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首页> 外文期刊>Acta Dermato-Venereologica >Effect of intradermal injection of methionine-enkephalin on human skin.
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Effect of intradermal injection of methionine-enkephalin on human skin.

机译:皮内注射甲硫氨酸脑啡肽对人皮肤的影响。

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摘要

Methionine-enkephalin (met-enk) detected in monocytes in psoriatic skin can modulate inflammatory processes and keratinocyte differentiation/proliferation in vitro. The purpose of the present study was to determine the effect of intradermal injection of met-enk on normal human skin and on the development of a delayed type skin hypersensitivity reaction. In 6 healthy volunteers, 50 microl of met-enk (16, 30, and 45 nmol) was injected once in the forearm and the reaction was evaluated clinically and by video-optical recording for 120 min. Compared to vehicle (0.9% saline), met-enk induced a time- and dose-dependent flare reaction, but no significant stimulation of a weal reaction. The flare reaction was maximal after 1 min and disappeared within 45 min. Pre-treatment with the antihistamine cetirizine reduced the flare reaction. Furthermore, the effect of met-enk on lymphocyte/monocyte infiltration and epidermal proliferation in normal skin and on a delayed type skin hypersensitivity reaction was assessed. Met-enk (45 nmol/ 50 microl) was injected at 0, 24 and 48 h. In normal skin, met-enk increased the number of dermal lymphocytes/monocytes (CD3/CD68 positive cells) and the degree of epidermal proliferation (MIBI-Ki67). In a delayed type hypersensitivity reaction induced by tuberculin (PPD), the degree of epidermal proliferation and the number of infiltrating lymphocytes/monocytes were reduced compared to PPD alone. Our study suggests that intradermal injection of met-enk in normal human skin induces an inflammatory reaction that may involve the release of histamine. In contrast, met-enk seems to down-regulate the development of a delayed type skin hypersensitivity reaction. These results may indicate that the direction of the effect of the opioid peptide met-enk on human skin depends on the rate of epidermal proliferation and the activity of immunocompetent cells.
机译:银屑病皮肤单核细胞中检测到的蛋氨酸脑啡肽(met-enk)可以调节炎症过程和体外角质形成细胞的分化/增殖。本研究的目的是确定皮内注射met-enk对正常人皮肤和延迟型皮肤超敏反应的发展的影响。在6名健康志愿者中,将50微升met-enk(16、30和45 nmol)注射到前臂一次,并通过临床和120分钟的视频录像来评估反应。与媒介物(0.9%的盐水)相比,met-enk引起了时间和剂量依赖性的耀斑反应,但没有明显刺激食欲反应。 1分钟后,耀斑反应达到最大,并在45分钟内消失。用抗组胺西替利嗪预处理可减少耀斑反应。此外,评估了met-enk对正常皮肤中淋巴细胞/单核细胞浸润和表皮增殖以及对延迟型皮肤超敏反应的影响。在0、24和48小时注射Met-enk(45nmol / 50微升)。在正常皮肤中,met-enk增加了真皮淋巴细胞/单核细胞(CD3 / CD68阳性细胞)的数量和表皮增殖的程度(MIBI-Ki67)。在结核菌素(PPD)诱导的迟发型超敏反应中,与单独使用PPD相比,表皮增殖程度和浸润淋巴细胞/单核细胞数量减少。我们的研究表明,在正常人的皮肤中皮内注射met-enk会引起炎症反应,可能涉及组胺的释放。相反,met-enk似乎下调了迟发型皮肤超敏反应的发生。这些结果可能表明阿片样肽met-enk对人皮肤的作用方向取决于表皮增殖的速率和免疫活性细胞的活性。

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