皮密莫司
特应性皮炎
丝状蛋白
总苞素
钙调神经磷酸酶
医学
免疫学
洛里克林
皮肤病科
药理学
角质形成细胞
生物
内科学
生物化学
移植
体外
作者
Jens‐Michael Jensen,Andreas Scherer,C. A. Wanke,Matthias Bräutigam,Sandrine Bongiovanni,Martin Letzkus,Frank Staedtler,Jeanne Kehren,Michael Zuehlsdorf,Thomas Schwarz,Michael Weichenthal,Regina Fölster‐Holst,Ehrhardt Proksch
出处
期刊:Allergy
[Wiley]
日期:2011-12-06
卷期号:67 (3): 413-423
被引量:72
标识
DOI:10.1111/j.1398-9995.2011.02747.x
摘要
BACKGROUND: Topical corticosteroids and calcineurin inhibitors are well-known treatments of atopic dermatitis (AD) but differ in their efficacy and side effects. We recently showed that betamethasone valerate (BM) although clinically more efficient impaired skin barrier repair in contrast to pimecrolimus in AD. OBJECTIVE: This study elucidates the mode of action of topical BM and pimecrolimus cream in AD. METHODS: Lesional AD skin samples after topical treatment with either BM or pimecrolimus were subjected to gene expression profile analysis. RESULTS: Betamethasone valerate resulted in a significant reduction in mRNA levels of genes encoding markers of immune cells and inflammation, dendritic cells, T cells, cytokines, chemokines, and serine proteases, whereas pimecrolimus exerted minor effects only. This corroborates the clinical finding that BM reduces inflammation more effectively than pimecrolimus. Genes encoding molecules important for skin barrier function were differently affected. Both BM and pimecrolimus normalized the expression of filaggrin and loricrin. BM, but not pimecrolimus, significantly reduced the expression of rate-limiting enzymes for lipid synthesis and the expression of involucrin and small proline-rich proteins, which covalently bind ceramides. This may explain the lack of restoration of functional stratum corneum layers observed after BM treatment. CONCLUSION: The gene expression profiles are consistent with our previous findings that corticosteroids may exert a more potent anti-inflammatory effect but may impair the restoration of the skin barrier. Corticosteroids are still the main treatment for severe and acutely exacerbated AD; pimecrolimus may be preferable for long-term treatment and stabilization.
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