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通过共振声学分析直接定量分析物浓度。

Direct quantification of analyte concentration by resonant acoustic profiling.

作者信息

Godber Benjamin, Thompson Kevin S J, Rehak Marian, Uludag Yildiz, Kelling Sven, Sleptsov Alexander, Frogley Mark, Wiehler Klaus, Whalen Christopher, Cooper Matthew A

机构信息

Akubio Ltd., Cambridge, United Kingdom.

出版信息

Clin Chem. 2005 Oct;51(10):1962-72. doi: 10.1373/clinchem.2005.053249. Epub 2005 Aug 4.

DOI:10.1373/clinchem.2005.053249
PMID:16081504
Abstract

BACKGROUND

Acoustic sensors that exploit resonating quartz crystals directly detect the binding of an analyte to a receptor. Applications include detection of bacteria, viruses, and oligonucleotides and measurement of myoglobin, interleukin 1beta (IL-1beta), and enzyme cofactors.

METHODS

Resonant Acoustic Profiling was combined with a microfluidic lateral flow device incorporating an internal reference control, stable linker chemistry, and immobilized receptors on a disposable sensor "chip". Analyte concentrations were determined by analyzing the rate of binding of the analyte to an appropriate receptor.

RESULTS

The specificity and affinity of antibody-antigen and enzyme-cofactor interactions were determined without labeling of the receptor or the analyte. We measured protein concentrations (recombinant human IL-1beta and recombinant human myoglobin) and quantified binding of cofactors (NADP+ and NAD+) to the enzyme glucose dehydrogenase. Lower limits of detection were approximately 1 nmol/L (17 ng/mL) for both IL-1beta and human myoglobin. The equilibrium binding constant for NADP+ binding to glucose dehydrogenase was 2.8 mmol/L.

CONCLUSIONS

Resonant Acoustic Profiling detects analytes in a relatively simple receptor-binding assay in <10 min. Potential applications include real-time immunoassays and biomarker detection. Combination of this technology platform with existing technologies for concentration and presentation of analytes may lead to simple, label-free, high-sensitivity methodologies for reagent and assay validation in clinical chemistry and, ultimately, for real-time in vitro diagnostics.

摘要

背景

利用共振石英晶体的声学传感器可直接检测分析物与受体的结合。其应用包括细菌、病毒和寡核苷酸的检测以及肌红蛋白、白细胞介素1β(IL-1β)和酶辅因子的测量。

方法

将共振声学分析与一种微流控侧向流动装置相结合,该装置包含内部参考对照、稳定的连接化学以及一次性传感器“芯片”上固定的受体。通过分析分析物与合适受体的结合速率来确定分析物浓度。

结果

在不标记受体或分析物的情况下测定了抗体 - 抗原和酶 - 辅因子相互作用的特异性和亲和力。我们测量了蛋白质浓度(重组人IL-1β和重组人肌红蛋白)并定量了辅因子(NADP + 和NAD +)与葡萄糖脱氢酶的结合。IL-1β和人肌红蛋白的检测下限约为1 nmol/L(17 ng/mL)。NADP + 与葡萄糖脱氢酶结合的平衡结合常数为2.8 mmol/L。

结论

共振声学分析可在不到10分钟的相对简单的受体结合测定中检测分析物。潜在应用包括实时免疫测定和生物标志物检测。将该技术平台与现有的分析物浓缩和呈现技术相结合,可能会产生用于临床化学中试剂和测定验证的简单、无标记、高灵敏度方法,并最终用于实时体外诊断。

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