Your search keyword '"hyperalgesia"' showing total 1,763 results

1. Gadolinium-based contrast agents aggravate mechanical and thermal hyperalgesia in a nitroglycerine-induced migraine model in male mice.

Author

Bilgin, Batuhan, Adam, Muhammed, Hekim, Munevver Gizem, Bulut, Ferah, and Ozcan, Mete

Subjects

*CONTRAST media, *MALE models, *MIGRAINE, *HYPERALGESIA, *SUMATRIPTAN, *PAIN threshold, *NEUROVASCULAR diseases

Abstract

In the diagnosis of migraine, which is a neurovascular disease, gadolinium-based contrast agents (GBCAs) are used to rule out more serious conditions. On the other hand, it remains unclear as a scientific gap whether GBCAs may trigger migraine-related pain. The aim of this study was to investigate the effect of GBCAs on mechanical and thermal pain behaviour in a nitroglycerin (NTG)-induced migraine model in mice. NTG (10 mg/kg) was administered intraperitoneally to adult (6–8 weeks old) BALB/c mice 2 h before behavioral tests 5 times every other day on days 1st, 3rd, 5th and 9th to induce migraine model (N = 50). As GBCAs, gadobenate dimeglumine (linear-ionic), Gadodiamide (linear-nonionic), and gadobutrol (macrocyclic-nonionic) were delivered intravenously through the tail vein of mice for 5 days on test days. Mechanical pain threshold (plantar and facial withdrawal threshold) was evaluated by plantar von Frey and periorbital von Frey tests on days 1st, 5th, and 9th, and thermal pain threshold (latency) was evaluated by hot plate and cold plate tests on days 3rd and 7th. There was a statistically significant increase in mechanical and thermal hyperalgesia in NTG administered groups compared to the control group. Gadodiamide, gadobutrol and gadobenate dimeglumine administration significantly decreased latency, paw and facial withdrawal threshold (0.18 ± 0.05, 0.17 ± 0.07, 0.16 ± 0.09; 9th day values respectively) compared to NTG group (0.27 ± 0.05). The results of this in vivo study show that GBCAs produce effects that may trigger migraine attacks in migraine. It is recommended that these effects be further investigated and supported by further clinical studies. [ABSTRACT FROM AUTHOR]

Published

2024

2. Effects of postoperative environmental noise on surgery induced pain: Evidence based on a prospective observational study.

Author

Ou, Wenjun, Tao, Chengkun, Zhang, Yang, Gan, Min, Xie, Yan, Wu, Yingcai, Zheng, Xuemei, Shu, Bin, Duan, Guangyou, and Xu, Fang

Subjects

*RISK assessment, *CESAREAN section, *SCIENTIFIC observation, *DESCRIPTIVE statistics, *SURGICAL complications, *LONGITUDINAL method, *ANALGESICS, *PAIN, *ENVIRONMENTAL exposure, *CONFIDENCE intervals

Abstract

Many patients recovering from surgery in wards are disturbed by environmental noise. However, the effects of environmental noise on postoperative pain are unclear. This study aimed to assess the association between postoperative noise and pain. This prospective study included 182 women who underwent cesarean sections. Postoperative noise was continuously recorded, and pain intensity at rest was assessed using a numerical rating scale (NRS) for 0–6, 6–12, 12–18, and 18–24 h after the patients were returned to the ward. Cumulative pain scores were calculated by summing the NRS scores at each time point and comprised the primary outcome. The maximum pain NRS score and analgesic consumption during the 24 h after surgery were also recorded. Mean environmental noise intensity during the daytime was an independent factor for cumulative pain scores, maximum pain scores, and analgesic use during the first postoperative 24 h (β, 0.37; 95% CI, 0.21–0.53 and β, 0.12; 95% CI, 0.07–0.17; P < 0.001 for both; β, 0.86; 95% CI, 0.25–1.46; P = 0.006). Cumulative and maximum NRS pain scores as well as the incidence of NRS ≥ 4 were significantly higher in patients under mean daytime environmental noise of ≥58, than <58 decibels (dB) (8.0 [6.0–11.3] vs. 6.0 (5.0–7.0); 3.0 [2.0–4.0] vs. 2.0 [2.0–2.0, and 25.6% vs. 11.0%; RR, 2.32; 95% CI, 1.19–4.54, respectively; P < 0.001 for all). Higher-level postoperative noise exposure was associated with more severe postoperative pain and increased analgesic needs, as well as a higher incidence of moderate-to-severe pain in patients recovering from cesarean delivery. Our findings indicate that reducing environmental ward noise might benefit for postoperative pain management. CD, cesarean delivery; PCIA, patient-controlled intravenous analgesia; BMI, body mass index; dB, decibel; NRS, number rating scale. [Display omitted] • We explored whether noise affects pain induced by surgery in patients receiving from cesarean delivery. • We found that higher-level postoperative noise correlated with more severe postoperative pain in patients undergoing cesarean delivery. • Given the affordability and safety of noise reduction measures, proactive steps to reduce noise pollution within patient wards is crucial. [ABSTRACT FROM AUTHOR]

Published

2024

3. Microglial Nrf2/HO-1 signaling gates remifentanil-induced hyperalgesia via suppressing TRPV4-mediated M1 polarization.

Author

Liu, Xiaowen, Cai, Huamei, Peng, Liang, Ma, Hongli, Yan, Yun, Li, Weixia, and Zhao, Jing

Subjects

*REMIFENTANIL, *HYPERALGESIA, *MICROGLIA, *TRPV cation channels, *SPINAL cord, *DEXMEDETOMIDINE

Abstract

Remifentanil-induced hyperalgesia (RIH) represents a significant clinical challenge due to the widespread use of opioids in pain management. However, the molecular and cellular mechanisms underlying RIH remain elusive. This study aimed to unravel the role of spinal cord microglia, focusing on the Nrf2/HO-1 signaling pathway and TRPV4 channels in the development of RIH. We used both in vivo and in vitro models to investigate the activation state of spinal cord microglia, the expression of TRPV4 channels, and the modulation of the Nrf2/HO-1 pathway under remifentanil exposure. In addition, we evaluated the potential therapeutic effects of dexmedetomidine, a perioperative α2-adrenergic agonist, on RIH and its related molecular pathways. Our results revealed a prominent role of spinal cord microglia in RIH, demonstrating an apparent microglial M1 polarization and increased TRPV4 channel expression. A notable observation was the downregulation of the Nrf2/HO-1 pathway, which was associated with increased neuroinflammation and mechanical allodynia. By upregulating or overexpressing Nrf2, we confirmed its ability to inhibit TRPV4 and thereby attenuate RIH-associated mechanical allodynia, M1 polarization, and neuroinflammation. Encouragingly, dexmedetomidine demonstrated therapeutic potential by positively modulating the Nrf2-TRPV4 nexus, attenuating mechanical allodynia, and reducing microglial inflammation. Our research highlights the critical role of spinal cord microglia in RIH mediated by the Nrf2-TRPV4 axis. The ability of dexmedetomidine to modulate this axis suggests its potential as an adjunctive therapy to remifentanil in mitigating RIH. Further studies are imperative to explore the broader implications and practical applicability of our findings. [Display omitted] • TRPV4 mediates spinal dorsal horn microglia M1 polarization and remifentanil-induced hyperalgesia (RIH). • Nrf2 regulates microglia M1 polarization via suppressing TRPV4 in vitro and in vivo. • Nrf2 gates RIH via suppressing TRPV4-related microglia neuroinflammation. • Targeting Nrf2-TRPV4 axis serves as promising strategy for RIH management. • Dexmedetomidine alleviated RIH via regulating microglial Nrf2-TRPV4 axis. [ABSTRACT FROM AUTHOR]

Published

2024

4. Activation of Transient Receptor Potential Vanilloid 1 Is Involved in Both Pain and Tumor Growth in a Mouse Model of Cancer Pain.

Author

Yoshida, Akari, Nishibata, Masayuki, Maruyama, Tomoyuki, Sunami, Shogo, Isono, Kyoichi, and Kawamata, Tomoyuki

Subjects

*CANCER pain, *TUMOR growth, *LABORATORY mice, *CALCITONIN gene-related peptide, *CYCLIC adenylic acid, *TRPV cation channels

Abstract

• Activation of CGRP-positive (+) sensory neurons is crucial for tumor growth. • However, how CGRP (+) sensory neurons are activated requires elucidation. • TRPV1 contributes to activation of CGRP (+) sensory neurons as well as cancer pain. • TRPV1 can be a target for new treatments for cancer pain and cancer development. Activation of calcitonin gene-related peptide (CGRP)-positive sensory neurons in the tumor microenvironment has been shown to be involved in tumor growth. However, how CGRP-positive sensory neurons are activated requires elucidation. In this study, we focused on transient receptor potential vanilloid 1 (TRPV1) and examined the contribution of TRPV1 to tumor growth and cancer pain in a mouse cancer model in which Lewis lung carcinoma was subcutaneously inoculated in the left plantar region. Tumor inoculation gradually increased the volumes of the hind paws of wild type (WT) mice over time, but those of both αCGRP knockout mice and TRPV1 knockout mice were significantly smaller than those of WT mice after tumor inoculation. Both TRPV1 and CGRP are therefore suggested to be involved in tumor growth. In an immunohistochemical study, the percentage of phosphorylated cyclic adenosine monophosphate response element-binding protein (p-CREB)-positive profiles in CGRP-positive dorsal root ganglion (DRG) neurons in WT mice was significantly increased after tumor inoculation. The percentage of p-CREB-positive profiles in CGRP-positive DRG neurons in TRPV1 knockout mice was also increased after tumor inoculation, but was significantly lower than that in WT mice, indicating the contribution of TRPV1 to activation of CGRP-positive DRG neurons. Cancer pain in TRPV1 knockout mice was significantly lower than that in WT mice. In conclusion, TRPV1 is involved in both tumor growth and cancer pain, potentially leading to a novel strategy for the treatment of cancer pain and cancer development. Cancer pain is also suggested to facilitate tumor growth. [ABSTRACT FROM AUTHOR]

Published

2024

5. Adolescent Alcohol Exposure Produces Sex-Specific Long-term Hyperalgesia via Changes in Central Amygdala Circuit Function.

Author

Secci, Maria E., Kelley, Leslie K., Avegno, Elizabeth M., Holmgren, Eleanor B., Chen, Lily, Rein, Sydney L., Engi, Sheila A., Quinlan, Virginia, Wilson, Lisa, Gilpin, Nicholas W., and Wills, Tiffany A.

Subjects

*AMYGDALOID body, *UNDERAGE drinking, *ALCOHOL drinking, *DRINKING behavior, *TEENAGERS, *HYPERALGESIA

Abstract

Exposure to alcohol during adolescence produces many effects that last well into adulthood. Acute alcohol use is analgesic, and people living with pain report drinking alcohol to reduce pain, but chronic alcohol use produces increases in pain sensitivity. We tested the acute and lasting effects of chronic adolescent intermittent ethanol (AIE) exposure on pain-related behavioral and brain changes in male and female rats. We also tested the long-term effects of AIE on synaptic transmission in midbrain (ventrolateral periaqueductal gray [vlPAG])-projecting central amygdala (CeA) neurons using whole-cell electrophysiology. Finally, we used circuit-based approaches (DREADDs [designer receptors exclusively activated by designer drugs]) to test the role of vlPAG-projecting CeA neurons in mediating AIE effects on pain-related outcomes. AIE produced long-lasting hyperalgesia in male, but not female, rats. Similarly, AIE led to a reduction in synaptic strength of medial CeA cells that project to the vlPAG in male, but not female, rats. Challenge with an acute painful stimulus (i.e., formalin) in adulthood produced expected increases in pain reactivity, and this effect was exaggerated in male rats with a history of AIE. Finally, CeA-vlPAG circuit activation rescued AIE-induced hypersensitivity in male rats. Our findings are the first, to our knowledge, to show long-lasting sex-dependent effects of adolescent alcohol exposure on pain-related behaviors and brain circuits in adult animals. This work has implications for understanding the long-term effects of underage alcohol drinking on pain-related behaviors in humans. [ABSTRACT FROM AUTHOR]

Published

2024

6. CWC22-Mediated Alternative Splicing of Spp1 Regulates Nociception in Inflammatory Pain.

Author

Song, Yu, Wang, Zhi-Yong, Luo, Jun, Han, Wen-Can, Wang, Xiao-Yi, Yin, Cui, Zhao, Wei-Nan, Hu, Su-Wan, Zhang, Qi, Li, Yan-Qiang, and Cao, Jun-Li

Subjects

*ALTERNATIVE RNA splicing, *CHRONIC pain, *NANOTECHNOLOGY, *GENOMICS, *HYPERALGESIA, *PROTEIN expression

Abstract

• The spliceosome-associated protein CWC22 of the spinal dorsal horn modulates nociception bidirectionally in mice; • Spp1 is a downstream gene of CWC22-mediated alternative splicing in inflammatory pain; • Spp1 splicing variants are variably regulated by CWC22, and Spp1 V4 is involved in nociception. Increasing evidence suggests that alternative splicing plays a critical role in pain, but its underlying mechanism remains elusive. Herein, we employed complete Freund's adjuvant (CFA) to induce inflammatory pain in mice. A combination of genomics research techniques, lentivirus-based genetic manipulations, behavioral tests, and molecular biological technologies confirmed that splicing factor Cwc22 mRNA and CWC22 protein were elevated in the spinal dorsal horn at 3 days after CFA injection. Knockdown of spinal CWC22 by lentivirus transfection (lenti-sh Cwc22) reversed CFA-induced thermal hyperalgesia and mechanical allodynia, whereas upregulation of spinal CWC22 (lenti- Cwc22) in naïve mice precipitated pain. Comprehensive transcriptome and genome analysis identified the secreted phosphoprotein 1 (Spp1) as a potential gene of CWC22-mediated alternative splicing, however, only Spp1 splicing variant 4 (Spp1 V4) was involved in thermal and mechanical nociceptive regulation. In conclusion, our findings demonstrate that spinal CWC22 regulates Spp1 V4 to participate in CFA-induced inflammatory pain. Blocking CWC22 or CWC22-mediated alternative splicing may provide a novel therapeutic target for the treatment of persistent inflammatory pain. [ABSTRACT FROM AUTHOR]

Published

2023

7. Modulation of the spinal N13 SEP component by high- and low-frequency electrical stimulation. Experimental pain models matter.

