Literature DB >> 29577089

Mrgprs activation is required for chronic itch conditions in mice.

Yuyan Zhu1, Claire E Hanson1, Qin Liu2, Liang Han1.   

Abstract

INTRODUCTION: Chronic itch has been drawing much attention due to its clinical significance and the complexity of its mechanisms. To facilitate the development of anti-itch strategies, it is necessary to investigate the key players in itch sensation under chronic itch conditions. Several members of the Mrgpr family were identified as itch receptors that detect cutaneous pruritogens in primary sensory neurons. However, the role of Mrgprs in chronic itch conditions has not been well described.
METHODS: Scratching behaviors of WT and Mrgpr-clusterΔ-/- mice were examined in dry skin model and contact dermatitis model to examine the role of Mrgpr genes in mediating chronic itch sensation. Scratching behaviors of the mice were also examined in allergic itch model. Real-time PCR were performed to examine the expression level of MrgprA3 and MrgprC11 under naïve and dry skin conditions. The MrgprA3+ itch-sensing fibers were labeled by tdTomato fluorescence in Mrgpra3GFP-Cre; ROSA26tdTomato mice, and the morphology and density of those fibers in the epidermis were analyzed under dry skin condition.
RESULTS: We showed that deleting a cluster of Mrgpr genes in mice reduced scratching behavior severely under two chronic itch conditions, namely dry skin and contact dermatitis, and the allergic itch condition. Moreover, the gene expressions of itch receptors MrgprA3 and MrgprC11 in dorsal root ganglia (DRG) were upregulated significantly under dry skin condition. Consistently, the percentage of MrgprA3+ itch-sensing neurons was increased as well. We also observed hyperinnervation of MrgprA3+ itch-sensing fibers in the epidermis of the skin under dry skin condition. DISCUSSION: We demonstrate that Mrgprs play important roles in mediating chronic itch and allergic itch. These findings enrich our knowledge of itch mechanism and may lead to the development of novel therapeutic approach to combat itch.

Entities:  

Keywords:  Chronic itch; MrgprA3; MrgprC11; skin

Year:  2017        PMID: 29577089      PMCID: PMC5860675          DOI: 10.1097/itx.0000000000000009

Source DB:  PubMed          Journal:  Itch (Phila)


  44 in total

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Review 8.  Itch mechanisms and circuits.

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Journal:  Annu Rev Biophys       Date:  2014       Impact factor: 12.981

Review 9.  The challenge of cholestatic pruritus.

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Authors:  Henk F Kauffman; Michael Tamm; J André B Timmerman; Peter Borger
Journal:  Clin Mol Allergy       Date:  2006-03-28
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2.  Specific β-Defensins Stimulate Pruritus through Activation of Sensory Neurons.

Authors:  Pang-Yen Tseng; Mark A Hoon
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Review 3.  Peripheral Mechanisms of Itch.

Authors:  Changxiong J Guo; Nathaniel S Grabinski; Qin Liu
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4.  Responses of neurons in the primary somatosensory cortex to itch- and pain-producing stimuli in rats.

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Review 5.  Peripheral and Central Mechanisms of Itch.

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Journal:  Neuron       Date:  2018-05-02       Impact factor: 17.173

6.  S1PR3 Mediates Itch and Pain via Distinct TRP Channel-Dependent Pathways.

Authors:  Rose Z Hill; Takeshi Morita; Rachel B Brem; Diana M Bautista
Journal:  J Neurosci       Date:  2018-08-06       Impact factor: 6.167

7.  Molecular Signature of Pruriceptive MrgprA3+ Neurons.

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8.  Visualizing the Itch-Sensing Skin Arbors.

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9.  TRPC3 Antagonizes Pruritus in a Mouse Contact Dermatitis Model.

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  10 in total

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