Chronic itch development in sensory neurons requires BRAF signaling pathways. - Wikidata - awgldk - TriplyDB

Chronic itch development in sensory neurons requires BRAF signaling pathways.

Chronic itch development in sensory neurons requires BRAF signaling pathways.

http://www.wikidata.org/entity/Q30554996

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Why we scratch an itch: the molecules, cells and circuits of itch Neuroimmune interactions in itch: Do chronic itch, chronic pain, and chronic cough share similar mechanisms?Molecular and neural basis of contagious itch behavior in mice.Tlx3 Function in the Dorsal Root Ganglion is Pivotal to Itch and Pain Sensations.Cross-inhibition of NMBR and GRPR signaling maintains normal histaminergic itch transmission TLR4 enhances histamine-mediated pruritus by potentiating TRPV1 activity.Descending control of itch transmission by the serotonergic system via 5-HT1A-facilitated GRP-GRPR signaling Primary afferent and spinal cord expression of gastrin-releasing peptide: message, protein, and antibody concerns A central role for spinal dorsal horn neurons that express neurokinin-1 receptors in chronic itch RAS and downstream RAF-MEK and PI3K-AKT signaling in neuronal development, function and dysfunction Spinal neurons that contain gastrin-releasing peptide seldom express Fos or phosphorylate extracellular signal-regulated kinases in response to intradermal chloroquine.Role of ERK1/2 activation on itch sensation induced by bradykinin B1 activation in inflamed skin.Enhanced itch elicited by capsaicin in a chronic itch model.Critical evaluation of the expression of gastrin-releasing peptide in dorsal root ganglia and spinal cord.IL-33/ST2 signaling excites sensory neurons and mediates itch response in a mouse model of poison ivy contact allergy.B-type natriuretic peptide is neither itch-specific nor functions upstream of the GRP-GRPR signaling pathway Extracellular signal-regulated kinase (ERK) activation is required for itch sensation in the spinal cord.Transmitting pain and itch messages: a contemporary view of the spinal cord circuits that generate gate control.In vitro approaches to pharmacological screening in the field of atopic dermatitis.The Gastrin-Releasing Peptide Receptor (GRPR) in the Spinal Cord as a Novel Pharmacological Target Transmission of pruriceptive signals.Antioxidants Attenuate Acute and Chronic Itch: Peripheral and Central Mechanisms of Oxidative Stress in Pruritus.Spinal Mechanisms of Itch Transmission.Sensory Neurons Co-opt Classical Immune Signaling Pathways to Mediate Chronic Itch.Comparative Anatomy of Gastrin-releasing Peptide Pathways in the Trigeminal Sensory System of Mouse and the Asian House Musk Shrew Suncus murinus.Distinct roles of NMB and GRP in itch transmission.Altered expression of target genes of spinal cord in different itch models compared with capsaicin assessed by RT-qPCR validation.Response to Comment on "Molecular and neural basis of contagious itch behavior in mice".Comment on "Molecular and neural basis of contagious itch behavior in mice".Expression of IL-22 in the Skin Causes Th2-Biased Immunity, Epidermal Barrier Dysfunction, and Pruritus via Stimulating Epithelial Th2 Cytokines and the GRP Pathway.Non-canonical Opioid Signaling Inhibits Itch Transmission in the Spinal Cord of Mice.

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P2860

Chronic itch development in sensory neurons requires BRAF signaling pathways.

http://www.wikidata.org/entity/Q30554996

description

2013 nî lūn-bûn

@nan

2013 թուականի Նոյեմբերին հրատարակուած գիտական յօդուած

@hyw

2013 թվականի նոյեմբերին հրատարակված գիտական հոդված

@hy

2013年の論文

@ja

2013年論文

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2013年論文

@zh-hant

2013年論文

@zh-hk

2013年論文

@zh-mo

2013年論文

@zh-tw

2013年论文

@wuu

name

Chronic itch development in sensory neurons requires BRAF signaling pathways.

@ast

Chronic itch development in sensory neurons requires BRAF signaling pathways.

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type

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Chronic itch development in sensory neurons requires BRAF signaling pathways.

@ast

Chronic itch development in sensory neurons requires BRAF signaling pathways.

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prefLabel

Chronic itch development in sensory neurons requires BRAF signaling pathways.

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Chronic itch development in sensory neurons requires BRAF signaling pathways.

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Journal of Clinical Investigation

P1476

Chronic itch development in sensory neurons requires BRAF signaling pathways.

@en

P2093

Ahu Turkoz

http://www.w3.org/2001/XMLSchema#string

Fu-Quan Huo

http://www.w3.org/2001/XMLSchema#string

Hui Li

http://www.w3.org/2001/XMLSchema#string

James F Battey

http://www.w3.org/2001/XMLSchema#string

Jian Zhong

http://www.w3.org/2001/XMLSchema#string

Joseph Jeffry

http://www.w3.org/2001/XMLSchema#string

Kaijie Ma

http://www.w3.org/2001/XMLSchema#string

Li Wan

http://www.w3.org/2001/XMLSchema#string

Lori Hampton

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Lynn A Cornelius

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P2860

Skin-derived TSLP triggers progression from epidermal-barrier defects to asthma

Cellular basis of itch sensation

The capsaicin receptor: a heat-activated ion channel in the pain pathway

Unidirectional cross-activation of GRPR by MOR1D uncouples itch and analgesia induced by opioids

Mechanisms of regulating the Raf kinase family

The neurobiology of itch

Neuromedin B and gastrin-releasing peptide mRNAs are differentially distributed in the rat nervous system

Lmx1b is required for maintenance of central serotonergic neurons and mice lacking central serotonergic system exhibit normal locomotor activity

The multiple pathways for itch and their interactions with pain

Mitogen-activated protein (MAP) kinase pathways: regulation and physiological functions

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4769-4780

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11

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123

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3809799

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