首页> 外文期刊>European Journal of Pharmacology: An International Journal >Tacrolimus hydrate ointment inhibits skin plasma extravasation in rats induced by topical m-xylene but not capsaicin.
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Tacrolimus hydrate ointment inhibits skin plasma extravasation in rats induced by topical m-xylene but not capsaicin.

机译:他克莫司水合物软膏抑制局部间二甲苯而不是辣椒素诱导的大鼠皮肤血浆外渗。

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摘要

Tacrolimus ointment is used to treat various chronic inflammatory skin diseases. However, the effect of this ointment on acute neurogenic inflammation in the skin remains to be fully elucidated. Topical capsaicin and m-xylene produce tachykinin release from sensory nerves in the skin, resulting in skin plasma leakage. We investigated the effect of tacrolimus ointment (0.1%) on skin microvascular leakage induced by topical capsaicin (10 mM) and m-xylene (neat), and intracutaneous compound 48/80 (c48/80) (10 microg/ml, 50 microl/site) in two groups of rats pretreated with excessive capsaicin or its vehicle. The amount of leaked Evans blue dye reflected skin plasma leakage. Capsaicin, m-xylene or c48/80 was applied to the shaved abdomens of rats 8 h after topical application of tacrolimus ointment or its base. Desensitization with capsaicin reduced the skin response to capsaicin and m-xylene by 100% and 65%, respectively, but not to c48/80. Tacrolimus ointment significantly inhibited the skin response induced by m-xylene and c48/80, regardless of pretreatment with capsaicin. However, topical tacrolimus did not influence the skin response induced by capsaicin. We also evaluated whether topical capsaicin and m-xylene, and intracutaneous c48/80 cause mast cell degranulation in skin treated with tacrolimus. Mast cell degranulation was microscopically assessed. Topical tacrolimus only significantly suppressed degranulation induced by m-xylene and c48/80. Our data shows that tacrolimus ointment partially inhibits plasma leakage and mast cell degranulation in rat skin induced by m-xylene and c48/80 but not capsaicin, suggesting that the inhibitory effect is not associated with a reduction in neurogenic-mediated mechanisms.
机译:他克莫司软膏用于治疗各种慢性炎症性皮肤病。然而,该药膏对皮肤中急性神经源性炎症的作用尚待充分阐明。局部辣椒素和间二甲苯会从皮肤的感觉神经释放速激肽,导致皮肤血浆渗漏。我们研究了他克莫司软膏(0.1%)对局部辣椒素(10 mM)和间二甲苯(纯)和皮内化合物48/80(c48 / 80)(10 microg / ml,50微升)引起的皮肤微血管渗漏的影响/位)在过量的辣椒素或其媒介物预处理的两组大鼠中。埃文斯蓝色染料的泄漏量反映了皮肤血浆泄漏。局部应用他克莫司软膏或其基质8小时后,将辣椒素,间二甲苯或c48 / 80应用于大鼠剃毛腹部。用辣椒素脱敏可将皮肤对辣椒素和间二甲苯的反应分别降低100%和65%,但对c48 / 80则没有。他克莫司软膏可显着抑制间二甲苯和c48 / 80诱导的皮肤反应,而与辣椒素预处理无关。然而,局部他克莫司不影响辣椒素诱导的皮肤反应。我们还评估了局部用辣椒素和间二甲苯以及皮内c48 / 80是否导致他克莫司治疗的皮肤肥大细胞脱粒。用显微镜评估肥大细胞脱粒。他克莫司局部用药只能显着抑制间二甲苯和c48 / 80引起的脱粒。我们的数据表明,他克莫司软膏部分抑制间苯二酚和c48 / 80诱导的大鼠皮肤血浆渗漏和肥大细胞脱粒,但不抑制辣椒素,这表明抑制作用与神经源性介导机制的减少无关。

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