us of stress-induced homeostatic imbalance. [ABSTRACT FROM AUTHOR]

Published

2024

24. A novel indicator to predict the outcome of percutaneous stereotactic radiofrequency rhizotomy for trigeminal neuralgia patients: diffusivity metrics of MR-DTI.

Author

Su, Xu, Wang, Zhengming, Wang, Zhijia, Cheng, Min, Du, Chao, and Tian, Yu

Abstract

Magnetic resonance-diffusion tensor imaging (MR-DTI) has been used in the microvascular decompression and gamma knife radiosurgery in trigeminal neuralgia (TN) patients; however, use of percutaneous stereotactic radiofrequency rhizotomy (PSR) to target an abnormal trigeminal ganglion (ab-TG) is unreported. Fractional anisotropy (FA), mean and radial diffusivity (MD and RD, respectively), and axial diffusivity (AD) of the trigeminal nerve (CNV) were measured in 20 TN patients and 40 healthy control participants immediately post PSR, at 6-months, and at 1 year. Longitudinal alteration of the diffusivity metrics and any correlation with treatment effects, or prognoses, were analyzed. In the TN group, either low FA (value < 0.30) or a decreased range compared to the adjacent FA (dFA) > 17% defined an ab-TG. Two-to-three days post PSR, all 15 patients reported decreased pain scores with increased FA at the ab-TG (P < 0.001), but decreased MD and RD (P < 0.01 each). Treatment remained effective in 10 of 14 patients (71.4%) and 8 of 12 patients (66.7%) at the 6-month and 1-year follow-ups, respectively. In patients with ab-TGs, there was a significant difference in treatment outcomes between patients with low FA values (9 of 10; 90%) and patients with dFA (2 of 5; 40%) (P < 0.05). MR-DTI with diffusivity metrics correlated microstructural CNV abnormalities with PSR outcomes. Of all the diffusivity metrics, FA could be considered a novel objective quantitative indicator of treatment effects and a potential indicator of PSR effectiveness in TN patients. [ABSTRACT FROM AUTHOR]

Published

2024

25. Subarachnoid Hemorrhage Depletes Calcitonin Gene-Related Peptide Levels of Trigeminal Neurons in Rat Dura Mater.

Author

Masood, Thannoon, Lakatos, Szandra, Kis, Gyöngyi, Ignácz, Melissza, Domoki, Ferenc, and Rosta, Judit

Subjects

*DURA mater, *CALCITONIN gene-related peptide, *SUBARACHNOID hemorrhage, *NEURONS, *NERVE fibers, *RATS

Abstract

Subarachnoid hemorrhage (SAH) remains a major cause of cerebrovascular morbidity, eliciting severe headaches and vasospasms that have been shown to inversely correlate with vasodilator calcitonin gene-related peptide (CGRP) levels. Although dura mater trigeminal afferents are an important source of intracranial CGRP, little is known about the effects of SAH on these neurons in preclinical models. The present study evaluated changes in CGRP levels and expression in trigeminal primary afferents innervating the dura mater 72 h after experimentally induced SAH in adult rats. SAH, eliciting marked damage revealed by neurological examination, significantly reduced the density of CGRP-immunoreactive nerve fibers both in the dura mater and the trigeminal caudal nucleus in the medulla but did not affect the total dural nerve fiber density. SAH attenuated ex vivo dural CGRP release by ~40% and in the trigeminal ganglion, reduced both CGRP mRNA levels and the number of highly CGRP-immunoreactive cell bodies. In summary, we provide novel complementary evidence that SAH negatively affects the integrity of the CGRP-expressing rat trigeminal neurons. Reduced CGRP levels suggest likely impaired meningeal neurovascular functions contributing to SAH complications. Further studies are to be performed to reveal the importance of impaired CGRP synthesis and its consequences in central sensory processing. [ABSTRACT FROM AUTHOR]

Published

2024

26. Models of Trigeminal Activation: Is There an Animal Model of Migraine?

Author

Spekker, Eleonóra, Fejes-Szabó, Annamária, and Nagy-Grócz, Gábor

Subjects

*MIGRAINE, *ANIMAL models in research, *LABORATORY animals, *SPREADING cortical depression, *PRIMARY headache disorders, *HUMAN ecology, *DURA mater, *MIGRAINE aura

Abstract

Migraine, recognized as a severe headache disorder, is widely prevalent, significantly impacting the quality of life for those affected. This article aims to provide a comprehensive review of the application of animal model technologies in unraveling the pathomechanism of migraine and developing more effective therapies. It introduces a variety of animal experimental models used in migraine research, emphasizing their versatility and importance in simulating various aspects of the condition. It details the benefits arising from the utilization of these models, emphasizing their role in elucidating pain mechanisms, clarifying trigeminal activation, as well as replicating migraine symptoms and histological changes. In addition, the article consciously acknowledges the inherent limitations and challenges associated with the application of animal experimental models. Recognizing these constraints is a fundamental step toward fine-tuning and optimizing the models for a more accurate reflection of and translatability to the human environment. Overall, a detailed and comprehensive understanding of migraine animal models is crucial for navigating the complexity of the disease. These findings not only provide a deeper insight into the multifaceted nature of migraine but also serve as a foundation for developing effective therapeutic strategies that specifically address the unique challenges arising from migraine pathology. [ABSTRACT FROM AUTHOR]

Published

2024

27. Satellite Glial Cells in Human Disease.

Author

Hanani, Menachem

Subjects

*SATELLITE cells, *NEUROGLIA, *SENSORY ganglia, *RHEUMATOID arthritis, *HERPES zoster