Author

Leone, C., Di Pietro, G., Salman, Y., Galosi, E., Di Stefano, G., Caspani, O., Garcia-Larrea, L., Mouraux, A., Treede, R.-D., and Truini, A.

Subjects

*ELECTRIC stimulation, *NEURAL stimulation, *SOMATOSENSORY evoked potentials, *ULNAR nerve, *HYPERALGESIA, *ELECTRICAL injuries

Abstract

• High and low frequency stimulation have a different effect on the N13 SEP component. • Dorsal horn excitability changes induced by low frequency stimulation can modulate the N13. • Different experimental models of central sensitization may induce dorsal horn excitability changes through different mechanisms. The N13 component of somatosensory evoked potential (N13 SEP) represents the segmental response of cervical dorsal horn neurons. Neurophysiological studies in healthy participants showed that capsaicin-induced central sensitization causes an increase of the N13 SEP amplitude. Consequently, in human research, this spinal component may serve as a valuable readout of central sensitization. In this study, we wanted to verify if the sensitivity of the N13 SEP for detecting central sensitization is consistent across different experimental pain models inducing central sensitization and secondary hyperalgesia, namely high and low-frequency electrical stimulation (HFS and LFS). In 18 healthy participants, we recorded SEP after bilateral ulnar nerve stimulation before and after secondary hyperalgesia was induced through HFS and LFS applied on the ulnar nerve territory of the hand of one side. The area of secondary hyperalgesia was mapped with a calibrated 128-mN pinprick probe, and the mechanical pain sensitivity with three calibrated 16–64-256-mN pinprick probes. Although both HFS and LFS successfully induced secondary hyperalgesia only LFS increased the amplitude of the N13 SEP. These findings suggest that the sensitivity of the N13 SEP for detecting dorsal horn excitability changes may critically depend on the different experimental pain models. Our results indicate that LFS and HFS could trigger central sensitization at the dorsal horn level through distinct mechanisms, however this still needs confirmation by replication studies. [ABSTRACT FROM AUTHOR]

Published

2023

8. Opioid infusions at different times of the day produce varying degrees of opioid-induced hyperalgesia.

Author

Shu, Bin, Liu, Huiting, Zheng, Xuemei, He, Jianrong, Wu, Yingcai, Chen, Jie, Chen, Yuanjing, Tian, Hongni, Ju, Dapeng, Huang, He, and Duan, Guangyou

Subjects

*HYPERALGESIA, *ANIMAL experimentation, *SPRAGUE Dawley rats, *REMIFENTANIL, *LABORATORY rats

Abstract

Opioids are metabolised by enzymes the activities of which vary with the circadian rhythm. We examined whether opioid infusions administered at different times of the day produce varying degrees of opioid-induced hyperalgesia (OIH) in animal experiments and clinical studies. Male Sprague–Dawley rats received remifentanil infusions (1 μg kg−1·min−1 for 1 h) at Zeitgeber times (ZT) 0, 4, 8, 12, 16, or 20 h. Rhythmicity of mechanical hypersensitivity was assayed after the infusion. Mechanical hypersensitivity, drug concentration, and metabolic enzyme activity of Wistar rats that received sufentanil (10 μg kg−1; four consecutive i.p. injections at 15-min intervals) or remifentanil infusion at ZT0 or ZT8 were assayed. Sixty patients who underwent abdominal laparoscopic surgery under general anaesthesia received remifentanil infusion (0.15 μg kg−1 min−1) and sufentanil injection (0.2 μg kg−1) at induction and skin incision, respectively. Postoperative pressure pain sensitivity, pain Numeric Rating Scale (NRS), drug concentrations, and nonspecific esterase activity were assessed. Sprague–Dawley rats that received remifentanil infusion exhibited a robust rhythmic paw withdrawal threshold (JTK_CYCLE: P =0.001, Q=0.001, Phase=26). Wistar rats infused with remifentanil or sufentanil at ZT8 exhibited greater OIH (P <0.001) than those infused at ZT0, with higher blood concentrations (P <0.001) and lower metabolic enzyme activities (P =0.026 and P =0.028, respectively). Patients in the afternoon group exhibited higher pressure pain sensitivity at forearm (P =0.002), higher NRS (P <0.05), higher drug concentrations (sufentanil: P =0.037, remifentanil: P =0.005), and lower nonspecific esterase activity (P =0.024) than the morning group. Opioid infusions administered at different times of day produced varying degrees of OIH, possibly related to circadian rhythms of metabolic enzyme activities. NCT 05234697. [ABSTRACT FROM AUTHOR]

Published

2023

9. Nerve terminals in the tumor microenvironment as targets for local infiltration analgesia.

Author

Madhusudanan, Pallavi, Jerard, Chinnu, Raju, Gayathri, Katiyar, Neeraj, and Shankarappa, Sahadev A.

Abstract

Nerve terminals within the tumor microenvironment as potential pain-mitigating targets for local infiltration analgesia is relatively less explored. In this study, we examine the role of key analgesics administered as local infiltration analgesia in a model of cancer-induced bone pain (CIBP). CIBP was induced by administration of allogenic MRMT1 breast cancer cells in the proximal tibia of rats, and tumor mass characterized using radiogram, micro-CT, and histological analysis. In vitro responsiveness to key analgesics δ-opioid receptor agonist (DOPr), Ca2+ channel and TRPV1 antagonists was assessed using ratiometric Ca2+ imaging in sensory neurons innervating the tumor site. Effectiveness of locally infiltrated analgesics administered independently or in combination was assessed by quantifying evoked limb withdrawal thresholds at two distinct sites for up to 14 days. CIBP animals demonstrated DOPr, N-, and L -type and TRPV1 expression in lumbar dorsal root ganglion neurons (DRG), comparable to controls. Evoked Ca2+ transients in DRG neurons from CIBP animals were significantly reduced in response to treatment with compounds targeting DOPr, N-, L -type Ca2+ channels and TRPV1 proteins. Behaviourally, evoked hyperalgesia at the tumor site was strongly mitigated by peritumoral injection of the DOPr agonist and T-type calcium antagonist, via its activity on bone afferents. Results from this study suggest that nerve terminals at tumor site could be utilized as targets for specific analgesics, using local infiltration analgesia. • Peripheral nerve terminals in tumours are good targets for local infiltration analgesia. • Cell bodies of neurons innervating bone tumor have higher calcium concentration and respond to common analgesics. • Delta opioid agonists can us utilized in local infiltration analgesia for mitigating tumor-induced pain. [ABSTRACT FROM AUTHOR]

Published

2023

10. TRPV1 and TRPA1 channels interact to mediate cold hyperalgesia in mice.

Author

Wang, Changming, Jin, Xiang, Zhang, Qing, Wang, Hanwen, Ji, Haiwang, Zhou, Yuan, Zhu, Chan, Yang, Yan, Yu, Guang, and Tang, Zongxiang

Subjects

*TRPV cation channels, *HYPERALGESIA, *MICE

Published

2023

11. A Deep-Learning Driven Investigation of the Circuit Basis for Reflexive Hypersensitivity to Thermal Pain.

Author

Reddy, Prannay, Vasudeva, Jayesh, Shah, Devanshi, Prajapati, Jagat Narayan, Harikumar, Nikhila, and Barik, Arnab

Subjects

*ANIMAL behavior, *ALLERGIES, *COMPUTER vision, *NEURAL circuitry, *BEHAVIORAL assessment, *THERMAL tolerance (Physiology), *PAIN threshold, *NEURAL codes

Abstract

• Analytical pipeline to automatically analyze rodent behavior on thermal-plate test. • Behavioral changes in mice with hyperalgesia. • Role of Tacr1 expressing neurons in the PBN contribute to thermal hyperalgesia. • Novel behavioral assay to test learning induced by noxious somatosensory stimuli. Objectively measuring animal behavior is vital to understanding the neural circuits underlying pain. Recent progress in machine vision has presented unprecedented scope in behavioral analysis. Here, we apply DeepLabCut (DLC) to dissect mouse behavior on the thermal-plate test — a commonly used paradigm to ascertain supraspinal contributions to noxious thermal sensation and pain hypersensitivity. We determine the signature characteristics of the pattern of mouse movement and posture in 3D in response to a range of temperatures from innocuous to noxious on the thermal-plate test. Next, we test how acute chemical and chronic inflammatory injuries sensitize mouse behaviors. Repeated exposure to noxious temperatures on the thermal plate can induce learning. In this study, we design a novel assay and formulate an analytical pipeline to facilitate the dissection of plasticity mechanisms in pain circuits in the brain. Last, we record and test how activating Tacr1 expressing PBN neurons (PBNTacr1) — a population responsive to sustained noxious stimuli- affects mouse behavior on the thermal plate test. Taken together, we demonstrate that by tracking a single body part of a mouse, we can reveal the behavioral signatures of mice exposed to noxious surface temperatures, report the alterations of the same when injured, and determine if a molecularly and anatomically defined pain-responsive circuit plays a role in the reflexive hypersensitivity to thermal pain. [ABSTRACT FROM AUTHOR]

Published

2023

12. Descending Facilitation of Nociceptive Transmission From the Rostral Ventromedial Medulla Contributes to Hyperalgesia in Mice with Sickle Cell Disease.

Author

Rogness, Victoria M., Juliette, Joseph, Khasabova, Iryna A., Gupta, Kalpna, Khasabov, Sergey G., and Simone, Donald A.

Subjects

*SICKLE cell anemia, *HYPERALGESIA, *MICE, *SPINAL cord

Abstract

• Hyperalgesia in mice with SCD is mediated by sensitization of spinal neurons. • We determined if the RVM contributes to hyperalgesia in sickle mice. • Blockade of the RVM with lidocaine attenuated hyperalgesia in sickle mice. • Electrophysiology showed that ON cells in the RVM of sickle mice were sensitized. • Sensitization of ON cells in the RVM contributes to hyperalgesia in sickle mice. Sickle cell disease (SCD) is an inherited blood disorder that is associated with acute episodic and chronic pain. Mice with SCD have robust hyperalgesia mediated, in part, by sensitization of spinal dorsal horn neurons. However, underlying mechanisms are not fully understood. Since the rostral ventromedial medulla (RVM) is a major component of descending circuitry that modulates nociceptive transmission in the spinal cord, we examined if the RVM contributes to hyperalgesia in mice with SCD. Injection of lidocaine, but not vehicle, into the RVM eliminated mechanical and heat hyperalgesia in sickle (HbSS-BERK) mice without altering mechanical and heat sensitivity in naïve C57B mice. These data indicate that the RVM contributes to the maintenance of hyperalgesia in mice with SCD. In electrophysiological studies, we determined the changes in response properties of RVM neurons that might contribute to hyperalgesia in sickle mice. Recordings were made from single ON, OFF, and Neutral cells in the RVM of sickle and control (HbAA-BERK) mice. Spontaneous activity and responses of ON, OFF and Neutral cells evoked by heat (50 °C) and mechanical (26 g) stimuli applied to the hind paw were compared between sickle and control mice. Although there were no differences in the proportions of functionally-identified neurons or spontaneous activity between sickle and control mice, evoked responses of ON cells to heat and mechanical stimuli were increased approximately 3-fold in sickle mice as compared to control mice. Thus, the RVM contributes to hyperalgesia in sickle mice via a specific ON cell-dependent descending facilitation of nociceptive transmission. [ABSTRACT FROM AUTHOR]

Published

2023

13. PAG neuronal NMDARs activation mediated morphine-induced hyperalgesia by HMGB1-TLR4 dependent microglial inflammation.

Author

Mo, Jingjing, Lu, Zijing, Peng, Jialing, Li, Xiang-pen, Lan, Lihuan, Wang, Hongxuan, and Peng, Ying

Subjects

*FRACTALKINE, *MYELOID differentiation factor 88, *NF-kappa B, *MICROGLIA, *METHYL aspartate receptors, *HYPERALGESIA, *GLUTAMATE receptors

Abstract

Morphine is one of the most effective and widely used analgesic drugs. However, chronic morphine use caused opioid-induced hyperalgesia (OIH). The development of OIH limits the use of morphine. The mechanisms of OIH are not fully understood. Toll-like receptor4 (TLR4) and glutamate receptors in the periaqueductal gray (PAG) are critical in OIH, however, the association between TLR4 and N-methyl-D-aspartate Receptors (NMDARs) activation in PAG remains unclear. Microglia activation, increased TLR4/p65 nuclear factor-kappa B (p65 NF-κB) and proinflammatory cytokines in microglia, and phosphorylation of NMDAR1 subunit (NR1) and NMDAR2B subunit (NR2B) in neurons were observed in PAG of OIH mice. Up-regulations of TLR4/p65 NF-κB and proinflammatory cytokines (IL-1β, IL-6, TNF-α) in BV2 cells were prevented by inhibiting and knocking down TLR4. By inhibiting myeloid differentiation factor 2 (MD2) and knocking down the High-mobility group box 1 (HMGB1), we found that morphine activated TLR4 by HMGB1 but not MD2. We co-cultured Neuro- 2a (N2A) with BV2 microglial cell line and found that instead of directly phosphorylating NMDAR subunits, morphine increased the phosphorylation of NR1 and NR2B by inducing TLR4-mediated microglia inflammation. Knocking TLR4 out of PAG by Lentivirus-GFP-TLR4 shRNA reversed these changes and relieved OIH. Our findings suggested that the secretion of HMGB1 induced by morphine-activated TLR4 in microglia, and the proinflammatory factors released by activated microglia phosphorylated NR1 and NR2B of adjacent neurons, induced increased neuronal excitability. In conclusion, TLR4/NMDARs in PAG were involved in the development and maintenance of OIH and supported novel strategies for OIH treatment. [ABSTRACT FROM AUTHOR]

Published

2023

14. MMG22 Potently Blocks Hyperalgesia in Cisplatin-treated Mice.

Author

Cataldo, Giuseppe, Lunzer, Mary M., Akgün, Eyup, Wong, Henry L., Portoghese, Philip S., and Simone, Donald A.

