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洋葱伯克霍尔德菌脂肪酶在水-有机界面激活的分子机制。

Molecular mechanism of activation of Burkholderia cepacia lipase at aqueous-organic interfaces.

作者信息

de Oliveira Ivan Pires, Jara Gabriel Ernesto, Martínez Leandro

机构信息

Institute of Chemistry and Center for Computational Engineering & Science, University of Campinas, Campinas, SP, Brazil.

出版信息

Phys Chem Chem Phys. 2017 Nov 29;19(46):31499-31507. doi: 10.1039/c7cp04466f.

Abstract

Lipases are water-soluble enzymes that catalyze the hydrolysis of lipids. Since lipids are mostly hydrophobic, lipase activity occurs preferentially at interfaces of aqueous and organic phases. In this work, we study the molecular mechanisms by which the Burkholderia cepacia lipase (BCL) is activated at interfaces of water with octane and with methyl caprylate (CAME). We show that BCL assumes very rapidly a preferential orientation at the interfaces, in which the active site is exposed to the organic phase. With BCL oriented to the interface, we compute the free energy of the aperture of the catalytic pocket using Adaptive Biasing Force MD simulations. The exposure to the organic phase promotes a clear stabilization of the open form of the catalytic pocket relative to the enzyme in water. This stabilization stems from the hydrophobicity of domains U1 and U2, which allows the penetration of organic solvents into the catalytic cleft impeding the closure of the pocket. Our results suggest that the structure and hydrophobicity of BCL are optimized for its activation in biphasic systems through the regulation of the accessibility of the catalytic pocket by, and for, hydrophobic substrates. The understanding of this mechanism may be useful for the design of proteins with targeted activation.

摘要

脂肪酶是催化脂质水解的水溶性酶。由于脂质大多具有疏水性,脂肪酶活性优先发生在水相和有机相的界面处。在这项工作中,我们研究了洋葱伯克霍尔德菌脂肪酶(BCL)在水与辛烷以及水与辛酸甲酯(CAME)界面处被激活的分子机制。我们表明,BCL在界面处非常迅速地呈现出一种优先取向,其中活性位点暴露于有机相。在BCL定向于界面的情况下,我们使用自适应偏置力分子动力学模拟计算催化口袋开口的自由能。相对于在水中的酶,暴露于有机相促进了催化口袋开放形式的明显稳定。这种稳定源于结构域U1和U2的疏水性,这使得有机溶剂能够渗透到催化裂隙中,从而阻碍口袋关闭。我们的结果表明,BCL的结构和疏水性通过调节催化口袋对疏水底物的可及性以及疏水底物对催化口袋的可及性,在双相系统中针对其激活进行了优化。对这一机制的理解可能有助于设计具有靶向激活功能的蛋白质。

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