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一种新型的基于液体活检的癌症高特异性诊断方法:通过结合 SERS 和等离子体增强荧光分析,减轻检测患者血浆来源循环 microRNAs 时的假阳性反应。

A novel liquid biopsy-based approach for highly specific cancer diagnostics: mitigating false responses in assaying patient plasma-derived circulating microRNAs through combined SERS and plasmon-enhanced fluorescence analyses.

机构信息

Department of Chemistry & Chemical Biology, Indiana University-Purdue University Indianapolis, 402 N. Blackford Street, Indianapolis, Indiana 46202, USA.

出版信息

Analyst. 2020 Jun 21;145(12):4173-4180. doi: 10.1039/d0an00538j. Epub 2020 Jun 3.

Abstract

Studies have shown that microRNAs, which are small noncoding RNAs, hold tremendous promise as next-generation circulating biomarkers for early cancer detection via liquid biopsies. A novel, solid-state nanoplasmonic sensor capable of assaying circulating microRNAs through a combined surface-enhanced Raman scattering (SERS) and plasmon-enhanced fluorescence (PEF) approach has been developed. Here, the unique localized surface plasmon resonance properties of chemically-synthesized gold triangular nanoprisms (Au TNPs) are utilized to create large SERS and PEF enhancements. With careful modification to the surface of Au TNPs, this sensing approach is capable of quantifying circulating microRNAs at femtogram/microliter concentrations. Uniquely, the multimodal analytical methods mitigate both false positive and false negative responses and demonstrate the high stability of our sensors within bodily fluids. As a proof of concept, microRNA-10b and microRNA-96 were directly assayed from the plasma of six bladder cancer patients. Results show potential for a highly specific liquid biopsy method that could be used in point-of-care clinical diagnostics to increase early cancer detection or any other diseases including SARS-CoV-2 in which RNAs can be used as biomarkers.

摘要

研究表明,微小 RNA 是一类小型非编码 RNA,作为通过液体活检进行早期癌症检测的下一代循环生物标志物,具有巨大的潜力。已经开发出一种新型固态纳米等离子体传感器,能够通过结合表面增强拉曼散射 (SERS) 和等离子体增强荧光 (PEF) 方法来检测循环中的微小 RNA。在这里,化学合成的金三角纳米棱镜 (Au TNPs) 的独特局部表面等离子体共振特性被用于产生大的 SERS 和 PEF 增强。通过仔细修饰 Au TNPs 的表面,这种传感方法能够以飞克/微升浓度定量检测循环中的微小 RNA。独特的是,多模态分析方法减轻了假阳性和假阴性反应,并证明了我们的传感器在体液中的高稳定性。作为概念验证,直接从六位膀胱癌患者的血浆中检测到微小 RNA-10b 和微小 RNA-96。结果表明,这种高特异性的液体活检方法具有很大的潜力,可用于即时临床诊断,以提高早期癌症检测的准确率,或者用于包括 SARS-CoV-2 在内的任何其他疾病,因为在这些疾病中 RNA 可以用作生物标志物。

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