Subjects

*HYPERALGESIA, *NEURALGIA, *MICE, *NERVOUS system injuries, *EXPERIMENTAL arthritis, *PAIN management, *VISCERAL pain

Abstract

• The bivalent ligand MMG22 consists of a MOR agonist and mGluR5 antagonist. • MMG22 reduced mechanical hyperalgesia produced by cisplatin in mice. • MMG22 reduced hyperalgesia without tolerance. • MMG22 may produce antinociception through the formation of a MOR-mGluR5 heteromer. MMG22 is a bivalent ligand containing MOR agonist and mGluR5 antagonist pharmacophores connected by a 22-atom linker. Intrathecal (i.t.) administration of MMG22 to inflamed mice has been reported to produce fmol-range antinociception in the reversal of LPS-induced hyperalgesia. MMG22 reduced hyperalgesia in the spared nerve injury (SNI) model of neuropathic pain at 10 days after injury but not at 30 days after injury, perhaps related to the inflammation that occurs early after injury but subsequently subsides. The present study determined the efficacy of MMG22 in cisplatin-treated male mice in order to provide data relating to the efficacy of MMG22 in the treatment of neuropathic pain that is associated with inflammation. Groups of eight mice each received daily intraperitoneal (i.p.) injections of cisplatin for seven days to produce robust mechanical allodynia defined by the decrease in withdrawal threshold using an electronic von Frey applied to the plantar surface of the hind paw. Intrathecal administration of MMG22 potently reduced mechanical hyperalgesia (ED 50 0.04 fmol/mouse) without tolerance, whereas MMG10 was essentially inactive. Morphine was less potent than MMG22 by >5-orders of magnitude and displayed tolerance. Subcutaneous MMG22 was effective (ED 50 = 2.41 mg/kg) and devoid of chronic tolerance. We propose that MMG22 induces the formation of a MOR-mGluR5 heteromer through selective interaction with the upregulated NR2B subunit of activated NMDAR, in view of the 4600-fold reduction of i.t. MMG22 antinociception by the selective NR2B antagonist, Ro25-6981. A possible explanation for the substantially reduced potency for MMG22 in the SNI model is discussed. [ABSTRACT FROM AUTHOR]

Published

2023

15. A novel suppressor of Piezo2 in rodent nociceptors.

Author

West, Aaron Keith and Schneider, Eve Rebecca

Subjects

*NOCICEPTORS, *RODENTS, *HYPERALGESIA, *ALLODYNIA, *FAMILIES

Abstract

Members of both the Piezo and transmembrane channel-like (TMC) families are bona fide mammalian mechanotransducers. In a recent study, Zhang, Shao et al. discovered that TMC7, a non-mechanosensitive TMC, inhibits Piezo2-dependent mechanosensation, with implications for the importance of cellular context for Piezo2 channels in normal and pathological responses to mechanical pain. [ABSTRACT FROM AUTHOR]

Published

2024

16. CYP1B1-derived epoxides modulate the TRPA1 channel in chronic pain.

Author

Sun, Lili, Zhang, Jie, Niu, Changshan, Deering-Rice, Cassandra E., Hughen, Ronald W., Lamb, John G., Rose, Katherine, Chase, Kevin M., Almestica-Roberts, Marysol, Walter, Markel, Schmidt, Eric W., Light, Alan R., Olivera, Baldomero M., and Reilly, Christopher A.

Subjects

CHRONIC pain, EPOXY compounds, DORSAL root ganglia, SPINAL nerves, ANALGESIA

Abstract

Pain is often debilitating, and current treatments are neither universally efficacious nor without risks. Transient receptor potential (TRP) ion channels offer alternative targets for pain relief, but little is known about the regulation or identities of endogenous TRP ligands that affect inflammation and pain. Here, transcriptomic and targeted lipidomic analysis of damaged tissue from the mouse spinal nerve ligation (SNL)-induced chronic pain model revealed a time-dependent increase in Cyp1b1 mRNA and a concurrent accumulation of 8,9-epoxyeicosatrienoic acid (EET) and 19,20-EpDPA post injury. Production of 8,9-EET and 19,20-EpDPA by human/mouse CYP1B1 was confirmed in vitro, and 8,9-EET and 19,20-EpDPA selectively and dose-dependently sensitized and activated TRPA1 in overexpressing HEK-293 cells and Trpa1 -expressing/AITC-responsive cultured mouse peptidergic dorsal root ganglia (DRG) neurons. TRPA1 activation by 8,9-EET and 19,20-EpDPA was attenuated by the antagonist A967079, and mouse TRPA1 was more responsive to 8,9-EET and 19,20-EpDPA than human TRPA1. This latter effect mapped to residues Y933, G939, and S921 of TRPA1. Intra-plantar injection of 19,20-EpDPA induced acute mechanical, but not thermal hypersensitivity in mice, which was also blocked by A967079. Similarly, Cyp1b1 -knockout mice displayed a reduced chronic pain phenotype following SNL injury. These data suggest that manipulation of the CYP1B1–oxylipin–TRPA1 axis might have therapeutic benefit. Targeting CYP1B1–Oxylipin–TRPA1 network may represent a novel treatment option for preventing chronic pain in patients. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

17. The nonopioid cholinergic agonist GTS-21 mitigates morphine-induced aggravation of burn injury pain together with inhibition of spinal microglia activation in young rats.

Author

Ren, Yang, Zhou, Yinhui, You, Zerong, Deng, Hao, Kem, William R., Mao, Jianren, Zhang, Wei, and Martyn, J.A. Jeevendra

Subjects

*NONOPIOID analgesics, *NF-kappa B, *MICROGLIA, *CANCER pain, *MYASTHENIA gravis, *NICOTINIC receptors, *PAIN threshold

Abstract

Background: Repetitive opioid use does not always alleviate basal pain, procedural pain, or both after burn injury. Mitigation of burn injury-site pain can be achieved by GTS-21 stimulation of α7-acetylcholine nicotinic receptors (α7AChRs) and reduced microglia activation in rat. We tested the hypothesis that morphine exaggerates burn injury-site pain and GTS-21 alleviates both morphine-induced aggravated burn injury pain and microglia activation.Methods: Young rats with dorsal paw burn injury or sham-burn received intraperitoneal saline, morphine, GTS-21, or a combination twice daily for 14 days. Ipsilateral plantar pain thresholds were tested every other day before morning drugs from days 0-20. Spinal microglia activation, evidenced as pain-transducer (tumour necrosis factor-α [TNF-α], interleukin [IL]-6, IL-1β, nuclear factor kappa B [NF-κB], Toll-like receptor 4 [TLR4]) expression, was examined using immunohistochemistry and immunoblot. In cultured microglia, morphine-induced cytokine expression was measured (quantitative polymerase chain reaction/enzyme-linked immunosorbent assay [qPCR/ELISA]).Results: Morphine aggravated allodynia at day 5 in sham-burn (P=0.039, n=8-11) but significantly aggravated burn injury site allodynia by day 3 (P=0.010, n=8-11). Microgliosis paralleled nociceptive behaviour changes where burn injury with morphine had highest microgliosis compared with burn injury, morphine alone, or controls (number of cells per field [SD]: 33.8 [2.4], 18.0 [4.1], 8.2 [1.9], and 4.8 [2.0], respectively; P<0.001, n=4-5]. GTS-21 reversed the morphine-induced pain component in sham-burn and burn injury rats together with reduced microgliosis and spinal pain-transducer expression (TNF-α, IL-6, IL-1β, NF-κB, and TLR4). Morphine-exposed microglial cells showed increased cytokine expression, which was mitigated by GTS-21.Conclusions: Morphine or burn injury alone increases pain together with microgliosis and pain-transducer expression. Morphine administration augments burn injury-site nociception sooner and aggravated spinal microgliosis and inflammatory pain-transducer expression. GTS-21 has the potential to treat morphine-induced pain in burn injury. [ABSTRACT FROM AUTHOR]

Published

2022

18. A multi-target ligand (JM-20) prevents morphine-induced hyperalgesia in naïve and neuropathic rats.

Author

Garrido-Suárez, Bárbara B., Garrido, Gabino, Bellma-Menéndez, Addis, Aparicio-López, Guillermo, Valdés-Martínez, Odalys, Morales-Aguiar, Ruth A., Fernández-Pérez, Miguel D., Ochoa-Rodríguez, Estael, Verdecia-Reyes, Yamila, and Delgado-Hernández, René

Subjects

*PATIENT compliance, *DRUG withdrawal symptoms, *SCIATIC nerve, *NEURALGIA, *SPRAGUE Dawley rats

Abstract

The present study examines the possible inhibitory effect of JM-20, a multi-target neuroprotective compound, on the development of morphine-induced hyperalgesia in Male Sprague-Dawley naïve rats. Additionally, the impact of JM-20 on chronic constriction injury (CCI) rats under chronic morphine exposure was investigated, and its efficacy in reducing mechanical hypersensitivity and histopathological changes in the sciatic nerve was assessed. JM-20 (20 mg/kg, per os [p.o.]), administered 60 min before morphine (10 mg/kg, s.c. twice daily at 12 h intervals) for ten days, significantly inhibited the development of morphine-induced hyperalgesia assessed using an electronic pressure-meter paw test, hot-plate, and formalin test, as well as the appearance of spontaneous withdrawal somatic symptoms in rats. Furthermore, JM-20 decreases spinal pro-inflammatory interleukin-1β and restores glutathione to close physiological concentrations, biomarkers directly related to the intensity of mechanical hypernociception. After CCI and sham surgery, co-treatment with JM-20 (10 mg/kg, p.o.) for five days decreased morphine increased-mechanical hypersensitivity, even 12 days after its discontinuation. Continued morphine treatment imposed a neuroinflammatory challenge in CCI animals, further increasing cellularity (>75% immune cell infiltration) with lymphocytes and macrophages. However, JM-20 co-treatment still reduced the presence of cellular infiltrates (51–75%) with a predominance of lymphocytes. Even in the absence of nerve injury, JM-20 attenuated the peripheral neuroinflammatory response observed in morphine-treated sham-operated animals (0% vs. 1–25%). These findings suggest that JM-20 could prevent morphine-induced hyperalgesia by anti-inflammatory and antioxidant mechanisms. [ABSTRACT FROM AUTHOR]

Published

2024

19. Ameliorative effects of probiotic Limosilactobacillus fermentum and Enterococcus lactis isolated from cameroonian traditionally processed milk and palm wine against chronic constriction injury induced neuropathic pain in mice.

Author

Ambe, Ngwa Fabrice, Bobga, Tanyi Pride, Toukam Tatsinkou, Liliane Laure, Sotoing Taiwe, Germain, and Fossi, Bertrand Tatsinkou

Subjects

*MILK microbiology, *NEURALGIA, *ENTEROCOCCUS, *BIOLOGICAL models, *ANTI-inflammatory agents, *MORPHINE, *TREATMENT effectiveness, *OXIDATIVE stress, *HYPERALGESIA, *PLANT extracts, *MICE, *RNA, *GENE expression, *LACTOBACILLUS, *ANIMAL experimentation, *ANTIOXIDANTS, *DRUG efficacy, *PROBIOTICS, *CULTURED milk, *CYTOKINES, *SEQUENCE analysis

Abstract

Fermented milk and palm wine are regularly used by several ethnic groups in Cameroon in traditional treatment rituals for infections, inflammatory, cardiovascular disorders, and even metabolic diseases such as diabetes, hypercholesterolemia etc. Reports from many studies have demonstrated that fermented milk and palm wine are potential sources of probiotic bacteria. However, the capacity of probiotics isolated from these natural sources to alleviate neuropathic pain has not been experimentally tested. This study aimed at investigating the ameliorative potential of lactic acid bacteria isolated from palm wine and traditional fermented cow milk on the chronic constriction injury (CCI) induced neuropathic pain in mice. Pour plating technique on De Man Rogasa (MRS) agar was utilised for isolation of lactic acid bacteria from fermented cow milk and palm wine, and identified using the 16S r RNA gene sequencing. Neuropathic pain was induced by chronic constriction injury of the sciatic nerve. These bacteria were orally administered at different concentrations to Balb/c mice by gavage for 14 consecutive days. Cold allodynia, mechanical hyperalgesia and exploratory behaviour were evaluated on day 0, 7th and 14th respectively. The total level of calcium, oxidative stress markers and myeloperoxidase were also quantified in the sciatic nerve homogenate. Cyclooxygenase-2(COX-2) and cytokine profile were determined from serum. Lactic acid bacteria were isolated from fermented cow milk and palm wine and two isolates were chosen according to their probiotic potentials and identified as strain of Limolactobacillus fermentum and Enterococcus lactis. Their 16 S rRNA gene sequences were deposited in NCBI genbank with accession number of OP896078 and OR619545, respectively. Pretreatment with Limosilactobacillus fermentum and Enterococcus lactis significantly alleviated mechanical hyperalgesia and cold allodynia with similar effect to the reference drug, morphine. These two isolates ameliorated CCI induced neuropathic pain by increasing antioxida776nts (GSH, CAT and SOD, P < 0.01) and decreasing pro-oxidants (MDA and NO, P < 0.01). Also, they inhibited the release of proinflammatory cytokines (IL-1β, TNF-α, IFN-γ, and IL-6; P < 0.01) and IL-10 level was significantly (P < 0.01) increased when compared to the negative control. Treatment with these bacteria significantly dropped the level of total calcium (P < 0.01), COX-2 (P < 0.01) and MPO (P < 0.01) when compared with the negative control. The neuroprotective potentials of these selected lactic acid bacteria against CCI induced neuropathic pain may be attributed to their anti-oxidant, anti-inflammatory properties and reduced calcium deposition in sciatic nerve. [Display omitted] • Fermented milk and palm wine are sources of lactic acid bacteria with probiotic potential. • Pretreatment with probiotic Limosilactobacillus fermentum and Enterococcus lactis significantly attenuated mechanical hyperalgesia and cold allodynia. • The neuroprotective potentials of Limosilactobacillus fermentum and Enterococcus lactis is associated to their anti-oxidant, anti-inflammatory properties. [ABSTRACT FROM AUTHOR]

Published

2024

20. The serotonin(5-HT)2A receptor is involved in the hypersensitivity of bladder afferent neurons in cyclophosphamide-induced cystitis.

