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Gradient Hydrogel Matrix for Microarray and Biosensor Applications: An Imaging SPR Study

机译:用于芯片和生物传感器应用的梯度水凝胶基质:成像SPR研究

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A biosensor matrix based on UV-initiated graft copolymerized polyethylene glycol) methacrylate and 2-hydroxyethyl methacrylate has been studied using imaging surface plasmon resonance (iSPR). By using a photo mask and a programmable shutter to vary the exposure time laterally, a gradient of matrix spots with physical thicknesses ranging from a few to tens of nanometers was generated. To maximize the dynamic range, imaging SPR was employed in wavelength interrogation mode. By finding the minimum in the reflectance spectra from each pixel of an image, SPR wavelength maps were constructed. The shift in SPR wavelength upon biospecific interaction was then measured both as a function of matrix thickness and composition. The performance of the matrix was evaluated in terms of immobilization of human serum albumin, biomolecular interaction with its antibody, and nonspecific binding of human fibrinogen. In addition, a low molecular weight interaction pair based on a synthetic polypeptide and calmodulin was also studied to explore the size selectivity of the hydrogel matrix. Our results show that the gradient matrix exhibits excellent properties for quick evaluation and screening of optimal hydrogel performance. The mixed hydrogel matrices display very low levels of nonspecific binding. It is also evident that the low molecular weight calmodulin is capable of freely diffusing and interacting throughout the entire hydrogel matrix, whereas the much larger albumin and its corresponding antibody, in particular, are partly/completely hindered from penetrating the interior of the matrix. This size-selectivity is attributed to a significant UV-initiated cross-linking or branching of the matrix during fabrication and/or protein mediated multipoint attachment during immobilization.
机译:使用成像表面等离子体激元共振(iSPR),研究了基于紫外线引发的接枝共聚的聚甲基丙烯酸乙二醇酯和甲基丙烯酸2-羟乙酯的生物传感器基质。通过使用光掩模和可编程快门横向改变曝光时间,可生成物理厚度范围从几纳米到几十纳米的基质斑点的梯度。为了最大化动态范围,在波长询问模式下采用了成像SPR。通过从图像的每个像素中找到反射光谱的最小值,可以构建SPR波长图。然后测量生物特异性相互作用后SPR波长的变化与基质厚度和组成的关系。根据人血清白蛋白的固定化,与抗体的生物分子相互作用以及人血纤蛋白原的非特异性结合来评估基质的性能。另外,还研究了基于合成多肽和钙调蛋白的低分子量相互作用对,以探索水凝胶基质的尺寸选择性。我们的结果表明,梯度基质具有出色的性能,可快速评估和筛选最佳水凝胶性能。混合的水凝胶基质显示出非常低的非特异性结合水平。同样明显的是,低分子量钙调蛋白能够在整个水凝胶基质中自由扩散和相互作用,而特别是部分/完全阻止了大得多的白蛋白及其相应的抗体穿透基质内部。该尺寸选择性归因于在制造过程中基质的明显的紫外线引发的交联或分支和/或在固定过程中蛋白质介导的多点附着。

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