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熊果苷与蘑菇酪氨酸酶相互作用的新认识。

New Insight into the Interactions of Arbutin with Mushroom Tyrosinase.

机构信息

National Institute for Genetic Engineering and Biotechnology, P.O. Box: 14965/161, Tehran, Iran.

出版信息

Protein J. 2021 Oct;40(5):689-698. doi: 10.1007/s10930-021-10004-x. Epub 2021 May 28.

Abstract

As a safe substitute for hydroquinone, β-arbutin, a natural plant substance, and its synthetic counterpart, α-arbutin, are used in depigmentation formulations. However, there are debatable points regarding the impact of arbutin on tyrosinase and the pigmentation process. To shed light on this issue, the effects of Pyrus biossieriana leaves extract (PbLE) and β-arbutin, extracted from PbLE, on mushroom tyrosinase (MT) were comprehensively examined. The study was focused on cresolase activity as the characteristic reaction of a tyrosinase. Kinetics studies disclosed that β-arbutin can modulate MT monophenolase activity from inhibition to activation or vice versa. β-Arbutin inhibited L-tyrosine (LTy) oxidation at concentrations < 0.3 mM but it increased (more than 400%) the enzymatic oxidation of L-tyrosine at the concentrations > 0.3 mM. An opposite pattern (activation then inhibition) was observed when a synthetic substrate was used instead of LTy. Computational studies, focused on the heavy chain of MT, indicated that β-arbutin effect could be overruled by the enzyme's ability to provide the ligand with a non-specific binding site (MTPc). A plausible mechanism was presented to show the influence of MTPc on the substrate pose in the active site. The possible determinant correlation between the findings of this research and the current studies on human tyrosinase role in the pigmentation process has been presented.

摘要

作为对氢醌的安全替代品,β-熊果苷,一种天然植物物质及其合成对应物α-熊果苷,被用于美白制剂中。然而,关于熊果苷对酪氨酸酶和色素形成过程的影响存在一些有争议的观点。为了阐明这个问题,本研究全面研究了梨叶提取物(PbLE)和从 PbLE 中提取的β-熊果苷对蘑菇酪氨酸酶(MT)的影响。研究重点是间苯二酚酶活性,作为酪氨酸酶的特征反应。动力学研究表明,β-熊果苷可以调节 MT 单酚酶活性,从抑制变为激活,或者相反。β-熊果苷在浓度<0.3 mM 时抑制 L-酪氨酸(LTy)的氧化,但在浓度>0.3 mM 时,它会增加(超过 400%)L-酪氨酸的酶促氧化。当使用合成底物代替 LTy 时,观察到相反的模式(激活然后抑制)。专注于 MT 重链的计算研究表明,β-熊果苷的作用可以被酶提供配体的非特异性结合位点(MTPc)的能力所推翻。提出了一种合理的机制来显示 MTPc 对活性位点中底物构象的影响。本文提出了这项研究的发现与当前关于人类酪氨酸酶在色素形成过程中作用的研究之间可能存在的决定性关联。

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