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Field Effect Transistor Biosensor Using Antigen Binding Fragment for Detecting Tumor Marker in Human Serum

机译:使用抗原结合片段的场效应晶体管生物传感器检测人血清中的肿瘤标志物

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Detection of tumor markers is important for cancer diagnosis. Field-effect transistors (FETs) are a promising method for the label-free detection of trace amounts of biomolecules. However, detection of electrically charged proteins using antibody-immobilized FETs is limited by ionic screening by the large probe molecules adsorbed to the transistor gate surface, reducing sensor responsiveness. Here, we investigated the effect of probe molecule size on the detection of a tumor marker, α-fetoprotein (AFP) using a FET biosensor. We demonstrated that the small receptor antigen binding fragment (Fab), immobilized on a sensing surface as small as 2–3 nm, offers a higher degree of sensitivity and a wider concentration range (100 pg/mL–1 μg/mL) for the FET detection of AFP in buffer solution, compared to the whole antibody. Therefore, the use of a small Fab probe molecule instead of a whole antibody is shown to be effective for improving the sensitivity of AFP detection in FET biosensors. Furthermore, we also demonstrated that a Fab-immobilized FET subjected to a blocking treatment, to avoid non-specific interactions, could sensitively and selectively detect AFP in human serum.
机译:肿瘤标志物的检测对于癌症诊断很重要。场效应晶体管(FET)是一种无标记检测痕量生物分子的有前途的方法。但是,使用抗体固定的FET检测带电荷的蛋白质受到离子筛查的限制,该离子筛查是通过吸附在晶体管栅极表面的大探针分子进行的,降低了传感器的响应能力。在这里,我们研究了使用FET生物传感器检测探针分子大小对检测肿瘤标志物α-甲胎蛋白(AFP)的影响。我们证明,固定在2至3 nm小感应表面上的小受体抗原结合片段(Fab)提供了更高的灵敏度和更宽的浓度范围(100 pg / mL–1μg/ mL)。与整个抗体相比,FET检测缓冲液中的AFP。因此,显示出使用小的Fab探针分子代替完整的抗体对于提高FET生物传感器中AFP检测的灵敏度是有效的。此外,我们还证明,经过阻断处理的固定有Fab的FET可以避免非特异性相互作用,从而可以灵敏地和选择性地检测人血清中的AFP。

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