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基于表面增强拉曼光谱的免疫传感器用于超灵敏和选择性检测野生型 p53 和突变型 p53。

Surface enhanced Raman spectroscopy based immunosensor for ultrasensitive and selective detection of wild type p53 and mutant p53.

机构信息

Biophysics & Nanoscience Centre, DEB, Università della Tuscia, Viterbo, Italy.

Biophysics & Nanoscience Centre, DEB, Università della Tuscia, Viterbo, Italy.

出版信息

Anal Chim Acta. 2018 Oct 31;1029:86-96. doi: 10.1016/j.aca.2018.04.049. Epub 2018 Apr 21.

DOI:10.1016/j.aca.2018.04.049
PMID:29907296
Abstract

p53 is a powerful transcription factor playing a pivotal role in the prevention of cancer development and in maintaining genome integrity. This oncosuppressor is found to be functionally inactivated by mutations in many human tumors. Accordingly, wild type p53 and its oncogenic mutants represent valuable cancer biomarkers for diagnostic and prognostic purposes. We developed a highly sensitive biosensor, based on Surface Enhanced Raman Spectroscopy, for detection of wild type p53 and of p53, which is one of the most frequent tumor-associated mutants of p53. Our approach combines the huge Raman signal enhancement, mainly arising from the plasmonic resonance effect on molecules close to gold nanoparticles, with the antigen-antibody biorecognition specificity. By following the enhanced signal of a specific Raman marker, intrinsic to the nanoparticle-antibody bioconjugation, we were able to push the antigen detection level down to the attomolar range in buffer and to the femtomolar range in spiked human serum. The method demonstrated a high reproducibility and a remarkable selectivity in discriminating between wild type p53 and p53 mutant, in both buffer and serum. A calibration plot was built and validated by ELISA for a reliable quantification of p53. These findings entitle our SERS-based immunosensor as a powerful and reliable tool for a non-invasive screening in human serum targeting p53 network. The approach could be easily extended to ultrasensitive detection of other markers of general interest, with feasible implementations into multiplex assays, functioning as lab-on-chip devices for several applications.

摘要

p53 是一种强大的转录因子,在预防癌症发展和维持基因组完整性方面发挥着关键作用。在许多人类肿瘤中,发现该抑癌基因因突变而功能失活。因此,野生型 p53 和其致癌突变体代表了有价值的癌症生物标志物,可用于诊断和预后目的。我们开发了一种基于表面增强拉曼光谱的高灵敏度生物传感器,用于检测野生型 p53 和 p53。p53 是 p53 中最常见的肿瘤相关突变体之一。我们的方法结合了巨大的拉曼信号增强,主要来自于靠近金纳米粒子的分子的等离子体共振效应,以及抗原-抗体生物识别特异性。通过跟踪纳米粒子-抗体生物缀合物中特有的特定拉曼标记物的增强信号,我们能够将抗原检测水平在缓冲液中降低到飞摩尔级,在加标人血清中降低到皮摩尔级。该方法在缓冲液和血清中均表现出高重复性和区分野生型 p53 和 p53 突变体的显著选择性。通过 ELISA 构建和验证校准曲线,可对 p53 进行可靠定量。这些发现使我们基于 SERS 的免疫传感器成为一种强大且可靠的工具,可用于非侵入性筛查人血清中的 p53 网络。该方法可以很容易地扩展到其他具有普遍兴趣的标记物的超灵敏检测,通过多路复用分析的可行实施,作为用于多种应用的芯片实验室设备。

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