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蛋白质在金点阵列上的选择性固定及利用化学力显微镜进行表征

Selective immobilization of proteins on gold dot arrays and characterization using chemical force microscopy.

作者信息

Kim Hyunsook, Park Jun Hyung, Cho Il-Hoon, Kim Sung-Kyoung, Paek Se-Hwan, Lee Haiwon

机构信息

Department of Chemistry, Hanyang University, Seoul 133-791, Republic of Korea.

出版信息

J Colloid Interface Sci. 2009 Jun 15;334(2):161-6. doi: 10.1016/j.jcis.2009.03.082. Epub 2009 Apr 8.

Abstract

Streptavidin that has four binding sites arranged in two opposing pairs is known as one of the most important linker proteins for binding the second biotinylated protein. To efficiently locate streptavidins to selective positions without nonspecific binding, we prepared well-controlled arrays of biotins on a gold surface by using a mixed self-assembly process. Two thiol derivatives (11-mercapto-1-undecanol and 11-mercaptoundecanoic-(8-biotinylamido-3,6-dioxaoctyl)amide) were used for preparing the mixed self-assembled monolayers. Fragment antibodies modified with biotin were immobilized on a gold surface covered with streptavidin. This system was applied to gold dot arrays formed by nanosphere lithography. The gold dot arrays were used as the mother structure to construct the array of proteins at the nanometer scale. Selective immobilization of antibodies was characterized by imaging the substrate with an atomic force microscope and measuring the interaction force between biomaterials by chemical force microscopy. Also, the interaction force between antibodies was compared with the force predicted using the Johnson-Kendall-Roberts theory.

摘要

链霉亲和素具有四个以两个相对的对排列的结合位点,是用于结合第二种生物素化蛋白的最重要的连接蛋白之一。为了在无非特异性结合的情况下将链霉亲和素有效地定位到选择性位置,我们通过混合自组装过程在金表面制备了可控的生物素阵列。两种硫醇衍生物(11-巯基-1-十一醇和11-巯基十一烷酸-(8-生物素基酰胺基-3, 6-二氧杂辛基)酰胺)用于制备混合自组装单分子层。用生物素修饰的片段抗体固定在覆盖有链霉亲和素的金表面上。该系统应用于通过纳米球光刻形成的金点阵列。金点阵列用作母结构以在纳米尺度构建蛋白质阵列。通过用原子力显微镜对底物成像并通过化学力显微镜测量生物材料之间的相互作用力来表征抗体的选择性固定。此外,将抗体之间的相互作用力与使用约翰逊-肯德尔-罗伯茨理论预测的力进行了比较。

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