Author

Chen, Xun, Lv, Rong, Li, Mingzhuo, Zhang, Lin, Sun, Yudong, Cao, Nailong, and Gu, Baojun

Subjects

*INTERSTITIAL cystitis, *LABORATORY rats, *SEROTONIN receptors, *TRPV cation channels, *CYSTITIS, *SEROTONIN

Abstract

Interstitial cystitis/bladder pain syndrome (IC/BPS) is a chronic bladder inflammation characterized by the main symptoms of urinary frequency, urgency, and pelvic pain. The hypersensitivity of bladder afferent neurons is considered a significant pathophysiologic mechanism in IC/PBS. Serotonin (5-HT, 5-hydroxytryptamine) receptors are known to be involved in the regulation of the micturition reflex and hyperalgesia, but the effect of 5-HT receptors on cystitis remains unknown. In this study, a rat model of interstitial cystitis induced by intraperitoneal injection of cyclophosphamide (CYP) was used to investigate the role of 5-HT receptors on cystitis. The histology and urodynamics exhibited chronic cystitis and overactive bladder in CYP-treated rats. Notably, among 5-HT1A, 5-HT2A and 5-HT7 receptors, the expression of 5-HT2A receptor was significantly increased in bladder afferent neurons in CYP-treated rats. Intrathecal administration of the 5-HT2A receptor antagonist M100907 could alleviate bladder overactivity and hyperalgesia in CYP-induced cystitis rats. Neuronal calcium imaging of bladder afferent neurons revealed increased calcium influx induced by the 5-HT2A receptor agonist or capsaicin in cystitis rats, which could be inhibited by M100907. Moreover, RNA sequencing indicated that differentially expressed genes were enriched in inflammation-related pathways and cellular calcium homeostasis. These findings suggest that the 5-HT2A receptor is involved in the hypersensitivity of bladder afferent neurons in CYP-induced cystitis, and M100907 could alleviate bladder overactivity and hyperalgesia in CYP-induced cystitis by inhibiting neuronal hypersensitivity in the afferent pathways. The 5-HT2A receptor may be a potential therapeutic target for the treatment of IC/BPS. • The expression of the 5-HT2A receptor was significantly upregulated in L6-S1 DRG in CYP-induced cystitis rats. • 5-HT2A receptor antagonist M100907 could alleviate bladder overactivity and hyperalgesia in cystitis rats. • M100907 inhibited calcium influx induced by capsaicin or the 5-HT2A receptor agonist in bladder afferent neurons. • RNA sequencing indicated that DEGs were enriched in inflammatory-related pathways and intracellular calcium homeostasis. [ABSTRACT FROM AUTHOR]

Published

2024

21. Chronic stress induces wide-spread hyperalgesia: The involvement of spinal CCK1 receptors.

Author

Li, Jia-Heng, Zhao, Shi-Jie, Guo, Yi, Chen, Fei, Traub, Richard J., Wei, Feng, and Cao, Dong-Yuan

Subjects

*PSYCHOLOGICAL stress, *IRRITABLE colon, *INTRATHECAL injections, *CHRONIC pain, *TEMPOROMANDIBULAR disorders

Abstract

Chronic primary pain (CPP) occurs in the absence of tissue injury and includes temporomandibular disorders (TMD), fibromyalgia syndrome (FMS) and irritable bowel syndrome (IBS). CPP is commonly considered a stress-related chronic pain and often presents as wide-spread pain or comorbid pain conditions in different regions of the body. However, whether prolonged stress can directly result in the development of CPP comorbidity remains unclear. In the present study, we adapted a 21 day heterotypic stress paradigm in mice and examined whether chronic stress induced wide-spread hyperalgesia, modeling comorbid CPP in the clinic. We found that chronic stress induced anxiety- and depression-like behaviors, and resulted in long-lasting wide-spread hyperalgesia over several body regions such as the orofacial area, hindpaw, thigh, upper back and abdomen in female mice. We further found that the expression of cholecystokinin (CCK) 1 receptors was significantly increased in the L4-L5 spinal dorsal horn of the female mice after 14 and 21 day heterotypic stress compared with the control animals. Intrathecal injection of the CCK 1 receptor antagonist CR-1505 blocked pain hypersensitivity in the subcervical body including the upper back, thigh, hindpaw and abdomen. These findings suggest that the upregulation of spinal CCK 1 receptors after chronic stress contributes to the central mechanisms underlying the development of wide-spread hyperalgesia, and may provide a potential and novel central target for clinical treatment of CPP. • Chronic stress models comorbid anxiety/depression like behaviors and pain. • Chronic heterotypic stress induces orofacial and wide-spread somatic hyperalgesia. • Chronic heterotypic stress induces visceral referred pain from the colon. • CCK 1 receptors in the spinal cord contribute to the wide-spread hyperalgesia. [ABSTRACT FROM AUTHOR]

Published

2024

22. Yangonin, one of the kavalactones isolated from Piper methysticum G. Forst, acts through cannabinoid 1 (CB1) receptors to induce an intrathecal anti-hyperalgesia.

Author

Chow, Lok-Hi, Lin, Pin-Chen, Chen, Ying-Jie, Chen, Yuan-Hao, and Huang, Eagle Yi-Kung

Subjects

*COMBINATION drug therapy, *ANTI-inflammatory agents, *SPINAL injections, *SCIATIC nerve, *PLANT roots, *NOCICEPTIVE pain, *LIGATURE (Surgery), *TREATMENT effectiveness, *PLANT extracts, *HYPERALGESIA, *RATS, *ANALGESIA, *POLYSACCHARIDES, *PAIN, *ANIMAL experimentation, *INFLAMMATION, *KAVA plant, *CANNABINOIDS, *CELL receptors, *ALLODYNIA

Abstract

Piper methysticum G. Forst (Piperaceae) is traditionally consumed in Polynesian culture. The roots are used to produce an entheogenic drink and traditional medicine with sedative and anxiolytic properties. There is also evidence that it functions as a pain reliever. Kavalactones, its main active ingredients, exhibit psychoactive effects on the central nervous system. However, the active ingredients and pharmacological mechanisms underlying the analgesic effect of kavalactones are unclear. This study investigated the effects of kavain and yangonin on nociception, inflammatory hyperalgesia, and neuropathic mechanical allodynia at the spinal level. Male Sprague–Dawley rats were administered kavain and yangonin (27.14 and 19.36 nmol/rat) via intrathecal injection. Tail-flick tests were performed to evaluate the anti-nociceptive properties. The efficacy of kavain and yangonin on inflammatory hyperalgesia was examined using a plantar test in rats with carrageenan-induced paw inflammation. The von Frey test was used to assess mechanical allodynia induced by partial sciatic nerve ligation. Intrathecal injection of yangonin demonstrated a relatively potent anti-nociceptive effect and attenuated carrageenan-induced hyperalgesia. These effects were completely reversed by the co-administration of PF 514273, a cannabinoid 1 (CB 1) receptor antagonist. However, yangonin did not affect mechanical allodynia at the spinal level. Kavain, another abundant kavalactone, did not affect nociception, hyperalgesia, or mechanical allodynia at the spinal level. Overall, our study demonstrated that yangonin exerts anti-nociception and anti-inflammatory hyperalgesia effects via CB 1 receptors at the spinal level. We identified a single kavalactone, yangonin, extracted from kava as a promising treatment for pain. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

23. Inflammatory injury induces pain sensitization that is expressed beyond the site of injury in male (and not in female) mice.

Author

Baumbach, Jennet L., Leonetti, Amanda M., and Martin, Loren J.

Subjects

*ELECTRIC stimulation, *SOFT tissue injuries, *HYPERALGESIA, *PHENOTYPES, *MICE, *ELECTRICAL injuries

Abstract

Pain is a crucial protective mechanism for the body. It alerts us to potential tissue damage or injury and promotes the avoidance of harmful stimuli. Injury-induced inflammation and tissue damage lead to pain sensitization, which amplifies responses to subsequent noxious stimuli even after an initial primary injury has recovered. This phenomenon, commonly referred to as hyperalgesic priming, was investigated in male and female mice to determine whether it is specific to the site of previous injury. We used 10 μ l of 50 % Freund's complete adjuvant (CFA) administered to the left hind paw as a model of peripheral injury. Both male and female mice exhibited robust site-specific mechanical hypersensitivity after CFA, which resolved within one-week post-injection. After injury resolution, only male CFA-primed mice showed enhanced and prolonged mechanical sensitivity in response to a chemical challenge or a single 0.5 mA electric footshock. Among CFA-primed male mice, shock-induced mechanical hypersensitivity was expressed in both the left (previously injured) and the right (uninjured) hind paws, suggesting a pivotal role for altered centralized processes in the expression of pain sensitization. These findings indicate that pain history regulates sensory responses to subsequent mechanical and chemical pain stimuli in a sex-specific manner—foot-shock-induced hyperalgesic priming expression among male mice generalized beyond the initial injury site. [Display omitted] • Mice exhibit sex-specific homecage phenotypes before and after CFA injection. • Male mice express pain sensitization after resolution of CFA injury. • Females did not express pain sensitization after resolution of CFA injury. • In males, electrical stimulation (footshock) elicited expression of sensitization. • Among males, footshock caused expression of sensitization in both hindpaws. [ABSTRACT FROM AUTHOR]

Published

2024

24. Corrigendum to "Valproate attenuates somatic hyperalgesia induced by orofacial inflammation combined with stress through inhibiting spinal IL-6 and STAT1 phosphorylation" [Brain Res. Bull. 208 (2024) 110889].

Author

Xu, Chen-Xi, Qiu, Xin-Yi, Guo, Yi, Xu, Tian-Ming, Traub, Richard J., Feng, Hai-Nan, and Cao, Dong-Yuan

Subjects

*STAT proteins, *VALPROIC acid, *INTERLEUKIN-6, *HYPERALGESIA, *PHOSPHORYLATION

Published

2024

25. Prazosin as an Adjuvant to Increase Effectiveness of Duloxetine in a Rat Model of Oxaliplatin-Induced Peripheral Neuropathy.

Author

Wagner, Monica A., Smith, Ellen M. Lavoie, Ayyash, Naji, and Holden, Janean E.

Abstract

Duloxetine, the only American Society of Clinical Oncology (ASCO) treatment recommended for chemotherapy-induced peripheral neuropathy (CIPN) in cancer survivors, is not effective for 40% of survivors. This study examined the ability of a duloxetine-prazosin combination to prevent the development of allodynia and hyperalgesia in a rat model of oxaliplatin-induced peripheral neuropathy (OPIN). Female (n = 24) and male (n = 41) rats were started on duloxetine (15 mg), prazosin (2 mg), or a duloxetine-prazosin combination one week prior to administration of the chemotherapy drug, oxaliplatin, and continued the duloxetine-prazosin combination for 32 days. Behavioral testing for mechanical allodynia and mechanical hyperalgesia was done with selected von Frey filaments over the course of the study. Overall percent paw withdrawal for rats that received the duloxetine-prazosin combination was significantly lower in female (p <.001 for both conditions) and male (p =.029 for allodynia; p <.001 for hyperalgesia) than those that received water. No significant posttreatment differences were found for allodynia or hyperalgesia between rats treated with duloxetine and rats that received the duloxetine-prazosin combination in either sex. These finding provide preliminary evidence that a duloxetine-prazosin combination can prevent the posttreatment development of allodynia and hyperalgesia in both male and female rats; however, the results suggest that the duloxetine-prazosin combination is no more efficacious than duloxetine alone in preventing chronic OIPN. The profession of nursing is built on clinical practice supported by scientific research. The current study addressed the clinical practice problem of prevention and management of painful OIPN, which is a priority area in oncology nursing. [ABSTRACT FROM AUTHOR]

Published

2024

26. Purpurin ameliorated neuropathic allodynia and hyperalgesia by modulating neuronal mitochondrial bioenergetics and redox status in type 1 diabetic mice.

