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Topical application of ST266 reduces UV-induced skin damage

机译:ST266的局部应用可减少紫外线引起的皮肤损伤

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Ultraviolet radiation (UVR) has a significant impact on human skin and is the major environmental factor for skin cancer formation. It is also believed that 80% of the signs of skin aging are attributed to UVR. UVR induces inflammatory changes in the skin via the increase in oxidative stress, DNA damage vascular permeability, and fluctuation in a myriad of cytokines. Acutely, UVR causes skin inflammation and DNA damage, which manifest as sunburn (erythema). ST266 is the secretome of proprietary amnion-derived cells that have been shown to reduce inflammation and accelerate healing of various wounds by promoting migration of keratinocytes and fibroblasts in preclinical animal studies. We hypothesized that ST266 has anti-inflammatory effects that can be used to reduce ultraviolet (UV) erythema and markers of inflammation. In this study, we examined the in vivo effects of ST266 on post UV-irradiated skin by measuring erythema, level of cyclobutane pyrimidine dimer (CPD), and expression level of xeroderma pigmentosum, complementation group A (XPA). We demonstrated that ST266 has the potential to reduce the acute effects of UV-induced skin damage when applied immediately after the initial exposure. In addition, ST266 is shown to reduce erythema, increase XPA DNA repair protein, and decrease damaged DNA.
机译:紫外线(UVR)对人体皮肤有重大影响,并且是皮肤癌形成的主要环境因素。还据信皮肤老化的迹象的80%归因于UVR。 UVR通过氧化应激的增加,DNA损伤血管的通透性以及多种细胞因子的波动来诱导皮肤的炎症变化。急性紫外线辐射会引起皮肤发炎和DNA损伤,表现为晒伤(红斑)。 ST266是专有羊膜来源细胞的分泌基因组,在临床前动物研究中,ST266已显示出通过促进角质形成细胞和成纤维细胞的迁移来减少炎症并加速各种伤口的愈合。我们假设ST266具有抗炎作用,可用于减少紫外线(UV)红斑和炎症标志物。在这项研究中,我们通过测量红斑,环丁烷嘧啶二聚体(CPD)的水平和干燥性色素皮肤的表达水平(补充组A(XPA)),检查了ST266对紫外线照射后皮肤的体内作用。我们证明,在初次暴露后立即使用ST266,有可能减少紫外线引起的皮肤损伤的急性影响。此外,ST266还可以减少红斑,增加XPA DNA修复蛋白并减少受损的DNA。

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