基于同源建模和分子对接的酪氨酸酶活性抑制效应评估

Q2 Biochemistry, Genetics and Molecular Biology

Enzyme Research Pub Date : 2015-12-15 DOI:10.1155/2015/262364

Daungkamon Nokinsee, L. Shank, V. Lee, P. Nimmanpipug

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引用次数: 33

摘要

酪氨酸酶是黑色素形成的关键酶。通常，双孢蘑菇酪氨酸酶被用作化妆品行业皮肤增白剂试验的模型。最近获得的巨型芽孢杆菌酪氨酸酶晶体结构与人酪氨酸酶具有较高的相似性(33.5%)，可作为构建人酪氨酸酶模型的模板。通过自动对接计算模拟酪氨酸酶与一系列抑制剂的结合。对接和MD模拟结果表明，N81、N260、H263和M280参与了抑制剂与蘑菇酪氨酸酶的结合。E195和H208是细菌酪氨酸酶中重要的残基，而E230、S245、N249、H252、V262和S265与抑制剂结合，在人酪氨酸酶中形成pi相互作用中起重要作用。

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Estimation of Inhibitory Effect against Tyrosinase Activity through Homology Modeling and Molecular Docking

Tyrosinase is a key enzyme in melanogenesis. Generally, mushroom tyrosinase from A. bisporus had been used as a model in skin-whitening agent tests employed in the cosmetic industry. The recently obtained crystal structure of bacterial tyrosinase from B. megaterium has high similarity (33.5%) to the human enzyme and thus it was used as a template for constructing of the human model. Binding of tyrosinase to a series of its inhibitors was simulated by automated docking calculations. Docking and MD simulation results suggested that N81, N260, H263, and M280 are involved in the binding of inhibitors to mushroom tyrosinase. E195 and H208 are important residues in bacterial tyrosinase, while E230, S245, N249, H252, V262, and S265 bind to inhibitors and are important in forming pi interaction in human tyrosinase.

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来源期刊

Enzyme Research Biochemistry, Genetics and Molecular Biology-Biochemistry

CiteScore

4.60

自引率

0.00%

发文量