Author

Chen, Wei, Wu, Jia-Yi, Fan, You-Ya, Li, Ben-Ling, Yuan, Hong-Bin, and Zhao, Xin

Subjects

*HYPERALGESIA, *BIOENERGETICS, *DORSAL root ganglia, *TYPE 1 diabetes, *ALLODYNIA, *PERIPHERAL nervous system

Abstract

A substantial proportion of diabetic patients suffer a debilitating and persistent pain state, known as peripheral painful neuropathy that necessitates improved therapy or antidote. Purpurin, a natural anthraquinone compound from Rubia tinctorum L., has been reported to possess antidepressant activity in preclinical studies. As antidepressants have been typically used as standard agents against persistent neuropathic pain, this study aimed to probe the effect of purpurin on neuropathic pain associated with streptozotocin-induced type 1 diabetes in male C57BL6J mice. The Hargreaves test and the von Frey test were used to assess the pain-like behaviors, shown as heat hyperalgesia and mechanical allodynia respectively. Chronic treatment of diabetic mice with purpurin not only ameliorated the established symptoms of heat hyperalgesia and mechanical allodynia, but also arrested the development of these pain states given preemptively at low doses. Although purpurin treatment hardly impacted on metabolic disturbance in diabetic mice, it ameliorated exacerbated oxidative stress in pain-associated tissues, improved mitochondrial bioenergetics in dorsal root ganglion neurons and restored nerve conduction velocity in sciatic nerves. Notably, the analgesic actions of purpurin were modified by pharmacologically manipulating redox status and mitochondrial bioenergetics. These findings unveil the analgesic activity of purpurin, an effect that is causally associated with its bioenergetics-enhancing and antioxidant effects, in mice with type 1 diabetes. [ABSTRACT FROM AUTHOR]

Published

2024

27. Chemical compounds, anti-tumor and anti-neuropathic pain effect of hemp essential oil in vivo.

Author

Xu, Yunhui, Luo, Jiajia, Guo, Yuhan, Zhou, Jing, Shen, Longhai, Gu, Fenghua, Shi, Chenfeng, Yao, Lijuan, and Hua, Moli

Subjects

*VEGETABLE oils, *NEURALGIA, *ANTI-inflammatory agents, *T cells, *ESSENTIAL oils, *ANTINEOPLASTIC agents, *IN vivo studies, *ANALGESICS, *MICE, *FLOWERS, *HYPERALGESIA, *ANIMAL experimentation, *LUNG tumors, *LEAVES, *CYTOKINES, *DRUG development, *CANNABINOIDS

Abstract

Hemp (Cannabis sativa L.), an annual dioecious plant, has shown extensive application in the fields of fibers, food, oil, medicine, etc. Currently, most attention has been paid to the therapeutic properties of phytocannabinoids. However, the pharmaceutical research on essential oil from hemp is still lacking. In this study, hemp essential oil (HEO) was extracted from hemp flowers and leaves, and the components were analyzed by GC–MS. Quatitative analysis of three main compounds β-caryophyllene, β-caryophyllene oxide, α -humulene were determined by GC-FID. The anti-tumor and anti-neuropathic pain effects of HEO were evaluated. In the paclitaxel induced neuropathic mice model, HEO reduced the serum level of inflammatory cytokines TNF-α to achieve the analgesic effect, which was tested by evaluating mechanical and thermal hyperalgesia. Further investigation with cannabinoid receptor 2 (CB2 R) antagonist AM630 revealed the mechanism of reversing mechanical hyperalgesia may be related to CB2 R. In Lewis lung cancer grafted mice model, the tumor growth was significantly inhibited, the levels of tumor inflammatory cytokines TNF-α and IL-6 were downregulated, immune organ index was modified and immune-related CD4+, CD8+ T lymphocytes level, CD4+/CD8+ ratio were increased when administered with HEO. These results reveal that HEO plays a role not only in tumor chemotherapy induced peripheral neuropathy treatment, but also in anti-tumor treatment which offers key information for new strategies in cancer treatment and provides reference for the medicinal development of hemp. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

28. Sympathetic skin response as an objective tool to estimate stimulus-associated arousal in a human model of hyperalgesia.

Author

Salameh, Charbel, Perchet, Caroline, Hagiwara, Koichi, and Garcia-Larrea, Luis

Subjects

*HYPERALGESIA, *MICROSATELLITE repeats, *HABITUATION (Neuropsychology), *COGNITION disorders

Abstract

Pain is a private experience, whose assessment relies on subjective self-reporting. Inaccurate communication renders pain evaluation unreliable in individuals with alteration of consciousness, lack of verbal interaction, cognitive dysfunction or simple malingering, hence the importance of developing reliable objective assessment tools. Since pain is associated with autonomic arousal, here we used readouts of autonomic activity to assess objectively the arousing effect of somatic stimuli in a human model of hyperalgesia. We used topical capsaicin to induce cutaneous hypersensitivity in the right arm of 20 healthy volunteers, and recorded sympathetic skin responses (SSR) and numerical perceptive ratings (NRS) to stimulation of the sensitized region and its homologous contralateral site, using brush (Aβ), pinprick (Aδ) and laser (C-Warmth) stimuli. Both subjective ratings and SSRs were significantly enhanced to stimulation of the sensitized region, and their respective ratios of maximal enhancement were positively correlated. At individual level, a significant association was observed between SSR and NRS behavior (χ2(1)= 11.03; p < 0.001), with a positive predictive value of 87% (CI95 [77-97%]) for SSR increase predicting enhancement of subjective reports. A "lie experiment" asking subjects to simulate elevated NRS failed to enhance SSRs. Significant habituation of SSRs appeared when stimuli were repeated at ∼15s intervals, hence decreasing their negative predictive value when several consecutive stimuli were averaged (NPV=46%; CI95 [30-62%]). The SSR may represent a rapid and reliable procedure to assess cutaneous hypersensitivity, simple to use in clinical practice and resistant to simulation. Rapid habituation is a drawback that can be countered by using few repetitions and low stimulus rates. [ABSTRACT FROM AUTHOR]

Published

2022

29. Dual orexin receptor antagonist drug suvorexant can help in amelioration of predictable chronic mild stress-induced hyperalgesia.

Author

Chavan, Parimal, Chikahisa, Sachiko, Shiuchi, Tetsuya, Shimizu, Noriyuki, Dalanon, Junhel, Okura, Kazuo, Séi, Hiroyoshi, and Matsuka, Yoshizo

Subjects

*DRUG receptors, *HYPERALGESIA, *ENDOTHELIN receptors, *PSYCHOLOGICAL stress, *INTRAPERITONEAL injections, *LABORATORY mice, *CATAPLEXY, *VISCERAL pain

Abstract

This study aimed to evaluate the involvement of the orexin system in predictable chronic mild stress (PCMS) and the effects of suvorexant, a dual orexin receptor antagonist, on nociceptive behavior in PCMS. Male C57BL/6 J mice were separated into various PCMS groups: a control group with sawdust on the floor of the rearing cage (C), a group with mesh wire on the floor (M), and a group with water just below the mesh wire (W). Activation of lateral hypothalamic orexin neurons was assessed using immunofluorescence. In another experiment, half of the mice in each group were administered an intraperitoneal injection of suvorexant (10 mg/kg), and the remaining mice were injected with the same amount of vehicle (normal saline). Thermal hyperalgesia was examined using tail immersion and hot plate tests, while mechanical hyperalgesia was investigated using the tail pinch test after 21 days of PCMS. Animals subjected to PCMS showed an increased percentage of activated orexin neurons in the lateral hypothalamic region after 21 days. Mice raised in the PCMS environment showed increased pain sensitivity in several pain tests; however, the symptoms were significantly reduced by suvorexant administration. The findings revealed that PCMS activates hypothalamic orexin neuronal activity, and the use of suvorexant can help attenuate PCMS-induced thermal and mechanical hyperalgesia. • PCMS activates hypothalamic orexin neuronal activity. • Administration of suvorexant attenuates PCMS-induced thermal and mechanical hyperalgesia. • Orexin system plays an important role in hyperalgesia induced by PCMS. [ABSTRACT FROM AUTHOR]

Published

2022

30. Accumulation of β-aminoisobutyric acid mediates hyperalgesia in ovariectomized mice through Mas-related G protein-coupled receptor D signaling.

Author

Tu, Chen, Chen, Yun-Biao, Lai, Si-Qi, Yu, Yong-Peng, Huang, Zhi-Wei, Li, Hong-Zhou, Ao, Rui-Feng, Han, Dong, Gao, Jia-Wen, Zhu, Guo-Zheng, Wu, Di-Zheng, Huang, Yu-Sheng, Zhao, Kai, Meng, Ting-Ting, and Zhong, Zhao-Ming

Subjects

*G protein coupled receptors, *HYPERALGESIA, *DORSAL root ganglia, *PAIN threshold, *TRANSCRANIAL direct current stimulation, *MICE

Abstract

Hyperalgesia is typified by reduced pain thresholds and heightened responses to painful stimuli, with a notable prevalence in menopausal women, but the underlying mechanisms are far from understood. β-Aminoisobutyric acid (BAIBA), a product of valine and thymine catabolism, has been reported to be a novel ligand of the Mas-related G protein coupled receptor D (MrgprD), which mediates pain and hyperalgesia. Here, we established a hyperalgesia model in 8-week-old female mice through ovariectomy (OVX). A significant increase in BAIBA plasma level was observed and was associated with decline of mechanical withdrawal threshold, thermal and cold withdrawal latency in mice after 6 weeks of OVX surgery. Increased expression of MrgprD in dorsal root ganglion (DRG) was shown in OVX mice compared to Sham mice. Interestingly, chronic loading with BAIBA not only exacerbated hyperalgesia in OVX mice, but also induced hyperalgesia in gonadally intact female mice. BAIBA supplementation also upregulated the MrgprD expression in DRG of both OVX and intact female mice, and enhanced the excitability of DRG neurons in vitro. Knockout of MrgprD markedly suppressed the effects of BAIBA on hyperalgesia and excitability of DRG neurons. Collectively, our data suggest the involvement of BAIBA in the development of hyperalgesia via MrgprD-dependent pathway, and illuminate the mechanisms underlying hyperalgesia in menopausal women. • Increased BAIBA levels associated with the development of hyperalgesia in ovariectomized (OVX) mice. • Reduced expression of AGXT2 and ABAT in OVX mice contributes to the elevation of BAIBA. • BAIBA enhances the excitability of DRG neurons via MrgprD. • MrgprD signaling is pivotal for BAIBA-induced hyperalgesia. [ABSTRACT FROM AUTHOR]

Published

2024

31. CHARACTERIZATION OF PAG-PROJECTING CEA CELLS IN ADULT MALE RATS WITH HYPERALGESIA INDUCED BY ALCOHOL EXPOSURE DURING ADOLESCENCE.

Author

Engi, SA, Secci, ME, Gilpin, NW, and Wills, TA

Subjects

*HYPERALGESIA, *RATS, *ADOLESCENCE, *MALES

Published

2024

32. Oxidative stress plays an important role in the central regulatory mechanism of orofacial hyperalgesia under low estrogen conditions.

Author

Lu, Jiali, Zhang, Linqian, Zhang, Jinglin, Sun, Yanrong, Wang, Hanfei, Wang, Wenjuan, Wang, Ke, Qin, Lihua, and Jia, Jing

Subjects

*OXIDATIVE stress, *HYPERALGESIA, *EXCITATORY amino acids, *ESTROGEN, *OXIDANT status

Abstract

Hyperalgesia occurs in the orofacial region of rats when estrogen levels are low, although the specific mechanism needs to be investigated further. Furthermore, oxidative stress plays an important role in the transmission of pain signals. This study aimed to explore the role of oxidative stress in orofacial hyperalgesia under low estrogen conditions. We firstly found an imbalance between oxidative and antioxidant capacity within the spinal trigeminal subnucleus caudalis (SP5C) of rats after ovariectomy (OVX), resulting in oxidative stress and then a decrease in the orofacial pain threshold. To investigate the mechanism by which oxidative stress occurs, we used virus as a tool to silence or overexpress the excitatory amino acid transporter 3 (EAAT3) gene. Further investigation revealed that the regulation of glutathione (GSH) and reactive oxygen species (ROS) can be achieved by regulating EAAT3, which in turn impacts the occurrence of oxidative stress. In summary, our findings suggest that reduced expression of EAAT3 within the SP5C of rats in the low estrogen state may decrease GSH content and increase ROS levels, resulting in oxidative stress and ultimately lead to orofacial hyperalgesia. This suggests that antioxidants could be a potential therapeutic direction for orofacial hyperalgesia under low estrogen conditions, though more research is needed to understand its mechanism. • Hyperalgesia occurs in the orofacial region of rats when estrogen levels are low. • Oxidative stress is a key element in the development of orofacial hyperalgesia. • EAAT3 can regulate the balance of GSH and ROS, and thus influences oxidative stress. • Antioxidant therapy may be an important direction in the treatment of orofacial pain. [ABSTRACT FROM AUTHOR]

Published

2024

33. S100 - Vulnerability to Hyperalgesia and Hyperkatifeia Drives Addiction-Like Behaviors.

Author

Marchette, Renata, Frye, Emma, Hastings, Lyndsay, Carlson, Erika, Vendruscolo, Leandro, Tejeda, Hugo, and Koob, George

Subjects

*HYPERALGESIA, *MOTOR vehicle driving

Published

2024

34. Nocebo hyperalgesia and other expectancy-related factors in daily fibromyalgia pain: Combining experimental and electronic diary methods.