Abstract

Satellite glial cells (SGCs) are the main type of glial cells in sensory ganglia. Animal studies have shown that these cells play essential roles in both normal and disease states. In a large number of pain models, SGCs were activated and contributed to the pain behavior. Much less is known about SGCs in humans, but there is emerging recognition that SGCs in humans are altered in a variety of clinical states. The available data show that human SGCs share some essential features with SGCs in rodents, but many differences do exist. SGCs in DRG from patients suffering from common painful diseases, such as rheumatoid arthritis and fibromyalgia, may contribute to the pain phenotype. It was found that immunoglobulins G (IgG) from fibromyalgia patients can induce pain-like behavior in mice. Moreover, these IgGs bind preferentially to SGCs and activate them, which can sensitize the sensory neurons, causing nociception. In other human diseases, the evidence is not as direct as in fibromyalgia, but it has been found that an antibody from a patient with rheumatoid arthritis binds to mouse SGCs, which leads to the release of pronociceptive factors from them. Herpes zoster is another painful disease, and it appears that the zoster virus resides in SGCs, which acquire an abnormal morphology and may participate in the infection and pain generation. More work needs to be undertaken on SGCs in humans, and this review points to several promising avenues for better understanding disease mechanisms and developing effective pain therapies. [ABSTRACT FROM AUTHOR]

Published

2024

28. LncRNA Anxa10-203 enhances Mc1r mRNA stability to promote neuropathic pain by recruiting DHX30 in the trigeminal ganglion.

Author

Liu, YaJing, Liu, Fei, Li, YiKe, Li, YueLing, Feng, YuHeng, Zhao, JiaShuo, Zhou, Cheng, Li, ChunJie, Shen, JieFei, and Zhang, YanYan

Subjects

*RNA analysis, *BIOLOGICAL models, *REVERSE transcriptase polymerase chain reaction, *CELL culture, *ANALYSIS of variance, *ANIMAL experimentation, *FACIAL pain, *SENSORY ganglia, *RISK assessment, *T-test (Statistics), *DESCRIPTIVE statistics, *GENE expression profiling, *REPEATED measures design, *DATA analysis software, *ALLERGIES, *BIOLOGICAL assay, *TRIGEMINAL neuralgia, *MICE, *DISEASE risk factors

Abstract

Background: Trigeminal nerve injury is one of the most serious complications in oral clinics, and the subsequent chronic orofacial pain is a consumptive disease. Increasing evidence demonstrates long non-coding RNAs (lncRNAs) play an important role in the pathological process of neuropathic pain. This study aims to explore the function and mechanism of LncRNA Anxa10-203 in the development of orofacial neuropathic pain. Methods: A mouse model of orofacial neuropathic pain was established by chronic constriction injury of the infraorbital nerve (CCI-ION). The Von Frey test was applied to evaluate hypersensitivity of mice. RT-qPCR and/or Western Blot were performed to analyze the expression of Anxa10-203, DHX30, and MC1R. Cellular localization of target genes was verified by immunofluorescence and RNA fluorescence in situ hybridization. RNA pull-down and RNA immunoprecipitation were used to detect the interaction between the target molecules. Electrophysiology was employed to assess the intrinsic excitability of TG neurons (TGNs) in vitro. Results: Anxa10-203 was upregulated in the TG of CCI-ION mice, and knockdown of Anxa10-203 relieved neuropathic pain. Structurally, Anxa10-203 was located in the cytoplasm of TGNs. Mechanistically, Mc1r expression was positively correlated with Anxa10-203 and was identified as the functional target of Anxa10-203. Besides, Anxa10-203 recruited RNA binding protein DHX30 and formed the Anxa10-203/DHX30 complex to enhance the stability of Mc1r mRNA, resulting in the upregulation of MC1R, which contributed to the enhancement of the intrinsic activity of TGNs in vitro and orofacial neuropathic pain in vivo. Conclusions: LncRNA Anxa10-203 in the TG played an important role in orofacial neuropathic pain and mediated mechanical allodynia in CCI-ION mice by binding with DHX30 to upregulate MC1R expression. The up-regulated lncRNA Anxa10-203 in the trigeminal ganglion of CCI-ION mice interacts with DHX30 to contribute to the excitability of TG neurons and orofacial pain by enhancing Mc1r mRNA stability. [ABSTRACT FROM AUTHOR]

Published

2024

29. New Evidence for Regulatory Role of Trigeminal Ganglion on the Intraocular Pressure Following Subarachnoid Hemorrhage.

Author

Findik, Huseyin, Kanat, Ayhan, Aydin, Mehmet Dumlu, Guvercin, Ali Riza, and Ozmen, Sevilay

Abstract

Background Increased intraocular pressure (IOP) likely secondary to an activated oculo-trigeminal reflex network is an important issue following subarachnoid hemorrhage (SAH). The relationship between the IOP and trigeminal ganglion (TGG) following experimental SAH was investigated in this study. Methods Twenty-three rabbits were used in this study. Five rabbits (n = 5) were used as the control group, another 5 as the sham group (n = 5), and the remaining 13 (n = 13) as the study group. The study group was further divided into two groups of animals with mild (n = 6) and severe (n = 7) TGG degeneration. The IOP values were recorded. After 2 weeks, the animals were decapitated. The mean degenerated neuron density of TGGs was estimated by stereological methods and analyzed statistically. Results The average IOP values were 11.85, 14.12, and 21.45 mm Hg in the control (n = 5), sham (n = 5), and study (n = 13) groups, respectively. The mean degenerated neuron density was 34, 237, and 3,165 mm3 in the control, sham, and study groups, respectively. Conclusion According to the findings of this study, the experimental SAH leads to changes in IOP by affecting the TGG. By predicting and preventing IOP elevation in the setting of SAH, our findings will shed light on secondary sequelae such as glaucoma and irreversible blindness. [ABSTRACT FROM AUTHOR]

