首页> 外文期刊>Nutrients >Topical Application of Trisodium Ascorbyl 6-Palmitate 2-Phosphate Actively Supplies Ascorbate to Skin Cells in an Ascorbate Transporter-Independent Manner
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Topical Application of Trisodium Ascorbyl 6-Palmitate 2-Phosphate Actively Supplies Ascorbate to Skin Cells in an Ascorbate Transporter-Independent Manner

机译:局部应用抗坏血酸6-棕榈酸三钠2-磷酸酯以不依赖于抗坏血酸转运蛋白的方式向皮肤细胞主动提供抗坏血酸。

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摘要

Ascorbic acid (AA) possesses multiple beneficial functions, such as regulating collagen biosynthesis and redox balance in the skin. AA derivatives have been developed to overcome this compound’s high fragility and to assist with AA supplementation to the skin. However, how AA derivatives are transferred into cells and converted to AA in the skin remains unclear. In the present study, we showed that AA treatment failed to increase the cellular AA level in the presence of AA transporter inhibitors, indicating an AA transporter-dependent action. In contrast, torisodium ascorbyl 6-palmitate 2-phosphate (APPS) treatment significantly enhanced the cellular AA level in skin cells despite the presence of inhibitors. In ex vivo experiments, APPS treatment also increased the AA content in a human epidermis model. Interestingly, APPS was readily metabolized and converted to AA in keratinocyte lysates via an intrinsic mechanism. Furthermore, APPS markedly repressed the intracellular superoxide generation and promoted viability associated with an enhanced AA level in Sod1 -deficient skin cells. These findings indicate that APPS effectively restores the AA level and normalizes the redox balance in skin cells in an AA transporter-independent manner. Topical treatment of APPS is a beneficial strategy for supplying AA and improving the physiology of damaged skin.
机译:抗坏血酸(AA)具有多种有益功能,例如调节胶原蛋白的生物合成和皮肤中的氧化还原平衡。已开发出AA衍生物来克服该化合物的高脆性,并有助于向皮肤补充AA。但是,如何将AA衍生物转移到细胞中以及如何在皮肤上转换为AA尚不清楚。在本研究中,我们表明AA处理无法在AA转运蛋白抑制剂存在下增加细胞AA水平,表明AA转运蛋白依赖性作用。相比之下,尽管存在抑制剂,抗坏血酸6-棕榈酸抗坏血酸环己酯2-磷酸酯(APPS)处理仍能显着提高皮肤细胞中的细胞AA水平。在离体实验中,APPS处理还增加了人表皮模型中的AA含量。有趣的是,APPS易于通过内在机制代谢并在角质形成细胞裂解物中转化为AA。此外,APPS显着抑制了细胞内超氧化物的产生,并促进了与Sod1缺乏的皮肤细胞中AA水平升高相关的生存能力。这些发现表明,APPS以独立于AA转运蛋白的方式有效恢复了AA水平,并使皮肤细胞中的氧化还原平衡正常化。 APPS的局部治疗是提供AA和改善受损皮肤生理的有益策略。

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