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首页> 外文期刊>Nature Communications >A signal-amplifiable biochip quantifies extracellular vesicle-associated RNAs for early cancer detection
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A signal-amplifiable biochip quantifies extracellular vesicle-associated RNAs for early cancer detection

机译:可信号放大的生物芯片可量化细胞外囊泡相关RNA,用于早期癌症检测

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Detection of extracellular vesicle (EV)-associated RNAs with low expression levels in early-stage cancer remains a challenge and is highly valuable. Here, we report a nanoparticle-based biochip that could capture circulating EVs without isolation, brighten encapsulated RNAs, and amplify fluorescence signals in situ in a single step. We confine catalyzed hairpin DNA circuit (CHDC) in cationic lipid-polymer hybrid nanoparticles (LPHNs) that are tethered on a chip. LPHN features a core-shell-corona structure that facilitates the transfer and mixing of CHDC with EV-associated RNAs when forming the LPHN–EV nanocomplex. CHDC is triggered upon target RNA binding and quickly generate amplified signals. The signal amplification efficiency of LPHN–CHDC is demonstrated in artificial EVs, cancer cells, and cancer cell-derived EVs. We show that LPHN–CHDC biochip with signal amplification capability could selectively and sensitively identify low expression glypican-1 mRNA in serum EVs, distinguishing patients with early- and late-stage pancreatic cancer from healthy donors and patients with benign pancreatic disease.
机译:在早期癌症中检测低表达水平的细胞外囊泡(EV)相关RNA仍然是一项挑战,具有很高的价值。在这里,我们报告了一种基于纳米粒子的生物芯片,该芯片可以捕获循环的EV,而无需分离,照亮封装的RNA,并在一个步骤中就地扩增荧光信号。我们将催化的发夹DNA电路(CHDC)限制在拴在芯片上的阳离子脂质-聚合物杂化纳米颗粒(LPHN)中。 LPHN具有核-壳-电晕结构,在形成LPHN-EV纳米复合物时,可促进CHDC与EV相关RNA的转移和混合。 CHDC在靶RNA结合后触发,并迅速产生放大的信号。 LPHN–CHDC的信号放大效率已在人造电动汽车,癌细胞和癌细胞衍生的电动汽车中得到证明。我们显示具有信号放大功能的LPHN–CHDC生物芯片可以选择性和敏感地识别血清EV中的低表达glypican-1 mRNA,从而将早期和晚期胰腺癌患者与健康供体和良性胰腺疾病患者区分开。

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