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通过表面压和表面电势测量以及原子力显微镜 (AFM) 成像研究了 Savinase 对胰岛素 Langmuir 单分子层的蛋白水解作用。

Savinase proteolysis of insulin Langmuir monolayers studied by surface pressure and surface potential measurements accompanied by atomic force microscopy (AFM) imaging.

机构信息

Sofia University, Faculty of Chemistry, Department of Physical Chemistry, Lab Biophysical Chemistry, 1, James Bourchier Ave., Sofia 1164, Bulgaria.

出版信息

J Colloid Interface Sci. 2011 Aug 15;360(2):654-61. doi: 10.1016/j.jcis.2011.04.101. Epub 2011 May 5.

Abstract

The mechanism of the enzymatic action of Savinase on an insulin substrate organized in a monolayer at the air-water interface was studied. We followed two steps experimental approach classical surface pressure and surface potential measurements in combination with atomic force microscopy imaging. Utilizing the barostat surface balance, the hydrolysis kinetic was followed by measuring simultaneously the decrease in the surface area and the change of the surface potential versus time. The decrease in the surface area is a result of the random scission of the peptide bonds of polypeptide chain, progressively appearance of amino acid residues, and their solubilization in the aqueous subphase. The interpretation of the surface potential data was based on the contribution of the dipole moments of the intact and broken peptide groups which remain at the interface during the proteolysis. An appropriate kinetic model for the Savinase action was applied, and the global kinetic constant was obtained. The application of the AFM revealed the state of the insulin monolayers before and after the Savinase action. The comparison of the topography of the films and the roughness analysis showed that insulin Langmuir-Blodgett (LB) films transferred before the enzyme action were flat, while at the end of hydrolysis, roughness of films has increased and the appearance of 3D structures was observed.

摘要

研究了 Savinase 在空气-水界面单层组织的胰岛素底物上的酶促作用机制。我们采用经典的表面压和表面电势测量方法,结合原子力显微镜成像,遵循两步实验方法。利用压力计表面天平,通过同时测量表面积的减少和表面电势随时间的变化,跟踪水解动力学。表面积的减少是由于多肽链的肽键随机断裂,氨基酸残基逐渐出现,并在水亚相中溶解的结果。表面电势数据的解释基于在蛋白水解过程中留在界面上的完整和断裂肽基团的偶极矩的贡献。应用了适当的 Savinase 作用动力学模型,并获得了全局动力学常数。原子力显微镜的应用揭示了 Savinase 作用前后胰岛素单层的状态。对薄膜的形貌和粗糙度分析进行比较表明,在酶作用之前转移的胰岛素 Langmuir-Blodgett(LB)薄膜是平坦的,而在水解结束时,薄膜的粗糙度增加,并且观察到 3D 结构的出现。

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