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Detection of single amino acid mutation in human breast cancer by disordered plasmonic self-similar chain

机译:无序等离激元自相似链检测人乳腺癌中的单个氨基酸突变

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Control of the architecture and electromagnetic behavior of nanostructures offers the possibility of designing and fabricating sensors that, owing to their intrinsic behavior, provide solutions to new problems in various fields. We show detection of peptides in multicomponent mixtures derived from human samples for early diagnosis of breast cancer. The architecture of sensors is based on a matrix array where pixels constitute a plasmonic device showing a strong electric field enhancement localized in an area of a few square nanometers. The method allows detection of single point mutations in peptides composing the BRCA1 protein. The sensitivity demonstrated falls in the picomolar (10?12 M) range. The success of this approach is a result of accurate design and fabrication control. The residual roughness introduced by fabrication was taken into account in optical modeling and was a further contributing factor in plasmon localization, increasing the sensitivity and selectivity of the sensors. This methodology developed for breast cancer detection can be considered a general strategy that is applicable to various pathologies and other chemical analytical cases where complex mixtures have to be resolved in their constitutive components.
机译:纳米结构的结构和电磁行为的控制提供了设计和制造传感器的可能性,这些传感器由于其固有的行为,可以为各个领域的新问题提供解决方案。我们显示了从人类样品中提取的多组分混合物中的多肽,可用于乳腺癌的早期诊断。传感器的架构基于矩阵阵列,其中像素构成等离激元器件,显示出位于几平方纳米区域的强电场增强。该方法可以检测组成BRCA1蛋白的肽中的单点突变。显示的灵敏度在皮摩尔(10 ?12 M)范围内。这种方法的成功是精确设计和制造控制的结果。光学建模中考虑了制造过程中引入的残留粗糙度,这是等离子体激元定位的另一个重要因素,从而增加了传感器的灵敏度和选择性。为乳腺癌检测开发的这种方法学可以被认为是一种通用策略,适用于各种病理学和其他化学分析案例,在这些案例中,复杂的混合物必须以其组成成分进行解析。

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