Sensory TRP channels contribute differentially to skin inflammation and persistent itch

Feng, Jing; Pu, Yang; Mack, Madison R.; Dryn, Dariia O.; Luo, Jialie; Gong, Xuan; Liu, Shenbin; Oetjen, Landon K.; Zholos, Alexander; Mei, Zhinan; Yin, Shen; Kim, Brian; Hu, Hongzhen

doi:10.1038/s41467-017-01056-8

Cited by 121 publications

(110 citation statements)

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“…In addition to sensing immune molecules and pathogens, afferent neurons actively modulate immune responses and inflammation, as demonstrated in experimental IBD (46), arthritis (48), asthma (60), skin inflammation and chronic itch (61, 62), and bacterial infection (3, 42). Sensory neurons release substance P (SP), calcitonin gene-related peptide (CGRP), vasoactive intestinal peptide (VIP), and other molecules interacting with the endothelium, neutrophils, macrophages, and other immune cells in the vicinity of axonal terminals (3, 42, 63) (Figure 2).…”

Section: Functional Neuroanatomy For Communication With the Immune Symentioning

confidence: 99%

Molecular and Functional Neuroscience in Immunity

Pavlov

Chavan

Tracey

2018

Annu. Rev. Immunol.

342

320

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The nervous system regulates immunity and inflammation. The molecular detection of pathogen fragments, cytokines, and other immune molecules by sensory neurons generates immunoregulatory responses through efferent autonomic neuron signaling. The functional organization of this neural control is based on principles of reflex regulation. Reflexes involving the vagus nerve and other nerves have been therapeutically explored in models of inflammatory and autoimmune conditions, and recently in clinical settings. The brain integrates neuro-immune communication, and brain function is altered in diseases characterized by peripheral immune dysregulation and inflammation. Here we review the anatomical and molecular basis of the neural interface with immunity, focusing on peripheral neural control of immune functions and the role of the brain in the model of the immunological homunculus. Clinical advances stemming from this knowledge within the framework of bioelectronic medicine are also briefly outlined.

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Section: Functional Neuroanatomy For Communication With the Immune Symentioning

confidence: 99%

Molecular and Functional Neuroscience in Immunity

Pavlov

Chavan

Tracey

2018

Annu. Rev. Immunol.

342

320

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“…Current research suggests that TRPV1 is involved in itch, and therefore, activation of these neurons may still confer itch transmission (Feng et al, ; Fukuyama, Ganchingco, Mishra, et al, ). Additionally, TRPA1 was shown to be necessary for itch transmission (Feng et al, ). Furthermore, substance P was shown to be biologically active on a pruriceptor and the NK‐1 receptor involved in itch transmission (Akiyama et al, , ; Azimi et al, ).…”

Section: Discussionmentioning

confidence: 99%

“…However, similar to previous studies there is a significant proportion of neurons responsive to a pruritogen and capsaicin concluding concurrent expression of pruriceptors and TRPV1 on these peripheral sensory neurons, demonstrating there are not separate pain and itch sensory neurons (Akiyama et al, 2010a(Akiyama et al, , 2012Akiyama, Merrill, Carstens, & Carstens, 2009;Akiyama, Tominaga, Takamori, Carstens, & Carstens, 2014;Gold, Dastmalchi, & Levine, 1996;Lu, Zhang, & Gold, 2006;Nakagawa & Hiura, 2013). Current research suggests that TRPV1 is involved in itch, and therefore, activation of these neurons may still confer itch transmission (Feng et al, 2017;Fukuyama, Ganchingco, Mishra, et al, 2017b). Additionally, TRPA1 was shown to be necessary for itch transmission (Feng et al, 2017).…”

