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首页> 外文期刊>Photochemical & photobiological sciences: the official journal of the European Photochemistry Association and the European Society for Photobiology >Integrating targeted gene expression and a skin model system to identify functional inhibitors of the UV activated p38 MAP kinase
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Integrating targeted gene expression and a skin model system to identify functional inhibitors of the UV activated p38 MAP kinase

机译:整合靶向基因表达和皮肤模型系统,以鉴定紫外线激活的p38 MAP激酶的功能抑制剂

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摘要

The stress-activated p38 alpha MAP Kinase is an integral and critical component of the UV-induced inflammatory response. Despite the advances in recent years in the development of p38 kinase inhibitors, validation of these compounds in the diseased models remains limited. Based on the pharmacological profile of p38a inhibitor lead compound, SB203580, we synthesized a series of pyrrole-derivatives. Using UV-irradiated human skin punch-biopsies and cell cultures, we identified and validated the inhibitory activity of the derivatives by quantitatively measuring their effect on the expression of p38a target genes using realtime PCR. This approach not only identified pyrrole-2 as a unique derivative of this series that specifically inhibited the UV-activated p38a kinase, but also documented the skin permeation, bioavailability and reversible properties of this derivative in a 3D structure. The successful skin permeation of pyrrole-2 and its impact on AREG, COX-2 and MMP-9 gene expression demonstrates its potential use in modulating inflammatory processes in the skin. This study underscored the importance of using adapted biological models to identify accurate bioactive compounds.
机译:应激激活的p38αMAP激酶是紫外线诱导的炎症反应的重要组成部分。尽管近年来在p38激酶抑制剂的开发方面取得了进展,但是在患病模型中对这些化合物的验证仍然有限。根据p38a抑制剂先导化合物SB203580的药理特性,我们合成了一系列吡咯衍生物。通过使用紫外线辐射的人类皮肤穿刺活检和细胞培养,我们通过使用实时PCR定量测量其对p38a靶基因表达的影响,鉴定并验证了其抑制活性。这种方法不仅将吡咯2确定为该系列的独特衍生物,该衍生物可特异性抑制UV激活的p38a激酶,而且还证明了该衍生物在3D结构中的皮肤渗透性,生物利用度和可逆特性。吡咯2的成功的皮肤渗透及其对AREG,COX-2和MMP-9基因表达的影响表明其潜在地用于调节皮肤的炎症过程。这项研究强调了使用适应性生物学模型来鉴定准确的生物活性化合物的重要性。

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