Published

2024

30. In situ tissue profile of rat trigeminal nerve in trigeminal neuralgia using spatial transcriptome sequencing.

Author

Wenbin Wei, Yuemin Liu, Yifen Shen, Tao Yang, Yabing Dong, Zixiang Han, Yiwen Wang, Zhiyang Liu, Ying Chai, Mengjie Zhang, Hanshao Wang, Hao Shen, Yihang Shen, and Minjie Chen

Abstract

Background: Trigeminal neuralgia (TN) is the most common neuropathic disorder in the maxillofacial region. The etiology and pathogenesis of TN have not been clearly determined to date, although there are many hypotheses. Objective: The goal of this study was to investigate the interactions between different types of cells in TN, particularly the impact and intrinsic mechanism of demyelination on the trigeminal ganglion, and to identify new important target genes and regulatory pathways in TN. Methods: TN rat models were prepared by trigeminal root compression, and trigeminal nerve tissues were isolated for spatial transcriptome sequencing. The gene expression matrix was reduced dimensionally by PCA and presented by UMAP. Gene function annotation was analyzed by Metascape. The progression of certain clusters and the developmental pseudotime were analyzed using the Monocle package. Modules of the gene coexpression network between different groups were analyzed based on weighted gene coexpression network analysis and assigned AddModuleScore values. The intercellular communication of genes in these networks via ligand--receptor interactions was analyzed using CellPhoneDB analysis. Results: The results suggested that the trigeminal ganglion could affect Schwann cell demyelination and remyelination responses through many ligand--receptor interactions, while the effect of Schwann cells on the trigeminal ganglion was much weaker. Additionally, ferroptosis may be involved in the demyelination of Schwann cells. Conclusions: This study provides spatial transcriptomics sequencing data on TN, reveals new markers, and redefines the relationship between the ganglion and myelin sheath, providing a theoretical basis and supporting data for future mechanistic research and drug development. [ABSTRACT FROM AUTHOR]

Published

2024

31. Early embryogenesis in CHDFIDD mouse model reveals facial clefts and altered cranial neurogenesis

Author

Marek Hampl, Nela Jandová, Denisa Lusková, Monika Nováková, Tereza Szotkowská, Štěpán Čada, Jan Procházka, Jiri Kohoutek, and Marcela Buchtová

Subjects

craniofacial development, orofacial clefts, axons, neurite outgrowth, cdk13, trigeminal ganglion, Medicine, Pathology, RB1-214

Published

2024

32. Variations in arterial sources and supply patterns to the human trigeminal ganglion with clinical significance

Author

Ethan L. Snow, William Srinivasan, Annika Covington, Matthew Vilburn, Travis L. McCumber, and William Thorell

Subjects

Trigeminal ganglion, Trigeminal nerve, Meckel's cave, CN V neurovasculature, Trigeminal neuralgia, Trigeminal neuropathy, Human anatomy, QM1-695

Abstract

Introduction: Trigeminal ganglia (TG) are bilateral collections of cell bodies from the first-order pseudounipolar neurons in each trigeminal nerve. Branches of the internal carotid artery (ICA), middle meningeal artery (MMA), accessory meningeal artery (AMA), and superior cerebellar artery (SCA) have been known to supply the TG, but information about the prevalence and patterns of these vessels supplying the TG is limited despite their important clinical relevance to basicranial surgeries. The objective of this study is to investigate the arterial sources and supply patterns to the TG and discuss their clinical implications. Methods: Gross arterial sources and supply patterns were examined on 139 TG from 90 embalmed human cadavers from ethically approved anatomical donor programs. Select specimens were photographed, and color replacement was utilized to aid structure identification. Vascular histology was examined with light microscopy and photographed on one specimen for methods validation. Results: One hundred and one TG (72.7%) received arterial supply from a single source: 71 (51.1%) from ICA, 18 (12.9%) from AMA, and 12 (8.6%) from MMA. Thirty-seven TG (26.6%) exhibited two distinct arterial sources from ICA, AMA, or MMA in either anastomotic (n = 25; 18.0%) or dual-independent (n = 12; 8.6%) patterns. One TG (0.7%) received supply from ICA, AMA, and MMA in a complex pattern. No gross arterial supply from SCA was found. Conclusions: The TG is predominantly supplied by ICA (prevalence = 76.3%), though AMA and MMA also represent considerable contributions (31.7% and 20.1%, respectively) in various supply patterns. The TG arterial sources and supply patterns reported in this study should be considered when deliberating treatment of meningiomas, schwannomas, and dural arteriovenous fistulas within and around Meckel's cave.

Published

2024

33. N-methyl-D-aspartate Receptor Subunits 2A and 2B Mediate Connexins and Pannexins in the Trigeminal Ganglion Involved in Orofacial Inflammatory Allodynia during Temporomandibular Joint Inflammation

Author

Li, Yue-Ling, Zhang, Yan-Yan, Song, Qin-Xuan, Liu, Fei, Liu, Ya-Jing, Li, Yi-Ke, Zhou, Cheng, and Shen, Jie-Fei

Published

2024

34. Transmaxillary approach for resection of maxillary division trigeminal schwannoma at foramen rotundum.

Author

Nassiri, Farshad, Liang, Allison, Agnoletto, Guilherme J., and Couldwell, William T.