Author

Karacaoglu, Merve, Peerdeman, Kaya J., Karch, Julian D., van Middendorp, Henriët, and Evers, Andrea W.M.

Subjects

*PAIN catastrophizing, *FIBROMYALGIA, *HYPERALGESIA, *NOCEBOS, *DIARY (Literary form), *ECOLOGICAL momentary assessments (Clinical psychology), *COGNITIVE therapy

Abstract

Expectancies are known to shape pain experiences, but it remains unclear how different types of expectancies contribute to daily pain fluctuations in fibromyalgia. This combined experimental and diary study aims to provide insights into how experimentally-derived nocebo hyperalgesia and other, diary-derived, expectancy-related factors are associated with each other and with daily pain in fibromyalgia. Forty-one female patients with fibromyalgia first participated in a lab procedure measuring nocebo hyperalgesia magnitude, then filled out an electronic diary 3 times a day over 3 weeks regarding the expectancy-related factors of pain expectancy, anxiety, optimism, and pain-catastrophizing thoughts, and current pain intensity. Our results indicate that experimentally-induced nocebo hyperalgesia was not significantly related to diary-assessed expectancy-related factors and did not predict daily fibromyalgia pain. Higher levels of the self-reported expectancy-related factors pain expectancy and pain catastrophizing, but not anxiety and optimism, predicted moment-to-moment pain increases in fibromyalgia, after controlling for current pain, moment-of-day and all other expectancy-related factors. Our exploratory research findings indicate that self-reported expectancy-related factors, particularly pain expectancy and pain catastrophizing, are potentially more relevant for predicting daily pain experience than experimentally-induced nocebo hyperalgesia. Further translation of nocebo hyperalgesia is needed from experimental to Ecological Momentary Assessment research. Our findings imply that targeting the decrease in pain expectancy and catastrophizing thoughts e.g., via Cognitive Behavioral Therapy, have potential for improving daily pain levels in fibromyalgia. • This study is the first to incorporate experimental and electronic diary methods. • Higher pain expectancy and catastrophizing predicted fibromyalgia pain increase. • Experimentally-induced nocebo hyperalgesia did not predict fibromyalgia pain. [ABSTRACT FROM AUTHOR]

Published

2024

35. The role of self-reported and physiological stress in nocebo hyperalgesia.

Author

Skvortsova, A., Meeuwis, S.H., Derksen, S., Kerkkänen, K., Sutter, E., Evers, A.W.M., and Veldhuijzen, D.S.

Subjects

*NOCEBOS, *PHYSIOLOGICAL stress, *HYPERALGESIA, *PHYSIOLOGY, *PSYCHOLOGICAL factors, *GALVANIC skin response, *SOCIAL anxiety

Abstract

Negative expectations can increase pain sensitivity, leading to nocebo hyperalgesia. However, the physiological and psychological factors that predispose individuals to this phenomenon are still not well understood. The present study examined whether stress induced by a social stressor affects nocebo hyperalgesia, and whether this effect is mediated by self-reported and physiological stress responses. We recruited 52 healthy participants (15 men) who were randomly assigned to either the Trier Social Stress Test (TSST) or a control condition (a friendly version of the TSST). Nocebo hyperalgesia was induced using negative suggestions combined with a validated pain conditioning paradigm. We assessed self-reported (anxiety and stress) and physiological (cortisol, alpha-amylase, heart rate, and skin conductance) responses to stress. Both groups exhibited significant nocebo hyperalgesia. The stress group showed higher levels of anxiety, self-reported stress, and cortisol levels compared to the control group while no significant differences were found in other physiological markers. The stress and control groups did not differ in the magnitude of nocebo hyperalgesia, but anxiety levels partially mediated the effects of the stress test on nocebo hyperalgesia. Our findings suggest that an external social stressor does not directly affect nocebo hyperalgesia, but that increased anxiety due to the stressor enhances its magnitude. Thus, it may be worthwhile to investigate whether reducing stress-related anxiety in clinical settings would help alleviate nocebo effects. • Social stress test does not directly influence nocebo hyperalgesia. • State anxiety partially mediates the effects of the social stress test on nocebo hyperalgesia. • Future research should study stress reduction for alleviation of nocebo effects. [ABSTRACT FROM AUTHOR]

Published

2024

36. Reduced sympathetic activity is associated with the development of pain and muscle atrophy in a female rat model of fibromyalgia.

Author

da Silva, Raquel Prado, Costa, Daniely Messias, da Cruz-Filho, João, Santos, Tatiane de Oliveira, dos Anjos-Santos, Hevely Catharine, Vasconcelos, Alan Bruno Silva, Heck, Lilian Carmo, Kettelhut, Ísis do Carmo, Navegantes, Luiz Carlos, dos Santos, José Ronaldo, de Souza, Patrícia Rodrigues Marques, Badauê-Passos Jr, Daniel, Mecawi, André Souza, DeSantana, Josimari Melo, and Lustrino, Danilo

Subjects

*FIBROMYALGIA, *MUSCULAR atrophy, *LABORATORY rats, *MYALGIA, *MUSCLE growth, *SYMPATHETIC nervous system

Abstract

• Plasma epinephrine is decreased in priming models of fibromyalgia-like pain. • Clenbuterol attenuates hyperalgesia in an acid saline-induced fibromyalgia-like pain model. • Clenbuterol mitigates muscle atrophy in fibromyalgia priming model. Fibromyalgia (FM) is characterized by chronic widespread musculoskeletal pain accompanied by fatigue and muscle atrophy. Although its etiology is not known, studies have shown that FM patients exhibit altered function of the sympathetic nervous system (SNS), which regulates nociception and muscle plasticity. Nevertheless, the precise SNS-mediated mechanisms governing hyperalgesia and skeletal muscle atrophy in FM remain unclear. Thus, we employed two distinct FM-like pain models, involving intramuscular injections of acidic saline (pH 4.0) or carrageenan in prepubertal female rats, and evaluated the catecholamine content, adrenergic signaling and overall muscle proteolysis. Subsequently, we assessed the contribution of the SNS to the development of hyperalgesia and muscle atrophy in acidic saline-injected rats treated with clenbuterol (a selective β2-adrenergic receptor agonist) and in animals maintained under baseline conditions and subjected to epinephrine depletion through adrenodemedullation (ADM). Seven days after inducing an FM-like model with acidic saline or carrageenan, we observed widespread mechanical hyperalgesia along with loss of strength and/or muscle mass. These changes were associated with reduced catecholamine content, suggesting a common underlying mechanism. Notably, treatment with a β2-agonist alleviated hyperalgesia and prevented muscle atrophy in acidic saline-induced FM-like pain, while epinephrine depletion induced mechanical hyperalgesia and increased muscle proteolysis in animals under baseline conditions. Together, the results suggest that reduced sympathetic activity is involved in the development of pain and muscle atrophy in the murine model of FM analyzed. [ABSTRACT FROM AUTHOR]

Published

2024

37. Efficacy assessment of novel methanimine derivatives in chronic constriction injury-induced neuropathic model: An in-vivo, ex-vivo and In-Silico approach.

Author

khan, Jawad, Ali, Gowhar, Saeed, Aamer, Khurshid, Asma, Ahmad, Sajjad, Kashtoh, Hamdy, Ataya, Farid S., Bathiha, Gaber El-Saber, Ullah, Aman, and Khan, Ajmal

Subjects

*TUMOR necrosis factors, *NEURALGIA, *SCIATIC nerve, *BINDING energy, *HYPERALGESIA, *CANCER pain, *PAIN management

Abstract

The multicomponent etiology, complex clinical implications, dose-based side effect and degree of pain mitigation associated with the current pharmacological therapy is incapable in complete resolution of chronic neuropathic pain patients which necessitates the perpetual requirement of novel medication therapy. Therefore, this study explored the ameliorative aptitude of two novel methanimine imitative like (E)-N-(4-nitrobenzylidene)-4‑chloro-2-iodobenzamine (KB 09) and (E)-N-(4-methylbenzylidene)-4‑chloro-2-iodobenzamine (KB 10) in chronic constriction injury (CCI) of sciatic nerve induced neuropathic pain in rat model. Standard behavioral tests like dynamic and static allodynia, cold, thermal and mechanical hyperalgesia along with rotarod activity were performed at various experimental days like 0, 3, 7, 14 and 21. Enzyme linked immunosorbent assay (ELISA) on spinal tissue and antioxidant assays on sciatic nerve were executed accompanied by molecular docking and simulation studies. Prolonged ligation of sciatic nerve expressively induced hyperalgesia as well as allodynia in rats. KB 09 and KB 10 substantially attenuated the CCI elicited hyperalgesia and allodynia. They significantly reduced the biomarkers of pain and inflammation like Interleukin-6 (IL-6) and tumor necrosis factor-alpha (TNF-α) in ELISA and while enhanced the GSH, SOD and CAT and diminished the MDA levels during antioxidant assays. KB 09 displayed -9.62 kcal/mol with TNF-α and -7.68 kcal/mol binding energy with IL-6 whereas KB 10 exhibited binding energy of -8.20 kcal/mol with IL-6 while -11.68 kcal/mol with TNF-α and hence both trial compounds ensured stable interaction with IL-6 and TNF-α during computational analysis. The results advocated that both methanimine derivatives might be novel candidates for attenuation of CCI-induced neuropathic pain prospects via anti-nociceptive, anti-inflammatory and antioxidant mechanisms. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

38. Cannabidiol and it fluorinate analog PECS-101 reduces hyperalgesia and allodynia in trigeminal neuralgia via TRPV1 receptors.

Author

Escobar-Espinal, Daniela Maria, Vivanco-Estela, Airam Nicole, Barros, Núbia, dos Santos Pereira, Maurício, Guimaraes, Francisco Silveira, Del Bel, Elaine, and Nascimento, Glauce C.

Subjects

*TRPV cation channels, *TRIGEMINAL neuralgia, *BLINKING (Physiology), *HYPERALGESIA, *CANNABIDIOL

Abstract

Trigeminal neuralgia (TN) is an intense and debilitating orofacial pain. The gold standard treatment for TN is carbamazepine. This antiepileptic drug provides pain relief with limited efficacy and side effects. To study the antinociceptive potential of cannabidiol (CBD) and its fluorinated analog PECS-101 (former HUF-101), we induced unilateral chronic constriction injury of the infraorbital nerve (IoN-CCI) in male Wistar rats. Seven days of treatment with CBD (30 mg/kg), PECS-101 (3, 10, and 30 mg/kg), or carbamazepine (10 and 30 mg/kg) reduced allodynia and hyperalgesia responses. Unlike carbamazepine, CBD and PECS-101 did not impair motor activity. The relief of the hypersensitive reactions has been associated with transient receptor potential vanilloid type 1 (TRPV1) modulation in the trigeminal spinal nucleus. CBD (30 mg/kg) and PECS-101 (10 and 30 mg/kg) reversed the increased expression of TRPV1 induced by IoN-CCI in this nucleus. Using a pharmacological strategy, the combination of the selective TRPV1 antagonist (capsazepine-CPZ – 5 mg/kg) with sub-effective doses of CBD (3 and 10 mg/kg) is also able to reverse the IoN-CCI-induced allodynia and hyperalgesia responses. This effect was accompanied by reduced TRPV1 protein expression in the trigeminal spinal nucleus. Our results suggest that CBD and PECS-101 may benefit trigeminal neuralgia without motor coordination impairments. PECS-101 is more potent against the hypernociceptive and motor impairment induced by TN compared to CBD and carbamazepine. The antinociceptive effect of these cannabinoids is partially mediated by TRPV1 receptors in the caudal part of the trigeminal spinal nucleus, the first central station of orofacial pain processing. Representation of the synergistic antinociceptive action of the CPZ/CBD combination in the endocannabinoid system and the TRPV1 receptor through the following mechanisms: (I) Blockage of the TRPV1 receptor by the CPZ antagonist, inhibiting its activity and preventing it from responding to stimuli that trigger the sensation of pain; (II) Activation of the TRPV1 receptor by CBD, leading to receptor desensitization after prolonged exposure; (III) Inhibition of the FAAH enzyme by CBD, increasing the level of AEA, which is an endocannabinoid known for its role in pain regulation and also desensitizing TRPV1. [Display omitted] • Natural and synthetic cannabinoid compounds exhibit antinociceptive effects in trigeminal neuralgia. • Natural and synthetic cannabinoid compounds do not result in motor coordination impairment. • Natural and synthetic cannabinoid compounds demonstrate superior antinociceptive effects in trigeminal neuralgia when compared to carbamazepine. • PECS-101 reduces the expression of the TRPV1 receptor protein at a lower dose compare to CBD. • An antagonist of TRPV1 receptor and CBD may offer promising therapeutic potential in the future. [ABSTRACT FROM AUTHOR]

Published

2024

39. The ethanol extract of cocoa pod husk minimizes hyperalgesia and blood glucose levels in diabetic neuropathy model through transient receptor protein vanilloid (TRPV)-1.

