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二氧化硅纳米管膜三维微孔阵列中的蛋白质捕获

Protein capture in silica nanotube membrane 3-D microwell arrays.

作者信息

Kang Myungchan, Trofin Lacramioara, Mota Miguel O, Martin Charles R

机构信息

Department of Chemistry and Center for Research at the Bio/Nano Interface, University of Florida, Gainesville, Florida 32611-7200, USA.

出版信息

Anal Chem. 2005 Oct 1;77(19):6243-9. doi: 10.1021/ac0508907.

Abstract

The microarray format has allowed for rapid and sensitive detection of thousands of analyte DNAs in a single sample, and there is considerable interest in extending this technology to protein biosensing. While glass is the most common substrate for microarrays, its binding capacity is limited because the glass surface is flat. One way to overcome this limitation is to develop arrays based on porous materials. Such "3-D" arrays can provide greater sensitivity because both the capture molecules and the analyte species they bind are immobilized throughout the thickness of the porous material. We describe here 3-D protein microarrays based on nanopore alumina membranes that contain silica nanotubes within the pores. These microarrays are prepared via a plasma-etch method using a TEM grid as the etch mask and consist of individual nanotube-containing microwells imbedded in a Ag film that coats the alumina membrane surface. We show that the microwells can be functionalized with antibodies and that these antibodies can capture their antigen proteins, which serve as prototype analytes. The analyte proteins are fluorescently tagged, which allows for fluorescence microscopy-based imaging of the array. The Ag surrounding the microwells shows very low background fluorescence, thus improving the signal-background ratio obtained from these arrays.

摘要

微阵列形式能够在单个样本中快速、灵敏地检测数千种分析物DNA,并且人们对将该技术扩展到蛋白质生物传感领域有着浓厚兴趣。虽然玻璃是微阵列最常见的基质,但其结合能力有限,因为玻璃表面是平的。克服这一限制的一种方法是开发基于多孔材料的阵列。这种“三维”阵列可以提供更高的灵敏度,因为捕获分子及其结合的分析物都固定在多孔材料的整个厚度中。我们在此描述基于纳米孔氧化铝膜的三维蛋白质微阵列,其孔内含有二氧化硅纳米管。这些微阵列通过使用透射电子显微镜(TEM)网格作为蚀刻掩膜的等离子体蚀刻方法制备,由嵌入涂覆在氧化铝膜表面的银膜中的单个含纳米管微孔组成。我们表明微孔可以用抗体进行功能化,并且这些抗体可以捕获其抗原蛋白,这些抗原蛋白用作原型分析物。分析物蛋白用荧光标记,这允许基于荧光显微镜对阵列进行成像。微孔周围的银显示出非常低的背景荧光,从而提高了从这些阵列获得的信号背景比。

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