Subjects

*CAVERNOUS sinus, *SKULL base, *SCHWANNOMAS, *MAXILLARY nerve, *FACIAL pain, *TREATMENT effectiveness, TUMOR surgery

Abstract

Background: The foramen rotundum and anterior cavernous sinus have traditionally been accessed by transcranial approaches that are limited by the high density of critical neurovascular structures. The transmaxillary approach provides an entirely extradural route to the foramen rotundum and anterior cavernous sinus. Method: This patient with neurofibromatosis and facial pain with trigeminal schwannoma at the foramen rotundum was successfully treated by transmaxillary resection of the tumor. This approach allowed for a direct extradural access to the pathology, with bony decompression and tumor resection, avoiding transcranial routes. Conclusion: The transmaxillary approach provides a safe and entirely extradural corridor to access smaller localized skull base lesions at and surrounding the cavernous sinus. [ABSTRACT FROM AUTHOR]

Published

2024

35. Effect of propranolol on temporomandibular joint pain in repeatedly stressed rats.

Author

Zanelatto, Fernanda Barchesi, Vieira, Willians Fernando, Nishijima, Catarine Massucato, Zanotto, Tamires Marques, Magalhães, Silviane Fernandes de, Sartori, César Renato, Parada, Carlos Amilcar, and Tambeli, Claudia Herrera

Subjects

*PHYSIOLOGICAL stress, *EXPERIMENTAL design, *REVERSE transcriptase polymerase chain reaction, *TEMPOROMANDIBULAR joint, *PAIN, *PROPRANOLOL, *ANIMAL experimentation, *TREATMENT effectiveness, *RATS, *GENE expression, *T-test (Statistics), *INTRA-articular injections, *RESEARCH funding, *DESCRIPTIVE statistics, *DOSE-effect relationship in pharmacology, *DATA analysis software, *EVALUATION

Abstract

Stress substantially increases the risk of developing painful temporomandibular disorders (TMDs) by influencing the release of endogenous catecholamines. Propranolol, an antagonist of β‐adrenergic receptors, has shown potential in alleviating TMD‐associated pain, particularly when the level of catecholamines is elevated. The aim of this study was to explore whether intra‐articular propranolol administration is effective in diminishing temporomandibular joint (TMJ) pain during repeated stress situations. Additionally, we investigated the effect of repeated stress on the expression of genes encoding β‐adrenoceptors in the trigeminal ganglion. In the present study, rats were exposed to a stress protocol induced by sound, then to the administration of formalin in the TMJ (to elicit a nociceptive response), followed immediately afterward by different doses of propranolol, after which the analgesic response to propranolol was evaluated. We also assessed the levels of beta‐1 and beta‐2 adrenergic receptor mRNAs (Adrb1 and Adrb2, respectively) using reverse transcription–quantitative PCR (RT‐qPCR). Our findings revealed that propranolol administration reduces formalin‐induced TMJ nociception more effectively in stressed rats than in non‐stressed rats. Furthermore, repeated stress decreases the expression of the Adrb2 gene within the trigeminal ganglion. The findings of this study are noteworthy as they suggest that individuals with a chronic stress history might find potential benefits from β‐blockers in TMD treatment. [ABSTRACT FROM AUTHOR]

Published

2024

36. The G protein‐coupled estrogen receptor of the trigeminal ganglion regulates acute and chronic itch in mice.

Author

Li, Jun, Gao, Po, Zhang, Siyu, Lin, Xiaoqi, Chen, Junhui, Zhang, Song, Jiao, Yingfu, Yu, Weifeng, Xia, Xiaoqiong, and Yang, Liqun

Subjects

*ITCHING, *G protein coupled receptors, *SENSORY neurons, *GANGLIA, *PAIN perception

Abstract

Aims: Itch is an unpleasant sensation that severely impacts the patient's quality of life. Recent studies revealed that the G protein‐coupled estrogen receptor (GPER) may play a crucial role in the regulation of pain and itch perception. However, the contribution of the GPER in primary sensory neurons to the regulation of itch perception remains elusive. This study aimed to investigate whether and how the GPER participates in the regulation of itch perception in the trigeminal ganglion (TG). Methods and Results: Immunofluorescence staining results showed that GPER‐positive (GPER+) neurons of the TG were activated in both acute and chronic itch. Behavioral data indicated that the chemogenetic activation of GPER+ neurons of the TG of Gper‐Cre mice abrogated scratching behaviors evoked by acute and chronic itch. Conversely, the chemogenetic inhibition of GPER+ neurons resulted in increased itch responses. Furthermore, the GPER expression and function were both upregulated in the TG of the dry skin‐induced chronic itch mouse model. Pharmacological inhibition of GPER (or Gper deficiency) markedly increased acute and chronic itch‐related scratching behaviors in mouse. Calcium imaging assays further revealed that Gper deficiency in TG neurons led to a marked increase in the calcium responses evoked by agonists of the transient receptor potential ankyrin A1 (TRPA1) and transient receptor potential vanilloid V1 (TRPV1). Conclusion: Our findings demonstrated that the GPER of TG neurons is involved in the regulation of acute and chronic itch perception, by modulating the function of TRPA1 and TRPV1. This study provides new insights into peripheral itch sensory signal processing mechanisms and offers new targets for future clinical antipruritic therapy. [ABSTRACT FROM AUTHOR]

Published

2024

37. Three‐dimensional topography of rat trigeminal ganglion neurons using a combination of retrograde labeling and tissue‐clearing techniques.