Author

Aprila Fajrin, Fifteen, Holidah, Diana, Nurhidayah, Heni, Suci Wulansari, Putri, Pudji Restanto, Didik, Azkiyah, Lailatul, Witono, Yuli, and Satia Nugraha, Ari

Abstract

• To our knowledge, this study is the first report of the potency of ethanolic extract from cocoa pod husk (EECPH) in neuropathy diabetes. In our finding, the EECPH dose of 750 mg/kg BW could reduce the blood glucose levels as well as hyperalgesia in alloxan-induced diabetic neuropathy mice. Other biochemical parameters also showed positive changes such as MDA levels, total cholesterol, SGOT, and SGPT. The EECPH dose of 750 mg/kg BW also improved the histology of the pancreas and spinal cords. The expression of TRPV1 in the pancreas and spinal cords were opposite and defined that TRPV1 might responsible for hyperalgesia and insulin secretion in DN mice. Oxidative stress accumulation becomes a pathophysiological factor in diabetic neuropathy (DN), activating TRPV-1. Resveratrol in cocoa pod husk exhibits antioxidant activity that could be beneficial in DN. This study examined how the ethanol extract of cocoa pod husk (EECPH) affects DN in mice by targeting TRPV-1. Cocoa pod husk was extracted using 96 % ethanol with remaceration. The antioxidant activity was measured using DPPH. Mice were induced using alloxan 210 mg/kg BW i.p. At day 14, mice were randomized into seven groups: normal, diabetic, gabapentin 100 mg/kg BW, metformin 250 mg/kg BW, and EECPH (doses 250, 500, and 750 mg/kg BW). Treatments were administered orally, once daily for 14 days. The latency time and blood glucose levels were measured on days 7, 14, 21, and 28. On day 29, mice were sacrificed, and the blood, pancreas, and spinal cord were removed. Malondialdehyde, cholesterol, and serum glutamic oxaloacetic/pyruvic transaminase (SGOT/PT) were examined. Morphology of the spinal cord and pancreas was determined using hematoxylin and eosin staining. The expression of TRPV-1 was assessed using immunohistochemistry. T he EECPH dose of 750 mg/kg BW showed the greatest effect in lowering hyperalgesia and blood glucose as well as cholesterol and SGOT/PT in mice. That dose also improved the histology of the pancreas and spinal cord by altering the expression of TRPV-1. It can be concluded that EECPH may lower the expression of TRPV-1 in the pancreas and spinal cord of mice. This activity was responsible of reducing hyperalgesia in DN mice. [ABSTRACT FROM AUTHOR]

Published

2024

40. Artesunate Reduces Remifentanil-induced Hyperalgesia and Peroxiredoxin-3 Hyperacetylation via Modulating Spinal Metabotropic Glutamate Receptor 5 in Rats.

Author

Zhang, Linlin, Zhao, Yuying, Gao, Tianyu, Zhang, Haoyue, Li, Jing, Wang, Guolin, Wang, Chunyan, and Li, Yize

Subjects

*REMIFENTANIL, *GLUTAMATE receptors, *HYPERALGESIA, *INTRATHECAL injections, *INTRAVENOUS therapy, *RATS, *VISCERAL pain

Abstract

• Remifentanil induces mGluR5-dependent peroxiredoxin-3 hyperacetylation. • Artesunate reduces remifentanil-induced hyperalgesia and mGluR5 expression. • Artesunate reduces remifentanil-induced peroxiredoxin-3 hyperacetylation. • mGluR5 antagonist prevents remifentanil-induced hyperalgesia. • Artesunate impairs the mGluR5 agonist-evoked acute pain. The experimental investigations on the pathogenesis of remifentanil-induced hyperalgesia (RIH) have been primarily conducted, but the effective treatment of RIH remains unclear. Recent reports highlight the necessity of ionotropic glutamate receptors in oxidative damage in spinal nociceptive transduction. Artesunate, the 1st-line anti-malaria drug, has been identified to be valid in removing superoxide in several pathological conditions. This study evaluated whether artesunate inhibits RIH via regulating metabotropic glutamate receptor 5 (mGluR5) and mitochondrial antioxidant enzyme peroxiredoxin-3 in rats. Artesunate was injected intrathecally 10 min before intravenous infusion of remifentanil (1 μg·kg−1·min−1 for 60 min) in rats. The antinociception of artesunate was verified by assessment of paw withdrawal mechanical threshold and paw withdrawal thermal latency. Spinal mGluR5 expression and peroxiredoxin-3 hyperacetylation were examined. Also, both the mGluR5 agonist DHPG and antagonist MPEP were utilized to explore the involvement of mGluR5 in the anti-hyperalgesic property of artesunate. Here, we found that artesunate (10 μg and 100 μg but not 1 μg) prevented RIH in a dose-dependent manner. Artesunate reduced remifentanil-related spinal over-expression of mGluR5 gene and protein, and hyperacetylation of peroxiredoxin-3. Intrathecal application of MPEP (10 nmol and 100 nmol but not 1 nmol) inhibited behavioral RIH and peroxiredoxin-3 acetylation. Moreover, hyperalgesia and peroxiredoxin-3 hyperacetylation were attenuated after the combination of artesunate (1 μg) and MPEP (1 nmol). Additionally, artesunate treatment reversed acute pain and peroxiredoxin-3 hyperacetylation following spinal exposure to DHPG. In conclusion, intrathecal injection of artesunate impairs RIH by down-regulating spinal mGluR5 expression and peroxiredoxin-3 hyperacetylation-mediated oxidative stress in rats. [ABSTRACT FROM AUTHOR]

Published

2022

41. Postoperative pain facilitates rat C-fibre activity-dependent slowing and induces thermal hypersensitivity in a sex-dependent manner.

Author

Velichkova, Atanaska N., Coleman, Sophie E., and Torsney, Carole

Subjects

*POSTOPERATIVE pain, *NERVOUS system injuries, *ALLERGIES, *SODIUM channels, *ECHO-planar imaging, *TETRODOTOXIN, *HEAT, *RATS, *ACTION potentials, *ANIMALS, *HYPERALGESIA

Abstract

Background: Postoperative pain is a common clinical problem that, in preclinical studies, has almost exclusively been studied in males. Altered C-fibre activity-dependent slowing (ADS) is a potential underlying mechanism, given it is altered after tissue inflammation and nerve injury, but this has not been explored post-incision. We therefore investigated the effect of hind-paw incision on C-fibre ADS in both sexes and the involvement of voltage-gated sodium channels (NaV) as they contribute to ADS. We also assessed mechanical and thermal sensitivity post-incision in both sexes.Methods: Dorsal roots were isolated from hind-paw incision (2-4 days post-surgery) or naive (control) juvenile rats of both sexes. Compound action potential recordings were made to assess C-fibre ADS in response to ×40 stimuli at 2 and 10 Hz and repeated in the presence of 20 nM tetrodotoxin/vehicle. Data were quantified by the normalised change in latency (negative peak) and width (positive-to-positive peak) of the triphasic C-fibre response. Hind-paw mechanical withdrawal thresholds and thermal withdrawal latencies were measured pre- and post-incision.Results: Incision facilitates C-fibre ADS in both sexes, with more pronounced facilitation in females. Tetrodotoxin induces sex- and injury-dependent changes in C-fibre ADS that were distinct between latency and width measures. Hind-paw incision induced comparable mechanical hypersensitivity in both sexes but less peak heat hypersensitivity in females.Conclusions: Hind-paw incision induces sex-dependent changes in C-fibre activity-dependent slowing, which likely contribute to the observed sex difference in peak thermal hypersensitivity. This may reflect sex- and incision-induced differences in functional expression of NaV channels that differs by C-fibre subtype. [ABSTRACT FROM AUTHOR]

Published

2022

42. Characteristics of sensory innervation in synovium of rats within different knee osteoarthritis models and the correlation between synovial fibrosis and hyperalgesia.

Author

Zhang, Li, Li, Mingchao, Li, Xiaochen, Liao, Taiyang, Ma, Zhenyuan, Xing, Runlin, Wang, Peimin, and Mao, Jun

Subjects

*KNEE osteoarthritis, *ANTERIOR cruciate ligament, *SYNOVIAL membranes, *HYPERALGESIA, *FIBROSIS, *INNERVATION

Abstract

[Display omitted] • Synovial fibrosis was positively correlated with pain sensitivity in KOA rats. • Synovial fibrosis was most prominent in DMM group 14 days after modeling. • ACLT replaced DMM to be the most typical at 28 days after modeling. • Increased synovial sensory innervation followed the same trend as fibrosis. • ACLT is more applicable for KOA pain research. Knee osteoarthritis (KOA) showed synovial fibrosis and hyperalgesia, although the correlation between the two is unclear. Besides, the specific changes of sensory innervation in animal models are still controversial, which makes it difficult to choose the modeling methods for KOA pain research. Study the characteristics of sensory innervation within three commonly used KOA rat models and the correlation between synovial fibrosis and hyperalgesia. KOA models were induced by destabilization of medial meniscus (DMM), anterior cruciate ligament transection (ACLT), and monoiodoacetate (MIA), respectively. Mechanical, cold and thermal withdrawal threshold (MWT, CWT and TWT) were measured. The harvested tissues were used for pathological sections, immunofluorescence and quantitative analysis. KOA synovium showed more type I collagen deposition, increased expression of CD31, VEGF and TGF-β. These changes were most pronounced in surgical models, with DMM presenting the most prominent at Day 14 and ACLT at Day 28. Day 14, changes in mechanical hyperalgesia and cold hyperalgesia were most typical in DMM model and statistically different from MIA. There was a negative correlation between the percentage of type I collagen and MWT value (r = −0.88), as well as CWT value (r = −0.95). DMM synovium showed more axonal staining, upregulated CGRP, TRPV1, NGF and Netrin1 compared with MIA. Above changes were also observed at Day 28, but ACLT replaced DMM as the most typical. In DRG, only the levels of CGRP and NGF were different among KOA models at Day 14, and the highest in DMM, which was statistically different compared with MIA. This study described the details of sensory innervation in different KOA model of rats, and the degree of synovial fibrosis was positively correlated with the pain sensitivity of KOA model rats. Additionally, surgical modeling especially ACLT method is more recommended for KOA pain research. [ABSTRACT FROM AUTHOR]

Published

2022

43. Behavioral, Cellular and Molecular Responses to Cold and Mechanical Stimuli in Rats with Bilateral Dopamine Depletion in the Mesencephalic Dopaminergic Neurons.

Author

Elshennawy, Mennatallah, Ouachikh, Omar, Aissouni, Youssef, Youssef, Shahira, Zaki, Shahira S., Durif, Franck, and Hafidi, Aziz

Subjects

*DOPAMINERGIC neurons, *EXTRACELLULAR signal-regulated kinases, *PROTEIN kinase C, *GLUTAMATE decarboxylase, *RATS, *CELLULAR mechanics

Abstract

• 6-OHDA-lesioned rats demonstrated pain sensitivity to cold temperature and acetone stimuli. • Paw acetone stimulus induced a significant pERK1/2 expression in multiple structures in 6-OHDA-lesioned rats compared with sham. • There was a significant increase in PKCγ and GAD67 in the spinal dorsal horn of lesioned rats. • Ropinirole administration reversed the changes in these markers. Pain is the major non-motor symptom in Parkinson's disease (PD). Preclinical studies have mostly investigated mechanical pain by considering the decrease in a nociceptive threshold. Only a few studies have focused on thermal pain in animal models of PD. Therefore, the goal of this study was to assess the thermal nociceptive behavior of rats subjected to 6-hydroxydopamine (6-OHDA) administration, which constitutes an animal model of PD. Thermal plate investigation demonstrated significant thermal sensitivity to cold temperatures of 10 °C and 15 °C, and not to higher temperatures, in 6-OHDA-lesioned rats when compared with sham. 6-OHDA-lesioned rats also showed cold allodynia as demonstrated by a significant difference in the number of flinches, latency and reaction time to acetone stimulus. Ropinirole administration, a dopamine receptor 2 (D2R) agonist, blocked the acetone-induced cold allodynia in 6-OHDA-lesioned rats. In addition, mechanical hypersensitivity and static allodynia, as demonstrated by a significant difference in the vocalization threshold and pain score respectively, were noticed in 6-OHDA-lesioned rats. Acetone stimulus induced a significant increase in extracellular signal-regulated protein kinases 1 and 2 (ERK1/2) phosphorylation, a pain process molecular marker, in the spinal dorsal horn (SDH), the insular and cingulate cortices in 6-OHDA-lesioned rats when compared to sham. In 6-OHDA-lesioned rats, there was a significant augmentation in the expression of both protein kinase C gamma (PKCγ) and glutamate decarboxylase 67 (GAD67) in the SDH. This highlighted an increase in excitation and a decrease in inhibition in the SDH. Overall, the present study demonstrated a clear cold thermal hypersensitivity, in addition to a mechanical one, in 6-OHDA-lesioned rats. [ABSTRACT FROM AUTHOR]

Published

2021

44. How different experimental models of secondary hyperalgesia change the nociceptive flexion reflex.

Author

Leone, C., Di Lionardo, A., Di Pietro, G., Di Stefano, G., Falco, P., Blockeel, A.J., Caspani, O., Garcia-Larrea, L., Mouraux, A., Phillips, K.G., Treede, R.D., and Truini, A.

