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Use of Nanotrap particles for the capture and enrichment of Zika, chikungunya and dengue viruses in urine

机译:使用纳米筏颗粒在尿液中捕获和富集Zika,Chikungunya和登革热病毒的捕获和富集

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Nanotrap ? (NT) particles are hydrogel microspheres developed for target analyte separation and discovery applications. NT particles consist of cross-linked N-isopropylacrylamide (NIPAm) copolymers that are functionalized with a variety of chemical affinity baits to enable broad-spectrum collection and retention of target proteins, nucleic acids, and pathogens. NT particles have been previously shown to capture and enrich arboviruses including Rift Valley fever and Venezuelan equine encephalitis viruses. Yet, there is still a need to enhance the detection ability for other re-emerging viruses such as Zika (ZIKV), chikungunya (CHIKV), and dengue (DENV) viruses. In this study, we exploited NT particles with different affinity baits, including cibacron blue, acrylic acid, and reactive red 120, to evaluate their capturing and enrichment capability for ZIKV, DENV and CHIKV in human fluids. Our results demonstrate that CN1030, a NT particle conjugated with reactive red 120, can recover between 8-16-fold greater genomic copies of ZIKV, CHIKV and DENV in virus spiked urine samples via RT-qPCR, superior to the other chemical baits. Also, we observed that CN1030 simultaneously enriched ZIKV, CHIKV and DENV in co-infection-based settings and could stabilize ZIKV, but not CHIKV infectivity in saliva spiked samples. CN1030 enriched viral detection at various viral concentrations, with significant enhancement observed at viral titers as low as 100 PFU/mL for ZIKV and 10 PFU/mL for CHIKV. The detection of ZIKV was further enhanced with NT particles by processing of larger volume urine samples. Furthermore, we developed a magnetic NT particle, CN3080, based on the same backbone of CN1030, and demonstrated that CN3080 could also capture and enrich ZIKV and CHIKV in a dose-dependent manner. Finally, in silico docking predictions support that the affinity between reactive red 120 and ZIKV or CHIKV envelope proteins appeared to be greater than acrylic acid. Overall, our data show that NT particles along with reactive red 120 can be utilized as a pre-processing technology for enhancement of detecting febrile-illness causing viruses.
机译:nanotrap? (NT)颗粒是为目标分析物分离和发现应用而开发的水凝胶微球。 NT颗粒由交联的N-异丙基丙烯酰胺(NIPAM)共聚物组成,其具有各种化学亲和力诱饵的官能化,以实现靶蛋白,核酸和病原体的广谱收集和保留。先前已显示NT颗粒以捕获和富集枝虫病毒,包括裂谷发热和委内瑞拉大当脑炎病毒。然而,仍然需要提高其他重新出现病毒的检测能力,如Zika(Zikv),Chikungunya(Chikv)和登革热(Denv)病毒。在这项研究中,我们利用不同亲和力诱饵的NT颗粒,包括Cibacron蓝,丙烯酸和反应性红色120,以评估它们在人流体中的Zikv,Denv和Chikv的捕获和富集能力。我们的结果表明,CN1030是与反应性红色120缀合的NT颗粒,可以通过RT-QPCR在病毒Spiked尿液中的ZIKV,Chikv和Denv的8-16倍较大的基因组拷贝之间恢复,通过RT-QPCR优于其他化学诱饵。此外,我们观察到CN1030同时富集ZIKV,CHIKV和DENV在基于共感染的环境中,并且可以稳定ZIKV,但在唾液中的CHIKV感染性飙升样品。 CN1030在各种病毒浓度下富集病毒检测,在病毒滴度下观察到显着的增强,对于ZIKV和10pfu / ml,对于CHIKV,如图100pfu / ml。通过加工较大的尿液样品,通过NT颗粒进一步增强了ZIKV的检测。此外,我们开发了基于CN1030的相同骨架的磁NT颗粒CN3080,并且证明CN3080还可以以剂量依赖的方式捕获和富集ZIKV和CHIKV。最后,在硅对接预测中,支持反应性红色120和Zikv或Chikv包膜蛋白之间的亲和力似乎大于丙烯酸。总的来说,我们的数据表明,NT颗粒以及反应性红色120可以用作预处理技术,用于增强检测造成病毒的疾病。

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