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在典型的人体模拟环境中具有优越热稳定性和黑色素脱色效率的重组木质素过氧化物酶。

Recombinant Lignin Peroxidase with Superior Thermal Stability and Melanin Decolorization Efficiency in a Typical Human Skin-Mimicking Environment.

机构信息

School of Energy and Chemical Engineering, Ulsan National Institute of Science and Technology (UNIST), 50, UNIST-gil, Ulsan 44919, Republic of Korea.

Bio Technology Lab, COSMAX BTI R&I Center, Seongnam 13486, Republic of Korea.

出版信息

Biomacromolecules. 2023 Jun 12;24(6):2633-2642. doi: 10.1021/acs.biomac.3c00123. Epub 2023 Apr 19.

Abstract

Recently, the desire for a safe and effective method for skin whitening has been growing in the cosmetics industry. Commonly used tyrosinase-inhibiting chemical reagents exhibit side effects. Thus, recent studies have focused on performing melanin decolorization with enzymes as an alternative due to the low toxicity of enzymes and their ability to decolorize melanin selectively. Herein, 10 different isozymes were expressed as recombinant lignin peroxidases (LiPs) from (PcLiPs), and PcLiP isozyme 4 (PcLiP04) was selected due to its high stability and activity at pH 5.5 and 37 °C, which is close to human skin conditions. In vitro melanin decolorization results indicated that PcLiP04 exhibited at least 2.9-fold higher efficiency than that of well-known lignin peroxidase (PcLiP01) in a typical human skin-mimicking environment. The interaction force between melanin films measured by a surface forces apparatus (SFA) revealed that the decolorization of melanin by PcLiP04 harbors a disrupted structure, possibly interrupting π-π stacking and/or hydrogen bonds. In addition, a 3D reconstructed human pigmented epidermis skin model showed a decrease in melanin area to 59.8% using PcLiP04, which suggests that PcLiP04 exhibits a strong potential for skin whitening.

摘要

近年来,化妆品行业对安全有效的皮肤美白方法的需求不断增长。常用的酪氨酸酶抑制化学试剂存在副作用。因此,最近的研究集中在使用酶进行黑色素脱色作为替代方法,因为酶的毒性低且能够选择性地脱色黑色素。在此,从 (PcLiPs)中表达了 10 种不同的同工酶作为重组木质素过氧化物酶 (LiP),由于其在 pH5.5 和 37°C 时的高稳定性和活性,选择了同工酶 4(PcLiP04),接近人体皮肤条件。体外黑色素脱色结果表明,在典型的模拟人体皮肤环境中,PcLiP04 的效率至少比知名木质素过氧化物酶(PcLiP01)高 2.9 倍。通过表面力仪(SFA)测量的黑色素膜之间的相互作用力表明,PcLiP04 对黑色素的脱色具有破坏结构的作用,可能中断了 π-π 堆积和/或氢键。此外,使用 PcLiP04 的 3D 重建人色素性表皮皮肤模型显示黑色素面积减少到 59.8%,这表明 PcLiP04 具有很强的皮肤美白潜力。

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