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协同漆酶-过氧化物酶酶复合物有效降解黑色素,用于皮肤增白和其他实际应用。

Effective melanin degradation by a synergistic laccase-peroxidase enzyme complex for skin whitening and other practical applications.

机构信息

Department of Biotechnology, Korea University, Seoul, Republic of Korea.

Department of Biotechnology, Korea University, Seoul, Republic of Korea; Department of Food Science and Biotechnology, College of Knowledge-Based Services Engineering, Sungshin Women's University, Seoul, Republic of Korea; Department of Food and Nutrition, College of Health & Wellness, Sungshin Women's University, Seoul, Republic of Korea.

出版信息

Int J Biol Macromol. 2019 May 15;129:181-186. doi: 10.1016/j.ijbiomac.2019.02.027. Epub 2019 Feb 7.

Abstract

Melanin is major cause of dark skin, which is regarded as social status in eastern Asia. As a result, researchers in cosmetic industries are developing skin whitening agents. Melanin can be decolorized by many oxidative enzymes. Laccase (CueO) from Escherichia coli and dye-decolorizing peroxidase (DyP) from Bacillus subtilis were merged with the dockerin domain of endoglucanase B from Clostridium cellulovorans. Scaffoldin has great potential to exert structural benefits that enable complementary enzyme effects. The carbohydrate binding module (CBM) in scaffoldin was replaced with the melanin binding peptide (MBP) to increase melanin binding and thereby enhance melanin degradation. The modified scaffoldin exhibits a nearly 64% increase in specific binding to melanin over that of the native scaffoldin. Laccase was used to degrade melanin via the production of hydrogen peroxide, which produced synergistic activity with peroxidase. The activity of the optimized complex was approximately 6.4-fold greater than that of laccase alone. This enzyme complex can also reduce the number of melanin granules in corneocytes. Based on these results, a recombinant enzyme complex is suitable for use in melanin degradation by next generation whitening agents in the skin cosmetics industry.

摘要

黑色素是导致皮肤黝黑的主要原因,而在东亚地区,皮肤黝黑被视为社会地位的象征。因此,化妆品行业的研究人员正在开发美白产品。许多氧化酶可以使黑色素褪色。将大肠杆菌的漆酶(CueO)和枯草芽孢杆菌的染料脱色过氧化物酶(DyP)与纤维二糖水解酶 B 的 dockerin 结构域融合。支架蛋白具有发挥结构优势的潜力,从而实现互补酶的协同作用。支架蛋白中的碳水化合物结合模块(CBM)被黑色素结合肽(MBP)取代,以增加黑色素结合,从而增强黑色素降解。与天然支架蛋白相比,修饰后的支架蛋白对黑色素的特异性结合增加了近 64%。漆酶通过产生过氧化氢来降解黑色素,而过氧化酶则产生协同作用。优化后的复合物的活性比单独使用漆酶时高出约 6.4 倍。该酶复合物还可以减少角蛋白细胞中的黑色素颗粒数量。基于这些结果,重组酶复合物适合用于下一代美白产品中的黑色素降解,以应用于皮肤化妆品行业。

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