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Micrometer sized immobilization of protein molecules onto Quartz, Silicium and Gold

机译:微米级将蛋白质分子固定在石英,硅和金上

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We demonstrate that ultraviolet light can be used to make sterically oriented covalent immobilization of a large variety of protein molecules onto either gold or thiolated quartz or silicium. The reaction mechanism behind the reported new technology involves light induced breakage of disulphide bridges in proteins upon UV illumination of nearby aromatic amino acids, resulting in the formation of free, reactive thiol groups that will form covalent bonds with thiol reactive surfaces. The protein molecules in general retain their function. The size of the immobilization spot is determined by the dimension of the UV beam. In principle, the spot size may be as small as 1 micrometer or less. We have developed the necessary technology for preparing large protein arrays of enzymes and fragments of monoclonal antibodies. Dedicated Image Processing Software has been developed for making quality assessment of the protein arrays. A multitude of important application areas such as drug carriers and drug delivery, bioelectronics, carbon nanotubes, nanoparticles as well as protein glue are discussed.
机译:我们证明了紫外线可以用来使多种蛋白质分子在空间上定向共价固定在金或硫醇化石英或硅上。报道的新技术背后的反应机理涉及在紫外线照射附近的芳香族氨基酸后,光诱导蛋白质中的二硫键断裂,导致形成游离的,反应性的硫醇基,该基团将与硫醇的反应性表面形成共价键。蛋白质分子通常保持其功能。固定点的大小取决于紫外线的大小。原则上,光点尺寸可以小至1微米或更小。我们已经开发出必要的技术,用于制备酶的大型蛋白质阵列和单克隆抗体片段。已经开发了专用图像处理软件来对蛋白质阵列进行质量评估。讨论了许多重要的应用领域,例如药物载体和药物递送,生物电子学,碳纳米管,纳米颗粒以及蛋白质胶。

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