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Aptamer-Based Microfluidic Electrochemical Biosensor for Monitoring Cell-Secreted Trace Cardiac Biomarkers

机译:基于适体的微流控电化学生物传感器用于监测细胞分泌的痕量心脏生物标志物。

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摘要

Continual monitoring of secreted biomarkers from organ-on-a-chip models is desired to understand their responses to drug exposure in a noninvasive manner. To achieve this goal, analytical methods capable of monitoring trace amounts of secreted biomarkers are of particular interest. However, a majority of existing biosensing techniques suffer from limited sensitivity, selectivity, stability, and require large working volumes, especially when cell culture medium is involved, which usually contains a plethora of nonspecific binding proteins and interfering compounds. Hence, novel analytical platforms are needed to provide noninvasive, accurate information on the status of organoids at low working volumes. Here, we report a novel microfluidic aptamer-based electrochemical biosensing platform for monitoring damage to cardiac organoids. The system is scalable, low-cost, and compatible with microfluidic platforms easing its integration with microfluidic bioreactors. To create the creatine kinase (CK)-MB biosensor, the microelectrode was functionalized with aptamers that are specific to CK-MB biomarker secreted from a damaged cardiac tissue. Compared to antibody-based sensors, the proposed aptamer-based system was highly sensitive, selective, and stable. The performance of the sensors was assessed using a heart-on-a-chip system constructed from human embryonic stem cell-derived cardiomyocytes following exposure to a cardiotoxic drug, doxorubicin. The aptamer-based biosensor was capable of measuring trace amounts of CK-MB secreted by the cardiac organoids upon drug treatments in a dose-dependent manner, which was in agreement with the beating behavior and cell viability analyses. We believe that, our microfluidic electrochemical biosensor using aptamer-based capture mechanism will find widespread applications in integration with organ-on-a-chip platforms for in situ detection of biomarkers at low abundance and high sensitivity.
机译:需要从芯片上器官模型中持续监测分泌的生物标志物,以了解其对药物暴露的无创性反应。为了实现这个目标,能够监测痕量分泌生物标志物的分析方法特别令人关注。然而,大多数现有的生物传感技术具有有限的灵敏度,选择性,稳定性,并且需要大量的工作量,尤其是在涉及细胞培养基的情况下,该细胞培养基通常包含大量的非特异性结合蛋白和干扰化合物。因此,需要新颖的分析平台来以低工作量提供有关类器官状态的无创,准确的信息。在这里,我们报告了一种新型的基于微适体的电化学生物传感平台,用于监测对心脏类器官的损害。该系统是可扩展的,低成本的,并且与微流体平台兼容,从而简化了与微流体生物反应器的集成。为了创建肌酸激酶(CK)-MB生物传感器,将微电极用对受损心脏组织分泌的CK-MB生物标志物具有特异性的适体进行功能化。与基于抗体的传感器相比,所提出的基于适体的系统具有高度的敏感性,选择性和稳定性。传感器的性能是通过使用由人体胚胎干细胞衍生的心肌细胞接触心脏毒性药物阿霉素构建的芯片上心脏系统来评估的。基于适体的生物传感器能够以剂量依赖的方式测量药物治疗后心脏类器官分泌的痕量CK-MB,这与跳动行为和细胞生存力分析相符。我们相信,我们的使用基于适体的捕获机制的微流体电化学生物传感器将在与芯片上器官平台相集成的低丰度和高灵敏度生物标志物原位检测中找到广泛的应用。

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