Author

Kuramoto, Eriko, Fukushima, Makoto, Sendo, Ryozo, Ohno, Sachi, Iwai, Haruki, Yamanaka, Atsushi, Sugimura, Mitsutaka, and Goto, Tetsuya

Abstract

The trigeminal nerve is the sensory afferent of the orofacial regions and divided into three major branches. Cell bodies of the trigeminal nerve lie in the trigeminal ganglion and are surrounded by satellite cells. There is a close interaction between ganglion cells via satellite cells, but the function is not fully understood. In the present study, we clarified the ganglion cells' three‐dimensional (3D) localization, which is essential to understand the functions of cell–cell interactions in the trigeminal ganglion. Fast blue was injected into 12 sites of the rat orofacial regions, and ganglion cells were retrogradely labeled. The labeled trigeminal ganglia were cleared by modified 3DISCO, imaged with confocal laser‐scanning microscopy, and reconstructed in 3D. Histograms of the major axes of the fast blue‐positive somata revealed that the peak major axes of the cells innervating the skin/mucosa were smaller than those of cells innervating the deep structures. Ganglion cells innervating the ophthalmic, maxillary, and mandibular divisions were distributed in the anterodorsal, central, and posterolateral portions of the trigeminal ganglion, respectively, with considerable overlap in the border region. The intermingling in the distribution of ganglion cells within each division was also high, in particular, within the mandibular division. Specifically, intermingling was observed in combinations of tongue and masseter/temporal muscles, maxillary/mandibular molars and masseter/temporal muscles, and tongue and mandibular molars. Double retrograde labeling confirmed that some ganglion cells innervating these combinations were closely apposed. Our data provide essential information for understanding the function of ganglion cell–cell interactions via satellite cells. [ABSTRACT FROM AUTHOR]

Published

2024

38. Overlooked evidence for transmission deficit of pupillary light reflex can be secondary to trigeminal nerve ganglion degeneration following subarachnoid hemorrhage; preliminary experimental study.

Author

Sahin, Mehmet Hakan, Kanat, Ayhan, Karadag, Mehmet Kursat, Akyuz, Mehmet Emin, Keles, Osman Nuri, Gundogdu, Omer Lutfi, Findik, Huseyin, Aydin, Mehmet Dumlu, Gel, Mehmet Selim, and Daltaban, Iskender Samet

Subjects

PUPILLOMETRY, PUPILLARY reflex, TRIGEMINAL nerve, SUBARACHNOID hemorrhage, NEURODEGENERATION, MANN Whitney U Test

Abstract

Although the effect of oculomotor and cervical sympathetic networks on pupil diameter is well known; the effect of the trigeminal nerve on pupil diameter has not been investigated yet. This subject was investigated. Five of 23 rabbits were used as a control group (GI; n = 5); 0.5 ccs saline solution into cisterna magna injected animals used as SHAM (GII; n = 5); autologous blood injected to produce SAH used as the study group (GIII; n = 13) and followed up three weeks. Light-stimulated pupil diameters were measured with an ocular tomography device before, middle, and at the end of the experiment. Considering the sclera area/pupil area ratio index (PRI) as the pupillary reaction area, we used this equation for the pupil's rush to light. Degenerated neuron densities of trigeminal ganglia and pupil diameters compared with the Mann-Whitney U test. The PRI, degenerated neuron density of trigeminal ganglia (n/mm3) were: (2.034 ± 0.301)/(13 ± 3) in GI; (1.678 ± 0.211)/(46 ± 9) in GII; and (0.941 ± 0.136)/(112 ± 21) in GIII. P-values between groups as: p < 0.005 in GI/GII; p < 0.0001 in GII/GIII and p < 0.00001 in GI/GIII. Light stimulates the cornea which is innervated by the trigeminal nerves. This experimental study indicates that the pupil remains mydriatic as the cornea is damaged by trigeminal ischemia following SAH and blocks the light flow. [ABSTRACT FROM AUTHOR]

Published

2024

39. The CSF1-CSF1R pathway in the trigeminal ganglion mediates trigeminal neuralgia via inflammatory responses in mice.

Author

He, Zile, Xu, Chao, Guo, Jiaqi, Liu, Tianyu, Zhang, Yunpeng, and Feng, Yi

Abstract

Background: Trigeminal neuralgia (TN) is the most severe type of neuropathic pain. The trigeminal ganglion (TG) is a crucial target for the pathogenesis and treatment of TN. The colony-stimulating factor 1 (CSF1) - colony-stimulating factor 1 receptor (CSF1R) pathway regulates lower limb pain development. However, the effect and mechanism of the CSF1-CSF1R pathway in TG on TN are unclear. Methods: Partial transection of the infraorbital nerve (pT-ION) model was used to generate a mouse TN model. Mechanical and cold allodynia were used to measure pain behaviors. Pro-inflammatory factors (IL-6, TNF-a) were used to measure inflammatory responses in TG. PLX3397, an inhibitor of CSF1R, was applied to inhibit the CSF1-CSF1R pathway in TG. This pathway was activated in naïve mice by stereotactic injection of CSF1 into the TG. Results: The TN model activated the CSF1-CSF1R pathway in the TG, leading to exacerbated mechanical and cold allodynia. TN activated inflammatory responses in the TG manifested as a significant increase in IL-6 and TNF-a levels. After using PLX3397 to inhibit CSF1R, CSF1R expression in the TG declined significantly. Inhibiting the CSF1-CSF1R pathway in the TG downregulated the expression of IL-6 and TNF-α to reduce allodynia-related behaviors. Finally, mechanical allodynia behaviors were exacerbated in naïve mice after activating the CSF1-CSF1R pathway in the TG. Conclusions: The CSF1-CSF1R pathway in the TG modulates TN by regulating neuroimmune responses. Our findings provide a theoretical basis for the development of treatments for TN in the TG. [ABSTRACT FROM AUTHOR]

Published

2024

40. Expression of CGRP in the Trigeminal Ganglion and Its Effect on the Polarization of Macrophages in Rats with Temporomandibular Arthritis.

