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疏水蛋白的固相处理:固定化疏水蛋白作为研究脂肪酶的新工具。

Solid-phase handling of hydrophobins: immobilized hydrophobins as a new tool to study lipases.

作者信息

Palomo José M, Peñas María M, Fernández-Lorente Gloria, Mateo César, Pisabarro Antonio G, Fernández-Lafuente Roberto, Ramírez Lucía, Guisán José M

机构信息

Departamento de Biocatálisis, Instituto de Catálisis, CSIC, Campus Universidad Autonóma, Cantoblanco, 28049 Madrid, Spain.

出版信息

Biomacromolecules. 2003 Mar-Apr;4(2):204-10. doi: 10.1021/bm020071l.

Abstract

Hydrophobins are fungal proteins that self-assemble spontaneously at hydrophilic-hydrophobic interfaces and change the polar nature of the surfaces to which they attach. This attribute can be used to introduce hydrophobic foci on the surface of hydrophilic supports where hydrophobins are attached by covalent binding. In this paper, we report the binding of Pleurotus ostreatus hydrophobins to a hydrophilic matrix (agarose) to construct a support for noncovalent immobilization and activation of lipases from Candida antarctica, Humicola lanuginosa, and Pseudomonas flourescens. Lipase immobilization on agarose-bound hydrophobins proceeded at very low ionic strength and resulted in increased lipase activity and stability. The enzyme could be desorbed from the support using moderate concentrations of Triton X-100, and its enantioselectivity was similar to that of lipases interfacially immobilized on conventional hydrophobic supports. These results suggest that lipase adsorption on hydrophobins follows an "interfacial activation" mechanism; immobilization on hydrophobins offers new possibilities for lipase study and modulation and reveals a new application for fungal hydrophobins.

摘要

疏水蛋白是一种真菌蛋白,能在亲水 - 疏水界面自发自组装,并改变其附着表面的极性。这一特性可用于在亲水载体表面引入疏水中心,疏水蛋白通过共价结合附着在该表面。在本文中,我们报道了平菇疏水蛋白与亲水基质(琼脂糖)的结合,以构建用于非共价固定和激活来自南极假丝酵母、疏棉状嗜热丝孢菌和荧光假单胞菌脂肪酶的载体。脂肪酶固定在琼脂糖结合的疏水蛋白上是在非常低的离子强度下进行的,这导致脂肪酶活性和稳定性增加。使用中等浓度的 Triton X - 100 可使酶从载体上解吸,其对映选择性与界面固定在传统疏水载体上的脂肪酶相似。这些结果表明,脂肪酶在疏水蛋白上的吸附遵循“界面激活”机制;固定在疏水蛋白上为脂肪酶的研究和调控提供了新的可能性,并揭示了真菌疏水蛋白的一种新应用。

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