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Merck
  • TRPA1 controls inflammation and pruritogen responses in allergic contact dermatitis.

TRPA1 controls inflammation and pruritogen responses in allergic contact dermatitis.

FASEB journal : official publication of the Federation of American Societies for Experimental Biology (2013-06-01)
Boyi Liu, Jasmine Escalera, Shrilatha Balakrishna, Lu Fan, Ana I Caceres, Eve Robinson, Aiwei Sui, M Craig McKay, M Allen McAlexander, Christina A Herrick, Sven E Jordt
要旨

Allergic contact dermatitis is a common skin disease associated with inflammation and persistent pruritus. Transient receptor potential (TRP) ion channels in skin-innervating sensory neurons mediate acute inflammatory and pruritic responses following exogenous stimulation and may contribute to allergic responses. Genetic ablation or pharmacological inhibition of TRPA1, but not TRPV1, inhibited skin edema, keratinocyte hyperplasia, nerve growth, leukocyte infiltration, and antihistamine-resistant scratching behavior in mice exposed to the haptens, oxazolone and urushiol, the contact allergen of poison ivy. Hapten-challenged skin of TRPA1-deficient mice contained diminished levels of inflammatory cytokines, nerve growth factor, and endogenous pruritogens, such as substance P (SP) and serotonin. TRPA1-deficient sensory neurons were defective in SP signaling, and SP-induced scratching behavior was abolished in Trpa1(-/-) mice. SP receptor antagonists, such as aprepitant inhibited both hapten-induced cutaneous inflammation and scratching behavior. These findings support a central role for TRPA1 and SP in the integration of immune and neuronal mechanisms leading to chronic inflammatory responses and pruritus associated with contact dermatitis.

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Sigma-Aldrich
4-エトキシメチレン-2-フェニル-2-オキサゾリン-5-オン, purified by recrystallization
Supelco
4-エトキシメチレン-2-フェニル-2-オキサゾリン-5-オン, analytical standard, for drug analysis