Author

Tao, Junli, Wang, Xiaohui, and Xu, Jie

Abstract

Calcitonin gene-related peptide (CGRP) is synthesized and secreted by trigeminal ganglion neurons, and is a key neuropeptide involved in pain and immune regulation. This study investigates the expression of CGRP in the trigeminal ganglion (TG) and its regulatory role in the polarization of macrophages in rats with temporomandibular arthritis. A rat model of temporomandibular arthritis was established using CFA. Pain behavior was then observed. Temporomandibular joint (TMJ) and the TG were collected, and immunohistochemistry, immunofluorescence (IF) staining, and RT-qPCR were used to examine the expression of CGRP and macrophage-related factors. To investigate the impact of CGRP on macrophage polarization, both CGRP and its antagonist, CGRP 8-37, were separately administered directly within the TG. Statistical analysis revealed that within 24 h of inducing temporomandibular arthritis using CFA, there was a significant surge in CD86 positive macrophages within the ganglion. These macrophages peaked on the 7th day before beginning their decline. In this context, it’s noteworthy that administering CGRP to the trigeminal ganglion can prompt these macrophages to adopt the M2 phenotype. Intriguingly, this study demonstrates that injecting the CGRP receptor antagonist (CGRP 8-37) to the ganglion counteracts this shift towards the M2 phenotype. Supporting these in vivo observations, we found that in vitro, CGRP indeed fosters the M2-type polarization of macrophages. CGRP can facilitate the conversion of macrophages into the M2 phenotype. The phenotypic alterations of macrophages within the TG could be instrumental in initiating and further driving the progression of TMJ disorders. [ABSTRACT FROM AUTHOR]

Published

2024

41. Anatomical measurements of trigeminal ganglion: a cadaver study.

Author

Zhang, Xiang, Bai, Yong, Hou, Jianfei, Chen, Wenbin, Cheng, Kailiang, Zi, Longjin, and Wang, Ping

Subjects

*MEDICAL cadavers, *TRIGEMINAL neuralgia, *GANGLIA, *RHIZOTOMY, *RADIO frequency, *ATRIAL flutter

Abstract

It is difficult to obtain specific information regarding the trigeminal ganglion (TG), especially pediatric TG. The aim of present study was to determine the parameters of the TG and assist in the neuroablative treatment of trigeminal neuralgia (TN). Thirty-seven sides of cadaver heads that had undergone gross anatomical examination were included, with 29 sides of adults and 8 sides of infants. The distance and angles were measured among 12 points, with nine points adjacent to the TG and three points on the foramen ovale (FO). The three points on FO were represented as three different surgical approaches for TN: posterior FO approach (PFO), lateral FO approach (LFO), and anterior FO approach (AFO). A high similarity was found in pediatric TG. No statistical difference was detected in either the distance or the angles between the 12 points. Statistical difference was found in adult heads in some of the distances, which included PFO to point 5 (17.97 ± 3.35 mm in the left and 15.52 ± 2.28 mm in the right; p = 0.03) and LFO to point 5 and point 8. Moreover, the angle for PFO to point 5 showed a statistically significant difference (60.10 ± 14.02 in the left and 46.63 ± 10.48 in the right; p = 0.01). These findings revealed that surgical neuroablation for patients with TN should be performed more carefully when the PFO or LFO approach is adopted, with a precise preoperative evaluation to avoid corneal complications. Two safety radiofrequency rhizotomy points are also presented to deal with two different kinds of TN. [ABSTRACT FROM AUTHOR]

Published

2024

42. Норадренергічний вплив на тонічну імпульсацію нейронів ганглія трійчастого нерва.

Author

Телька, М. В., Маслов, В. Ю., Веселовський, М. С., and Федулова, С. А.

Abstract

Adrenoreceptors play a key role in sympathetic influences on sensory neurons in normal and neuropathic conditions. We studied noradrenaline action on tonic firing in cultured rat trigeminal ganglion neurons. In a majority of the neurons (68%), Noradrenaline application had no marked effect on the firing properties. The rest of the cells (32%) were highly sensitive to noradrenaline action; they lost the ability to tonic firing and single action potential parameters significantly changed. It was established that NA-induced action on the firing is mainly due to the activation kinetics slowing of voltage-gated calcium channels. The data suggest a possibility of differential sympatho-sensory interaction in the trigeminal pathways. [ABSTRACT FROM AUTHOR]

Published

2024

43. PAR2-dependent phosphorylation of TRPV4 at the trigeminal nerve terminals contributes to tongue cancer pain.

Author

Akasaka, Ryuta, Furukawa, Akihiko, Hayashi, Yoshinori, Hitomi, Suzuro, Koyama, Ryo, Oshima, Eri, Tamura, Miki, Yonemoto, Mamiko, Hojo, Yasushi, Takahashi, Ryosuke, Shibuta, Ikuko, Iwata, Koichi, Yonehara, Yoshiyuki, and Shinoda, Masamichi

Abstract

This study aimed to clarify the interactions between the tongue and primary afferent fibers in tongue cancer pain. A pharmacological analysis was conducted to evaluate mechanical hypersensitivity of the tongues of rats with squamous cell carcinoma (SCC). Changes in trigeminal ganglion (TG) neurons projecting to the tongue were analyzed using immunohistochemistry and western blotting. SCC inoculation of the tongue caused persistent mechanical sensitization and tumor formation. Trypsin expression was significantly upregulated in cancer lesions. Continuous trypsin inhibition or protease-activated receptor 2 (PAR2) antagonism in the tongue significantly inhibited SCC-induced mechanical sensitization. No changes were observed in PAR2 and transient receptor potential vanilloid 4 (TRPV4) levels in the TG or the number of PAR2-and TRPV4-expressing TG neurons after SCC inoculation. In contrast, the relative amount of phosphorylated TRPV4 in the TG was significantly increased after SCC inoculation and abrogated by PAR2 antagonism in the tongue. TRPV4 antagonism in the tongue significantly ameliorated the mechanical sensitization caused by SCC inoculation. Our findings indicate that tumor-derived trypsin sensitizes primary afferent fibers by PAR2 stimulation and subsequent TRPV4 phosphorylation, resulting in severe tongue pain. [ABSTRACT FROM AUTHOR]

