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Nanoplasmonic Quantification of Tumor-derived Extracellular Vesicles in Plasma Microsamples for Diagnosis and Treatment Monitoring

机译:血浆微样品中肿瘤来源的细胞外囊泡的纳米等离子体定量用于诊断和治疗监测

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摘要

Tumour-derived extracellular vesicles (EVs) are of increasing interest as a resource of diagnostic biomarkers. However, most EV assays require large samples, are time-consuming, low-throughput and costly, and thus impractical for clinical use. Here, we describe a rapid, ultrasensitive and inexpensive nanoplasmon-enhanced scattering (nPES) assay that directly quantifies tumor-derived EVs from as little as 1 μL of plasma. The assay uses the binding of antibody-conjugated gold nanospheres and nanorods to EVs captured by EV-specific antibodies on a sensor chip to produce a local plasmon effect that enhances tumour-derived EV detection sensitivity and specificity. We identified a pancreatic cancer EV biomarker, ephrin type-A receptor 2 (EphA2), and demonstrate that an nPES assay for EphA2-EVs distinguishes pancreatic cancer patients from pancreatitis patients and healthy subjects. EphA2-EVs were also informative in staging tumour progression and in detecting early responses to neoadjuvant therapy, with better performance than a conventional enzyme-linked immunosorbent assay. The nPES assay can be easily refined for clinical use, and readily adapted for diagnosis and monitoring of other conditions with disease-specific EV biomarkers.
机译:肿瘤来源的细胞外囊泡(EVs)作为诊断生物标志物的资源越来越受到关注。但是,大多数EV分析需要大量样品,耗时,通量低且价格昂贵,因此在临床上不切实际。在这里,我们描述了一种快速,超灵敏且廉价的纳米等离子体增强散射(nPES)分析方法,该方法可直接从低至1μL的血浆中直接量化肿瘤衍生的EV。该测定利用结合抗体的金纳米球和纳米棒与传感器芯片上的EV特异性抗体捕获的EV结合,产生局部等离激元效应,从而增强了肿瘤衍生的EV检测的灵敏度和特异性。我们确定了胰腺癌电动车生物标志物,ephrin A型受体2(EphA2),并证明EphA2-EVs的nPES分析可将胰腺癌患者与胰腺炎患者和健康受试者区分开。与传统的酶联免疫吸附试验相比,EphA2-EVs在肿瘤进展分期和检测对新辅助疗法的早期反应方面也提供了很多信息。 nPES测定法可以很容易地改进以用于临床,并可以通过疾病特异性的EV生物标记物轻松地用于诊断和监测其他疾病。

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