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Effect of volume- and time-based constraints on capture of analytes in microfluidic heterogeneous immunoassays

机译:基于体积和时间的约束条件对微流异质免疫分析中捕获分析物的影响

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摘要

Despite the prevalence of microfluidic-based heterogeneous immunoassays (where analytes in solution are captured on a solid surface functionalized with a capture molecule), there is incomplete understanding of how assay parameters influence the amount of captured analytes. This study presents computational results and corresponding experimental binding assays in which the capture of analytes is studied under variations in both mass transfer and surface binding, constrained by real-world assay conditions of finite sample volume, assay time, and capture area. Our results identify: 1) a "reagent-limited" regime which exists only under the constraints of finite sample volume and assay time; 2) a critical flow rate (e.g. 0.5 μL min~(-1) under our assay conditions) to gain the maximum signal with the fastest assay time; 3) an increase in signal by using a short concentrated plug (e.g. 5 μL, 100 nM) rather than a long dilute plug (e.g. 50 μL, 10 nM) of sample; 4) the possibility of spending a considerable fraction of the assay time out of the reaction-limited regime. Overall, an improved understanding of fundamental physical processes may be particularly beneficial for the design of point-of-care assays, where volumes of reagents and available samples are limited, and the desired time-to-result short.
机译:尽管普遍存在基于微流体的异质免疫测定(其中溶液中的分析物被捕获分子功能化的固体表面捕获),但对测定参数如何影响捕获的分析物数量尚不完全了解。这项研究提出了计算结果和相应的实验结合测定法,其中在传质和表面结合力的变化下研究分析物的捕获,并受到有限样品量,测定时间和捕获面积的实际测定条件的限制。我们的结果表明:1)仅在有限的样品量和测定时间的约束下存在的“试剂受限”方案; 2)临界流速(例如在我们的测定条件下为0.5μLmin〜(-1)),以最快的测定时间获得最大信号; 3)通过使用短的浓缩塞子(例如5μL,100 nM)而不是长的稀释塞子(例如50μL,10 nM)来增加信号; 4)有可能在反应受限的条件下花费相当一部分测定时间。总体而言,对基本物理过程的更好理解可能对设计即时点检测特别有利,因为即时检测的试剂和可用样品量有限,所需的结果时间较短。

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