Published

2023

44. Angle and Distance Analysis on Percutaneous Trigeminal Radiofrequency Rhizotomy for Trigeminal Neuralgia.

Author

Güner, Yahya Efe, Salman, Necati, and Savaş, Ali

Subjects

TRIGEMINAL neuralgia, RHIZOTOMY, SURGEONS, ANALGESIA, RADIOLOGY

Abstract

Copyright of Journal of Ankara University Faculty of Medicine / Ankara Üniversitesi Tip Fakültesi Mecmuasi is the property of Galenos Yayinevi Tic. LTD. STI and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

45. Antiviral CD19+CD27+ Memory B Cells Are Associated with Protection from Recurrent Asymptomatic Ocular Herpesvirus Infection

Author

Dhanushkodi, Nisha R, Prakash, Swayam, Srivastava, Ruchi, Coulon, Pierre-Gregoire A, Arellano, Danielle, Kapadia, Rayomand V, Fahim, Raian, Suzer, Berfin, Jamal, Leila, Vahed, Hawa, and BenMohamed, Lbachir

Subjects

Immunization, Sexually Transmitted Infections, Infectious Diseases, Biotechnology, Rare Diseases, Neurosciences, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Animals, Antigens, CD19, Herpes Simplex, Herpesvirus 1, Human, Immunity, Immunoglobulin A, Immunoglobulin G, Keratitis, Herpetic, Memory B Cells, Mice, Reinfection, Trigeminal Ganglion, Tumor Necrosis Factor Receptor Superfamily, Member 7, Virus Activation, B memory cells, plasma cells, ocular herpes, asymptomatic herpes, virus-specific B cell, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology

Abstract

Reactivation of herpes simplex virus 1 (HSV-1) from latently infected neurons of the trigeminal ganglia (TG) leads to blinding recurrent herpetic disease in symptomatic (SYMP) individuals. Although the role of T cells in herpes immunity seen in asymptomatic (ASYMP) individuals is heavily explored, the role of B cells is less investigated. In the present study, we evaluated whether B cells are associated with protective immunity against recurrent ocular herpes. The frequencies of circulating HSV-specific memory B cells and of memory follicular helper T cells (CD4+ Tfh cells), which help B cells produce antibodies, were compared between HSV-1-infected SYMP and ASYMP individuals. The levels of IgG/IgA and neutralizing antibodies were compared in SYMP and ASYMP individuals. We found that (i) the ASYMP individuals had increased frequencies of HSV-specific CD19+CD27+ memory B cells, and (ii) high frequencies of HSV-specific switched IgG+CD19+CD27+ memory B cells detected in ASYMP individuals were directly proportional to high frequencies of CD45R0+CXCR5+CD4+ memory Tfh cells. However, no differences were detected in the level of HSV-specific IgG/IgA antibodies in SYMP and ASYMP individuals. Using the UV-B-induced HSV-1 reactivation mouse model, we found increased frequencies of HSV-specific antibody-secreting plasma HSV-1 gD+CD138+ B cells within the TG and circulation of ASYMP mice compared to those of SYMP mice. In contrast, no significant differences in the frequencies of B cells were found in the cornea, spleen, and bone-marrow. Our findings suggest that circulating antibody-producing HSV-specific memory B cells recruited locally to the TG may contribute to protection from symptomatic recurrent ocular herpes. IMPORTANCE Reactivation of herpes simplex virus 1 (HSV-1) from latently infected neurons of the trigeminal ganglia (TG) leads to blinding recurrent herpetic disease in symptomatic (SYMP) individuals. Although the role of T cells in herpes immunity against blinding recurrent herpetic disease is heavily explored, the role of B cells is less investigated. In the present study, we found that in both asymptomatic (ASYMP) individuals and ASYMP mice, there were increased frequencies of HSV-specific memory B cells that were directly proportional to high frequencies of memory Tfh cells. Moreover, following UV-B-induced reactivation, we found increased frequencies of HSV-specific antibody-secreting plasma B cells within the TG and circulation of ASYMP mice compared to those of SYMP mice. Our findings suggest that circulating antibody-producing HSV-specific memory B cells recruited locally to the TG may contribute to protection from recurrent ocular herpes.

Published

2022

46. Progesterone distribution in the trigeminal system and its role to modulate sensory neurotransmission: influence of sex

Author

Aida Maddahi, Karin Warfvinge, Anja Holm, Jacob C. A. Edvinsson, Philip Victor Reducha, Spyridoula Kazantzi, Kristian A. Haanes, and Lars Edvinsson

Subjects

Progesterone, Trigeminal ganglion, Dura matter, Progesterone receptor, CGRP, Migraine, Medicine

