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使用粒子光刻技术控制蛋白质的表面覆盖率和排列。

Controlling the surface coverage and arrangement of proteins using particle lithography.

作者信息

Ngunjiri Johnpeter N, Daniels Stephanie L, Li Jie-Ren, Serem Wilson K, Garno Jayne C

机构信息

Chemistry Department, Center for BioModular, Multi-Scale Systems, Louisiana State University, Baton Rouge, LA 70803, USA.

出版信息

Nanomedicine (Lond). 2008 Aug;3(4):529-41. doi: 10.2217/17435889.3.4.529.

Abstract

AIMS

The applicability of particle lithography with monodisperse mesospheres is tested with various proteins to control the surface coverage and dimensions of protein nanopatterns.

METHODS & MATERIALS: The natural self-assembly of monodisperse spheres provides an efficient, high-throughput route to prepare protein nanopatterns. Mesospheres assemble spontaneously into organized crystalline layers when dried on flat substrates, which supply a structural frame or template to direct the placement of proteins. The template particles are displaced with a simple rinsing step to disclose periodic arrays of protein nanopatterns on surfaces.

RESULTS & DISCUSSION: The proteins are attached securely to the surface, forming nanopatterns with a measured thickness of a single layer. The morphology and diameter of the protein nanostructures can be tailored by selecting the diameter of the mesospheres and choosing the protein concentration.

CONCLUSIONS

Particle lithography is shown to be a practical, highly reproducible method for patterning proteins on surfaces of mica, glass and gold. High-throughput patterning was achieved with ferritin, apoferritin, bovine serum albumin and immunoglobulin-G. Depending on the ratio of proteins to mesospheres, either porous films or ring structures were produced. This approach can be applied for fundamental investigations of protein-binding interactions of biological systems in surface-bound bioassays and biosensor surfaces.

摘要

目的

用各种蛋白质测试单分散中层球粒子光刻技术在控制蛋白质纳米图案的表面覆盖率和尺寸方面的适用性。

方法与材料

单分散球体的自然自组装提供了一种高效、高通量的制备蛋白质纳米图案的途径。中层球在平坦基底上干燥时会自发组装成有组织的晶体层,为蛋白质的放置提供结构框架或模板。通过简单的冲洗步骤去除模板颗粒,以揭示表面上蛋白质纳米图案的周期性阵列。

结果与讨论

蛋白质牢固地附着在表面,形成单层厚度的纳米图案。可以通过选择中层球的直径和蛋白质浓度来定制蛋白质纳米结构的形态和直径。

结论

粒子光刻技术被证明是一种在云母、玻璃和金表面对蛋白质进行图案化的实用、高度可重复的方法。使用铁蛋白、脱铁铁蛋白、牛血清白蛋白和免疫球蛋白G实现了高通量图案化。根据蛋白质与中层球的比例,可产生多孔膜或环形结构。这种方法可应用于表面结合生物测定和生物传感器表面生物系统蛋白质结合相互作用的基础研究。

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