Subjects

*REFLEXES, *PAIN threshold, *HYPERALGESIA, *NEURAL stimulation, *CAPSAICIN

Abstract

• Central sensitization manifesting with secondary hyperalgesia is similarly induced by high-frequency stimulation and topical capsaicin. • High frequency stimulation and topical capsaicin do not significantly activate the endogenous pain modulatory system. • RIII reflex variables reflecting central sensitization are similarly modulated by high frequency stimulation and topical capsaicin. In this neurophysiological study in healthy humans, we assessed how central sensitization induced by either high-frequency stimulation (HFS) or topical capsaicin application modulates features of the RIII reflex response. The ability of these stimuli to engage the endogenous pain modulatory system was also tested. In 26 healthy participants we elicited an RIII reflex using suprathreshold stimulation of the sural nerve. Subsequently HFS or capsaicin were applied to the foot and the RIII reflex repeated after 15 minutes. Contact heating of the volar forearm served as the heterotopic test stimulus to probe activation of the endogenous pain modulatory system. HFS significantly reduced the pain threshold by 29% and the RIII reflex threshold by 20%. Capsaicin significantly reduced the pain threshold by 17% and the RIII reflex threshold by 18%. Both HFS and capsaicin left RIII reflex size unaffected. Numerical Rating Scale (NRS) pain scores elicited by the heterotopic noxious heat stimulus were unaffected by capsaicin and slightly increased by HFS. HFS and capsaicin similarly modulated the pain threshold and RIII reflex threshold, without a concomitant inhibitory effect of the endogenous pain modulatory system. Our neurophysiological study supports the use of the RIII reflex in investigating central sensitization in humans. [ABSTRACT FROM AUTHOR]

Published

2021

45. The impact of foot shock-induced stress on pain-related behavior associated with burn injury.

Author

Wu, Pau Yen, Menta, Blaise, Visk, Alexander, Ryals, Janelle M., Christianson, Julie A., Wright, Douglas E., and Chadwick, Andrea L.

Subjects

*LABORATORY mice, *IMMOBILIZATION stress, *WOUNDS & injuries, *FOOT pain, *CHRONIC pain, *STRAINS & stresses (Mechanics), *ALLODYNIA, *INHALATION injuries, *BURNS & scalds complications, *BIOLOGICAL models, *PAIN, *ANIMAL experimentation, *RESEARCH funding, *MICE, *HYPERALGESIA

Abstract

Acute pain is prevalent following burn injury and can often transition to chronic pain. Prolonged acute pain is an important risk factor for chronic pain and there is little preclinical research to address this problem. Using a mouse model of second-degree burn, we investigated whether pre-existing stress influences pain(sensitivity) after a burn injury. We introduced a contribution of stress in two different ways: (1) the use of foot-shock as a pre-injury stressor or (2) the use of A/J mice to represent higher pre-existing stress compared to C57Bl/6 mice. C57Bl/6 and A/J mice were exposed to repeated mild foot shock to induce stress for 10 continuous days and mice underwent either burn injury or sham burn injury of the plantar surface of the right hind paw. Assessments of mechanical and thermal sensitivities of the injured and uninjured paw were conducted during the shock protocol and at intervals up to 82-day post-burn injury. In both strains of mice that underwent burn injury, thermal hypersensitivity and mechanical allodynia appeared rapidly in the ipsilateral paw. Mice that were stressed took much longer to recover their hind paw mechanical thresholds to baseline compared to non-stressed mice in both burn and non-burn groups. Analysis of the two mouse strains revealed that the recovery of mechanical thresholds in A/J mice which display higher levels of baseline anxiety was shorter than C57Bl/6 mice. No differences were observed regarding thermal sensitivities between strains. Our results support the view that stress exposure prior to burn injury affects mechanical and thermal thresholds and may be relevant to as a risk factor for the transition from acute to chronic pain. Finally, genetic differences may play a key role in modality-specific recovery following burn injury. [ABSTRACT FROM AUTHOR]

Published

2021

46. IGF1-driven induction of GPCR kinase 2 in the primary afferent neuron promotes resolution of acute hyperalgesia.

Author

Takemura, Hitomi, Kushimoto, Kohsuke, Horii, Yasuhiko, Fujita, Daisuke, Matsuda, Megumi, Sawa, Teiji, and Amaya, Fumimasa

Subjects

*SOMATOMEDIN C, *AFFERENT pathways, *HYPERALGESIA, *DORSAL root ganglia, *CELL physiology, *LIPOXINS

Abstract

Dynamic regulation of G-protein-coupled receptor (GPCR) kinase 2 (GRK2) expression restores cellular function by protecting from overstimulation via GPCR and non-GPCR signaling. In the primary afferent neurons, GRK2 negatively regulates nociceptive tone. The present study tested the hypothesis that induction of GRK2 in the primary afferent neurons contributes to the resolution of acute pain after tissue injury. GRK2 expression in the dorsal root ganglion (DRG) was analyzed at 1 and 7 days after the incision. Intraperitoneal administration of a GRK2 inhibitor was performed 7 days post-incision in male Sprague-Dawley rats who underwent plantar incisions to analyze the pain-related behavioral effect of the GRK2 inhibitor. Separately, GRK2 expression was analyzed after injecting insulin-like growth factor 1 (IGF1) into the rat hind paw. In addition, an IGF1 receptor (IGF1R) inhibitor was administered in the plantar incision rats to determine its effect on the incision-induced hyperalgesia and GRK2 expression. Plantar incision induced an increase in GRK2 in the DRG at 7 days, but not at 1 day post-incision. Acute hyperalgesia after the plantar incision disappeared by 7 days post-incision. Intraperitoneal injection of the GRK2 inhibitor at this time reinstated mechanical hyperalgesia, although the GRK2 inhibitor did not produce hyperalgesia in naive rats. After the incision, IGF1 expression increased in the paw, but not in the DRG. Intraplantar injection of IGF1 increased GRK2 expression in the ipsilateral DRG. IGF1R inhibitor administration prevented both the induction of GRK2 and resolution of hyperalgesia after the plantar incision. These findings demonstrate that induction of GRK2 expression driven by tissue IGF1 has potent analgesic effects and produces resolution of hyperalgesia after tissue injury. Dysregulation of IGF1-GRK2 signaling could potentially lead to failure of the spontaneous resolution of acute pain and, hence, development of chronic pain after surgery. • GRK2 was present in DRG neurons, and its expression was significantly increased 7 days after the incision. • GRK2 inhibitor treatment 7 days after the incision led to the return of hyperalgesia. • IGF1 treatment increases GRK2 expression in the DRG. • IGF1 inhibitor suppressed GRK2 induction and extended the duration of hyperalgesia after the tissue injury. [ABSTRACT FROM AUTHOR]

Published

2021

47. P2Y1 purinergic receptor inhibition attenuated remifentanil-induced postoperative hyperalgesia via decreasing NMDA receptor phosphorylation in dorsal root ganglion.

Author

Su, Lin, Bai, Xiaoqing, Niu, Tongxiang, Zhuang, Xinqi, Dong, Beibei, Wang, Guolin, and Yu, Yonghao

Subjects

*REMIFENTANIL, *DORSAL root ganglia, *PURINERGIC receptors, *PHOSPHORYLATION, *METHYL aspartate receptors, *HYPERALGESIA, *WESTERN immunoblotting, *IMMUNOFLUORESCENCE

Abstract

Remifentanil-induced postoperative hyperalgesia is an intractable side effect of the clinical use of remifentanil, the mechanism of which remains obscure, especially in the peripheral nervous system. N-methyl- D -aspartate receptor (NMDAR) phosphorylation in dorsal root ganglion (DRG) plays a pronociceptive role in neuropathic pain. The contribution of the P2Y1 purinergic receptor (P2Y1R) in DRG to pain hypersensitivity derived from various origins and P2Y1R upregulation-induced NMDAR activation in neurons have also been uncovered. This study aimed to investigate whether P2Y1R participates in nociceptive processing in the DRG and spinal cord in remifentanil-induced postoperative hyperalgesia. Rats with remifentanil-induced postoperative hyperalgesia were intrathecally injected with NMDAR antagonist MK801 or P2Y1R antagonist MRS2179 at 10 min prior to remifentanil infusion. Mechanical allodynia, heat hyperalgesia, and cold hyperalgesia were measured at −24 h, 2 h, 6 h, 24 h, and 48 h following remifentanil infusion. The P2Y1R expression and NMDAR expression and phosphorylation in DRG ipsilateral to the incision were detected by Western blot and immunofluorescence. Incision and remifentanil induced mechanical allodynia, heat hyperalgesia, and cold hyperalgesia accompanied by upregulated P2Y1R expression, increased NMDAR subunit NR1 expression and phosphorylation at Ser896, and NR2B expression and phosphorylation at Tyr1472 in DRG. Inhibition of NMDAR phosphorylation by MK801 effectively attenuated remifentanil-induced postoperative hyperalgesia. Furthermore, P2Y1R blockade by MRS2179 not only lessened remifentanil-evoked postoperative hypersensitivity to mechanical, heat, and cold stimuli, but also suppressed the increases in NR1 and NR2B expression and phosphorylation in DRG induced by incision and remifentanil. The process by which P2Y1R mediates NMDAR expression and phosphorylation represents a mechanism of remifentanil-induced postoperative hyperalgesia in the DRG and/or spinal cord. • Incision-evoked mechanical, heat and cold pain were worsened by remifentanil infusion. • P2Y1R expression and NMDAR phosphorylation were increased in rats with hyperalgesia. • Both inhibiting P2Y1R and lowering NMDAR phosphorylation relieved hyperalgesia. • P2Y1R blockade suppressed the increases in NMDAR expression and phosphorylation. [ABSTRACT FROM AUTHOR]

Published

2021

48. Circadian rhythms in opioid-induced hyperalgesia: call for comprehensive research. Comment on Br J Anaesth 2023; 131: 1072–81.

Author

Liu, Xiaowen and Zhao, Jing

Subjects

*CIRCADIAN rhythms, *HYPERALGESIA

Published

2024

49. Peripheral mechanisms involved in Tityus bahiensis venom-induced pain.

Author

Ferraz, Camila R., Manchope, Marília F., Andrade, Ketlem C., Saraiva-Santos, Telma, Franciosi, Anelise, Zaninelli, Tiago H., Bagatim-Souza, Julia, Borghi, Sergio M., Cândido, Denise M., Knysak, Irene, Casagrande, Rubia, Kwasniewski, Fábio H., and Verri, Waldiceu A.

Subjects

*TITYUS, *NF-kappa B, *TUMOR necrosis factors, *SNAKE venom

Abstract

Scorpionism is a public health burden in Brazil. Tityus bahiensis is responsible for most accidents in the Southeastern region of Brazil. Here, the hyperalgesic mechanisms of Tityus bahiensis venom were investigated, focusing on the role of pro-inflammatory cytokines (tumor necrosis factor alpha [TNF-α] and interleukin 1 beta [IL-1β]) and activation of the transcription factor NFκB. Intraplantar (i.pl.) administration of Tityus bahiensis venom (0.2, 0.6, 1.2 and 2.4 μg/20 μL i.pl.) induced mechanical hyperalgesia and thermal hyperalgesia. The 2.4 μg dose of Tityus bahiensis venom induced overt pain-like behavior and increased myeloperoxidase (MPO) and N-acetyl-beta-D-glucosaminidase (NAG) activities, TNF-α and IL-1β levels in the paw tissue. Systemic pre-treatment with etanercept (soluble TNF-α receptor; 10 mg/kg), IL-1ra (IL-1 receptor antagonist; 30 mg/kg) and pyrrolidine dithiocarbamate (PDTC, nuclear factor kappa B [NFκB] inhibitor; 100 mg/kg) inhibited Tityus bahiensis venom-induced mechanical and thermal hyperalgesia, MPO and NAG activity and overt pain-like behavior. These data demonstrate the involvement of TNF-α and IL-1β signaling as well as NFκB activation in Tityus bahiensis venom-induced mechanical and thermal hyperalgesia, overt pain-like behavior, and MPO activity and NAG activity, indicating thus, that targeting these mechanisms might contribute to reducing the pain in this scorpionism. • Tityus bahiensis venom increased tumor necrosis factor α (TNF-α) and interleukin 1 β (IL-1β) levels in the paw tissue. • Treatment with inhibitors of TNF-α, IL-1β and nuclear factor kappa B (NFκB) reduced Tityus bahiensis venom-induced pain. • Those treatments also reduced Tityus bahiensis venom-induced myeloperoxidase and N-acetyl-beta-D-glucosaminidase activities. • This is the first demonstration of TNF-α, IL-1β and NFκB contribution to Tityus bahiensis venom-induced pain. [ABSTRACT FROM AUTHOR]

Published

2021

50. Evaluation of Secondary Thermal Hyperalgesia Resulting from Pulpal Inflammation in Patients with Symptomatic Irreversible Pulpitis.

Author

Sooratgar, Aidin, Ahmadi, Zohreh, Asadi, Yasin, Dibaji, Fatemeh, Shamshiri, Ahmad Reza, and Afkhami, Farzaneh

Subjects

PULPITIS, HYPERALGESIA, PERIPHERAL nervous system, ROOT canal treatment, CENTRAL nervous system

Abstract

Inflammation can lead to hyperalgesia and allodynia by activation or sensitization of peripheral and central nervous system neurons. This study aimed to assess the occurrence of secondary thermal hyperalgesia in patients with symptomatic irreversible pulpitis (SIP). The cold sensitivity test (visual analog scale) was performed for the tooth with SIP, its adjacent sound tooth, the same sound tooth in the opposite jaw, and the contralateral sound tooth in the opposite quadrant of the same jaw. Next, the tooth with SIP underwent root canal treatment, and 3 weeks later, after complete elimination of pain, the teeth underwent cold sensitivity testing again. A total of 64 patients, including 41 women and 23 men 18–65 years old, were evaluated in this study. The response to the cold sensitivity test significantly decreased in the tooth with SIP (P <.001), its adjacent sound tooth (P <.001), and the same sound tooth in the opposite jaw (P =.004) but not in the contralateral sound tooth in the opposite quadrant of the same jaw (P =.45) after endodontic treatment. No significant difference was noted between men and women in the groups (P >.05). Hypersensitivity to cold test due to pulpal inflammation can also result in exaggerated response of the adjacent sound tooth and the same tooth in the opposite jaw to cold sensitivity test; these observations can be explained by the central and peripheral sensitization mechanisms. [ABSTRACT FROM AUTHOR]

Published

2021