Abstract

Abstract Background Women are disproportionately affected by migraine, representing up to 75% of all migraine cases. This discrepancy has been proposed to be influenced by differences in hormone levels between the sexes. One such hormone is progesterone. Calcitonin gene-related peptide (CGRP) system is an important factor in migraine pathophysiology and could be influenced by circulating hormones. The purpose of this study was to investigate the distribution of progesterone and its receptor (PR) in the trigeminovascular system, and to examine the role of progesterone to modulate sensory neurotransmission. Methods Trigeminal ganglion (TG), hypothalamus, dura mater, and the basilar artery from male and female rats were carefully dissected. Expression of progesterone and PR proteins, and mRNA levels from TG and hypothalamus were analyzed by immunohistochemistry and real-time quantitative PCR. CGRP release from TG and dura mater were measured using an enzyme-linked immunosorbent assay. In addition, the vasomotor effect of progesterone on male and female basilar artery segments was investigated with myography. Results Progesterone and progesterone receptor -A (PR-A) immunoreactivity were found in TG. Progesterone was located predominantly in cell membranes and in Aδ-fibers, and PR-A was found in neuronal cytoplasm and nucleus, and in satellite glial cells. The number of positive progesterone immunoreactive cells in the TG was higher in female compared to male rats. The PR mRNA was expressed in both hypothalamus and TG; however, the PR expression level was significantly higher in the hypothalamus. Progesterone did not induce a significant change neither in basal level nor upon stimulated release of CGRP from dura mater or TG in male or female rats when compared to the vehicle control. However, pre-treated with 10 µM progesterone weakly enhanced capsaicin induced CGRP release observed in the dura mater of male rats. Similarly, in male basilar arteries, progesterone significantly amplified the dilation in response to capsaicin. Conclusions In conclusion, these results highlight the potential for progesterone to modulate sensory neurotransmission and vascular responses in a complex manner, with effects varying by sex, tissue type, and the nature of the stimulus. Further investigations are needed to elucidate the underlying mechanisms and physiological implications of these findings. Graphical Abstract

Published

2023

47. Histopathologic Examinations Following Neuraxial Drug Delivery

Author

Cramer, Sarah D., Butt, Mark T., Yaksh, Tony, editor, and Hayek, Salim, editor

Published

2023

48. Varicella-zoster virus proteome-wide T-cell screening demonstrates low prevalence of virus-specific CD8 T-cells in latently infected human trigeminal ganglia

Author

Michiel van Gent, Werner J. D. Ouwendijk, Victoria L. Campbell, Kerry J. Laing, Georges M. G. M. Verjans, and David M. Koelle

Subjects

Varicella-zoster virus, Herpes simplex virus, Human, Trigeminal ganglion, Latency, T-cells, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Trigeminal ganglia (TG) neurons are an important site of lifelong latent varicella-zoster virus (VZV) infection. Although VZV-specific T-cells are considered pivotal to control virus reactivation, their protective role at the site of latency remains uncharacterized. Methods Paired blood and TG specimens were obtained from ten latent VZV-infected adults, of which nine were co-infected with herpes simplex virus type 1 (HSV-1). Short-term TG-derived T-cell lines (TG-TCL), generated by mitogenic stimulation of TG-derived T-cells, were probed for HSV-1- and VZV-specific T-cells using flow cytometry. We also performed VZV proteome-wide screening of TG-TCL to determine the fine antigenic specificity of VZV reactive T-cells. Finally, the relationship between T-cells and latent HSV-1 and VZV infections in TG was analyzed by reverse transcription quantitative PCR (RT-qPCR) and in situ analysis for T-cell proteins and latent viral transcripts. Results VZV proteome-wide analysis of ten TG-TCL identified two VZV antigens recognized by CD8 T-cells in two separate subjects. The first was an HSV-1/VZV cross-reactive CD8 T-cell epitope, whereas the second TG harbored CD8 T-cells reactive with VZV specifically and not the homologous peptide in HSV-1. In silico analysis showed that HSV-1/VZV cross reactivity of TG-derived CD8 T-cells reactive with ten previously identified HSV-1 epitopes was unlikely, suggesting that HSV-1/VZV cross-reactive T-cells are not a common feature in dually infected TG. Finally, no association was detected between T-cell infiltration and VZV latency transcript abundance in TG by RT-qPCR or in situ analyses. Conclusions The low presence of VZV- compared to HSV-1-specific CD8 T-cells in human TG suggests that VZV reactive CD8 T-cells play a limited role in maintaining VZV latency.

Published

2023

49. Sensitization of meningeal afferents to locomotion-related meningeal deformations in a migraine model

Author

Andrew S Blaeser, Jun Zhao, Arthur U Sugden, Simone Carneiro-Nascimento, Mark L Andermann, and Dan Levy

Subjects

migraine, afferent, trigeminal ganglion, locomotion, meninges, deformation, Medicine, Science, Biology (General), QH301-705.5

Abstract

Migraine headache is hypothesized to involve the activation and sensitization of trigeminal sensory afferents that innervate the cranial meninges. To better understand migraine pathophysiology and improve clinical translation, we used two-photon calcium imaging via a closed cranial window in awake mice to investigate changes in the responses of meningeal afferent fibers using a preclinical model of migraine involving cortical spreading depolarization (CSD). A single CSD episode caused a seconds-long wave of calcium activation that propagated across afferents and along the length of individual afferents. Surprisingly, unlike previous studies in anesthetized animals with exposed meninges, only a very small afferent population was persistently activated in our awake mouse preparation, questioning the relevance of this neuronal response to the onset of migraine pain. In contrast, we identified a larger subset of meningeal afferents that developed augmented responses to acute three-dimensional meningeal deformations that occur in response to locomotion bouts. We observed increased responsiveness in a subset of afferents that were already somewhat sensitive to meningeal deformation before CSD. Furthermore, another subset of previously insensitive afferents also became sensitive to meningeal deformation following CSD. Our data provides new insights into the mechanisms underlying migraine, including the emergence of enhanced meningeal afferent responses to movement-related meningeal deformations as a potential neural substrate underlying the worsening of migraine headache during physical activity.

Published

2024

50. Sex differences in expression of CGRP family of receptors and ligands in the rat trigeminal system

Author

Maddahi, Aida, Edvinsson, Jacob C. A., and Edvinsson, Lars

Published

2024