Involvement of TRPM2 in a wide range of inflammatory and neuropathic pain mouse models

So, Kanako; Haraguchi, Kayo; Asakura, Kayoko; Isami, Koichi; Sakimoto, Shinya; Shirakawa, Hisashi; Mori, Yasuo; Nakagawa, Takayuki; Kaneko, Shuji

doi:10.1016/j.jphs.2014.10.003

Cited by 32 publications

(21 citation statements)

References 54 publications

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“…Intraplantar injection of H 2 O 2 caused brief nociceptive pain [19], but specific subcutaneous versus deep tissue injections were not studied and would be difficult in such small spaces like the hind paw. In other previous studies, after intraplantar injection of H 2 O 2 , nociceptive behavior was short-lasting (< 5 min), which is consistent with our finding after subcutaneous injection over the gastrocnemius [30, 33, 34]. In humans, cutaneous wounds are frequently flushed or rinsed with much higher concentrations of H 2 O 2 (880 mM concentration of commercially-available 3% H 2 O 2 ).…”

Section: Discussionsupporting

confidence: 92%

Muscle Reactive Oxygen Species (ROS) Contribute to Post-Incisional Guarding via the TRPA1 Receptor

2017

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BackgroundDeep tissues and their afferents have unique responses to various stimuli and respond to injury distinctively. However, the types of receptors and endogenous ligands that have a key role in pain after deep tissue incision are unknown. TRPA1 has been shown to mediate pain-related responses in inflammation- and nerve injury-induced pain models. We hypothesized that TRPA1 has an important role in pain behaviors after deep tissue incision.MethodsThe effect of various doses of intraperitoneal (i.p.) TRPA1 antagonist, HC-030031, on pain behaviors after skin + deep tissue incision of the rat hind paw was measured. In vivo reactive oxygen species (ROS)-imaging and hydrogen peroxide (H2O2) levels after incision were also evaluated. Separate groups of rats were examined for H2O2-evoked pain-related behaviors after injections into the deep tissue or the subcutaneous tissue.ResultsGuarding pain behavior after skin + deep tissue incision was decreased by i.p. HC-030031. However, HC-030031 did not affect mechanical or heat responses after incision. Treatment either before or after incision was effective against incision-induced guarding behavior. ROS increased after skin + deep tissue incision in both the incised muscle and the skin. Tissue H2O2 also increased in both skin and muscle after incision. H2O2 injection produced pain behaviors when injected into muscle but not after subcutaneous injection.ConclusionsThis study demonstrates that TRPA1 antagonist HC-030031 reduced spontaneous guarding pain behavior after skin + deep tissue incision. These data indicate that TRPA1 receptors on nociceptors are active in incised fascia and muscle but this is not evident in incised skin. Even though endogenous TRPA1 agonists like ROS and H2O2 were increased in both incised skin and muscle, those in skin do not contribute to nociceptive behaviors. This study suggests that endogenous TRPA1 ligands and the TRPA1 receptor are important targets for acute pain from deep tissue injury.

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Section: Discussionsupporting

confidence: 92%

Muscle Reactive Oxygen Species (ROS) Contribute to Post-Incisional Guarding via the TRPA1 Receptor

2017

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“…Microglial/Macrophagic TRPM2 Channels in Neuropathic Pain TRPM2 is thought to be involved in a range of pathological pain states, including neuropathic pain. 31,36,37) Evidence suggests that peripheral and spinal neuroinflammation mediated by the interaction between nociceptive neurons and immune/glial cells plays a pivotal role in neuropathic pain. 38) After peripheral nerve injury, pro-nociceptive inflammatory mediators, such as pro-inflammatory cytokines, chemokines, and excess ROS produced by peripheral tissues and the spinal cord, can lead to peripheral and central sensitization of nociceptive neurons.…”

Section: Physiological Roles Of Trpm Channels In Gliamentioning

confidence: 99%

“…36) Consequently, TRPM2 is involved in a wide range of pathological pain states induced by peripheral and spinal neuroinflammation-such as inflammatory pain, osteoarthritic pain, neuropathic pain induced by peripheral nerve injury, chemotherapy-induced peripheral neuropathy, and painful diabetic neuropathy-rather than in physiological nociceptive pain. 37) …”

Section: Physiological Roles Of Trpm Channels In Gliamentioning

confidence: 99%

Physiological and Pathophysiological Roles of Transient Receptor Potential Channels in Microglia-Related CNS Inflammatory Diseases

Shirakawa

Kaneko

2018

Biological & Pharmaceutical Bulletin

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Central nervous system (CNS) inflammation is a potential therapeutic target for neurodegenerative diseases. In recent years, a number of studies have focused on the links between neurodegenerative diseases and CNS glial cells, especially microglia. Microglia are the main resident immune cells in the CNS and represent approximately 10-15% of all CNS cells. Microglia play an important role in maintaining brain homeostasis at rest by surveying the environment, and engulfing apoptotic cells and debris in the healthy brain. However, under certain pathological conditions, microglia can generate neurotoxic factors, such as pro-inflammatory cytokines and molecules like nitric oxide (NO), which lead to CNS inflammatory diseases. In this review, we discuss the evidence that regulation of microglial ion channels may modulate CNS inflammation and subsequent tissue damage in neurological disorders. In particular, we discuss the role of transient receptor potential (TRP) channels in microglia in both acute and chronic inflammatory conditions, and describe the physiological and pathophysiological roles of TRP channels in CNS inflammatory pathways. Additionally, we describe the benefits of stimulation/inhibition of TRP channels in animal models of microglia-related CNS inflammatory diseases.

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“…TRPM2 also activates ERK MAPK and induces nuclear translocation of NFκB, resulting in production of proinflammatory cytokines and chemokines [76,77,81,83,84]. Consequently, pharmacological and genetic studies have demonstrated that TRPM2 contributes to inflammatory and neuropathic nociceptive hypersensitivity [77–79,82,85]. …”

Section: Mechanisms Of Nitroxidative Signaling In Neuronal Hyperexcitmentioning

confidence: 99%

Nitroxidative Signaling Mechanisms in Pathological Pain

Grace

Gaudet

Staikopoulos

et al. 2016

Trends in Neurosciences

102

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Tissue injury can initiate bidirectional signaling between neurons, glia and immune cells that creates and amplifies pain. While the ability for neurotransmitters, neuropeptides, and cytokines to initiate and maintain pain has been extensively studied, recent work has identified a key role for reactive oxygen and nitrogen species (nitroxidative species), including superoxide, peroxynitrite, and hydrogen peroxide. In this review, we describe how nitroxidative species are generated after tissue injury, and the mechanisms by which they enhance neuroexcitability in pain pathways. Finally, we discuss potential therapeutic strategies for normalizing nitroxidative signaling, which may also enhance opioid analgesia, to help to alleviate the enormous burden of pathological pain.

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Involvement of TRPM2 in a wide range of inflammatory and neuropathic pain mouse models

Cited by 32 publications

References 54 publications

Muscle Reactive Oxygen Species (ROS) Contribute to Post-Incisional Guarding via the TRPA1 Receptor

Muscle Reactive Oxygen Species (ROS) Contribute to Post-Incisional Guarding via the TRPA1 Receptor

Physiological and Pathophysiological Roles of Transient Receptor Potential Channels in Microglia-Related CNS Inflammatory Diseases

Nitroxidative Signaling Mechanisms in Pathological Pain

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