Section: Discussionmentioning

confidence: 99%

“…This study aims to incorporate both itch and pain transmission by exposure of sensory neurons to agonists that are determined to be either pruritogenic through histamine‐dependent pathways (histamine) and histamine‐independent pathways (chloroquine, bovine adrenal medulla peptide, canine protease‐activated receptor 2 activating peptide, compound 48/80, and 5‐hydroxytryptamine) or algogenic (substance P, allyl isothiocyanate, capsaicin) (Akiyama & Carstens, ; Akiyama, Carstens, & Carstens, ; Davidson et al, ; Han et al, ; Metz, Grundmann, & Stander, ; Nakagawa & Hiura, ; Ohtori et al, ; Paus et al, ; Schemann et al, ; Valtcheva et al, ). The distinction of these algogenic substances only involved in pain has become less clear as current research has also shown their receptors associated with inducing itch and an off‐target activation of a pruriceptor by substance P (Akiyama et al, ; Azimi et al, ; Feng et al, ; Fukuyama, Ganchingco, Mishra, et al, ; Ständer & Yosipovitch, ). Receptors for these agonists are mainly G protein‐coupled receptors, including tachykinin receptor‐1, histamine‐1 receptor, sensory neuron receptor, protease‐activated receptor 2, and mas‐related G protein‐coupled receptors (Mrgprs).…”

Section: Introductionmentioning

confidence: 99%

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Calcium imaging of primary canine sensory neurons: Small‐diameter neurons responsive to pruritogens and algogens

et al. 2019

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IntroductionRodent primary sensory neurons are commonly used for studying itch and pain neurophysiology, but translation from rodents to larger mammals and humans is not direct and requires further validation to make correlations.MethodsThis study developed a primary canine sensory neuron culture from dorsal root ganglia (DRG) excised from cadaver dogs. Additionally, the canine DRG cell cultures developed were used for single‐cell ratiometric calcium imaging, with the activation of neurons to the following pruritogenic and algogenic substances: histamine, chloroquine, canine protease‐activated receptor 2 (PAR2) activating peptide (SLIGKT), compound 48/80, 5‐hydroxytryptamine receptor agonist (5‐HT), bovine adrenal medulla peptide (BAM8‐22), substance P, allyl isothiocyanate (AITC), and capsaicin.ResultsThis study demonstrates a simple dissection and rapid processing of DRG collected from canine cadavers used to create viable primary sensory neuron cultures to measure responses to pruritogens and algogens.ConclusionRatiometric calcium imaging demonstrated that small‐diameter canine sensory neurons can be activated by multiple stimuli, and a single neuron can react to both a pruritogenic stimulation and an algogenic stimulation.

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“…Cytokine receptors directly associated with itch are the IL‐4 receptor α (IL‐4R α), IL‐31 receptor, oncostatin M receptor (OSMR) and the thymic stromal lymphopoietin (TSLP) receptor . Additionally, some ion channels such as voltage‐gated sodium channel (NaV1.7) and the transient receptor potential (TRP) channels TrpV1 and TrpA1 have been shown to be involved in the transmission of itch signals …”

Section: Potential Targets In Chronic Pruritusmentioning

confidence: 99%

Treatments for chronic pruritus outside of the box

Metz

2019

Experimental Dermatology

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Patients with chronic pruritus are in desperate need of novel treatment options, as current therapeutic possibilities are often not effective, have a poor level of evidence and are mostly off‐label. In recent years, much effort has been put into the identification of potential targets for the treatment of chronic pruritus. More importantly, a number of promising new drugs that are aimed at treating pruritus in different conditions are currently in advanced stages of clinical trials. Here, current pharmacological developments leading to potential new drugs for the treatment of chronic pruritus within various conditions are summarized. Hopefully, these new approaches will result in effective and safe therapies for our patients with chronic pruritus associated with dermatological or non‐dermatological diseases in the near future.

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Sensory TRP channels contribute differentially to skin inflammation and persistent itch

Cited by 121 publications

References 59 publications

Molecular and Functional Neuroscience in Immunity

Molecular and Functional Neuroscience in Immunity

Calcium imaging of primary canine sensory neurons: Small‐diameter neurons responsive to pruritogens and algogens

Treatments for chronic pruritus outside of the box

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