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Improved biomarker quantification of silicon nanowire field-effect transistor immunosensors with signal enhancement by RNA aptamer: Amyloid beta as a case study

机译:通过RNA适体的信号增强改进了硅纳米线场效应晶体管免疫调传料的生物标志物定量:淀粉样蛋白β作为案例研究

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Quantifying proteins at ultra-low levels in high ionic-strength solutions by silicon nanowire field-effect transistor (SiNWFET) immunosensors is critically hindered due to the limited Debye length, charge distributions and uncontrollable orientations of protein molecules on the NW surfaces. In this study, we propose a novel strategy to overcome this issue by employing aptamer as bio-amplifier for different types of SiNWFET immunosensors to quantify Amyloid Beta (Ass) 1-42, a biomarker for early-stage diagnosis of Alzheimer disease (AD) with ultra-low level in human serum (HS), as a representative target. Our method, presented for the first time, exhibits an outstanding performance in combination with mSAM-SiNWFET immunosensors (designed by integrating SiNWFET as transducer, mouse antibody as bio-receptor, and mixed self-assembled monolayers (mSAMs) for biofouling resistance) to sense Ass 1-42 down to 100 fg/mL in HS, the lowest level achieved in comparison with the most advanced sensing technologies for Ass 1-42. The empirical data also reveal that varied concentrations of Ass 1-42 in diverse high ionic-strength environments (150 mM BTP and HS) express good linear relationship with signal amplified by aptamer. This novel approach is therefore potentially applied for early-stage diagnosis of AD and other clinical trials of biomarkers with ultra-low content in blood.
机译:在高离子强度溶液超低水平通过硅纳米线场效应晶体管定量蛋白质(SiNWFET)免疫传感器被临界受阻由于有限的德拜长度,电荷分布和NW表面上的蛋白分子的不可控的取向。在这项研究中,我们提出了一个新的战略,通过采用适体的生物放大为不同类型的SiNWFET免疫传感器的量化淀粉样蛋白(ASS)1-42,阿尔茨海默病的早期诊断的生物标记物来解决这个问题(AD)在人血清(HS)的超低级别,作为代表性的目标。我们的方法,提出了在第一时间,表现出组合的杰出性能MSAM-SiNWFET免疫传感器来感测(通过集成SiNWFET如换能器,小鼠抗体作为生物受体,和混合自组装单层(mSAMs),用于生物结垢阻力设计)屁股1-42降到100 FG / mL,在HS中,与最先进的传感技术屁股1-42比较实现的最低水平。经验数据还揭示了屁股1-42中的是改变浓度在不同的高离子强度环境中(150mM的BTP和HS)表达与由适体放大后的信号良好的线性关系。因此,这种新颖的方法潜在地适用于AD和与血液中的超低含量生物标志物的其它临床试验的早期诊断。

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