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A shape-code nanoplasmonic biosensor for multiplex detection of Alzheimer's disease biomarkers

机译:一种形状典型纳米升性生物传感器,用于多重检测Alzheimer疾病生物标志物

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摘要

AbstractAlzheimer's disease (AD) is a neurodegenerative disease associated with the loss of nerve cells in the brain. The disease is affected by multifactorial pathways and leads to changes in related biomolecular levels as AD progresses. Therefore, AD should be diagnosed with combined detection of several lesions to improve accuracy. Amyloid beta 1–40, 1–42 and τ (tau) protein are milestones in AD pathology and can be used as main screening and diagnostic target markers. Here, we suggest a highly selective biosensor for detection of AD core biomarkers on one platform through distinct localized surface plasmon resonance (LSPR) depending on gold nanoparticles shapes, called a shape-code biosensor. This plasmonic sensor consists of only gold nanoparticles and antibody, but does not need additory methods for precise separation from multifarious samples and identification of markers. Under physiological condition, we determined a detection limit of 34.9fM for amyloid beta (Aβ) 1–40, 26fM for Aβ 1–42 and 23.6fM for τ protein corresponding to the ~ 1, ~ 2.23 and ~ 3.12nm of Rayleigh scattering peak shift on shape-code plasmon system for each biomarker in mimicked blood. This is the first highly sensitive shape-code biosensor to detect AD biomarkers which can be used to diagnose AD easily in the future.Highlights
机译:<![cdata [ 抽象 阿尔茨海默病(AD)是一种与脑中神经细胞丧失相关的神经变性疾病。该疾病受到多因素途径的影响,并且随着广告的进展而导致相关的生物分子水平的变化。因此,应诊断出综合检测若干病变以提高精度。淀粉样蛋白β1-40,1-42和τ(tau)蛋白是AD病理学中的里程碑,可用作主筛选和诊断靶标记。在这里,我们建议通过不同的局面等离子体共振(LSPR)来检测一个平台上的AD核心生物标志物的高度选择性生物传感器,这取决于金纳米颗粒形状,称为形状代码生物传感器。这种等离子体传感器仅由金纳米颗粒和抗体组成,但不需要附加方法,以精确分离从多种样本和标记的鉴定。在生理条件下,我们确定淀粉样蛋白β(Aβ)1-40,26fm的34.9fm的检出限为τ1-42和23.6fm的τ蛋白对应于〜1,〜2.23和3.12nm的瑞利散射峰值对模仿血液中每种生物标志物的形状码等离子体系统转移。这是第一个高度敏感的形状编码生物传感器,用于检测可用于将来轻松诊断广告的广告生物标记。 亮点

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