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靶向催化 DNA 四链结用于 miRNA 的 CRET 成像、级联逻辑运算以及 DNA 纳米水凝胶的自组装用于靶向药物递送。

Target-Catalyzed DNA Four-Way Junctions for CRET Imaging of MicroRNA, Concatenated Logic Operations, and Self-Assembly of DNA Nanohydrogels for Targeted Drug Delivery.

机构信息

Shandong Province Key Laboratory of Detection Technology for Tumor Markers, School of Chemistry and Chemical Engineering, Linyi University , Linyi 276005, China.

Collaborative Innovation Center for Marine Biomass Fiber Materials and Textiles, College of Chemical Science and Engineering, Laboratory of Fiber Materials and Modern Textiles, the Growing Base for State Key Laboratory, Shandong Sino-Japanese Center for Collaborative Research of Carbon Nanomaterials, Qingdao University , Qingdao 266071, China.

出版信息

ACS Appl Mater Interfaces. 2015 Oct 21;7(41):23310-9. doi: 10.1021/acsami.5b07827. Epub 2015 Oct 9.

Abstract

Here we report a target-catalyzed DNA four-way junction (DNA-4WJ) on the basis of toehold-mediated DNA strand displacement reaction (TM-SDR), which is readily applied in enzyme-free amplified chemiluminescence resonance energy transfer (CRET) imaging of microRNA. In this system, the introduction of target microRNA-let-7a (miR-let-7a) activates a cascade of assembly steps with four DNA hairpins, followed by a disassembly step in which the target microRNA is displaced and released from DNA-4WJ to catalyze the self-assembly of additional branched junctions. As a result, G-quadruplex subunit sequences and fluorophore fluorescein amidite (FAM) are encoded in DNA-4WJ in a close proximity, stimulating a CRET process in the presence of hemin/K(+) to form horseradish peroxidase (HRP)-mimicking DNAzyme that catalyzes the generation of luminol/H2O2 chemiluminescence (CL), which further transfers to FAM. The background signal is easily reduced using magnetic graphene oxide (MGO) to remove unreacted species through magnetic separation, which makes a great contribution to improve the detection sensitivity and achieves a detection limit as low as 6.9 fM microRNA-let-7a (miR-let-7a). In addition, four-input concatenated logic circuits with an automatic reset function have been successfully constructed relying on the architecture of the proposed DNA-4WJ. More importantly, DNA nanohydrogels are self-assembled using DNA-4WJs as building units after centrifugation, which are driven by liquid crystallization and dense packaging of building units. Moreover, the DNA nanohydrogels are readily functionalized by incorporating with aptamers, bioimaging agents, and drug loading sites, which thus are served as efficient nanocarriers for targeted drug delivery and cancer therapy with high loading capacity and excellent biocompatibility.

摘要

在这里,我们基于引发链置换反应(TM-SDR),报道了一种基于靶标催化的 DNA 四链结(DNA-4WJ),该方法可应用于无酶放大化学发光共振能量转移(CRET)成像分析 microRNA。在该体系中,目标 microRNA-let-7a(miR-let-7a)的引入激活了四链发夹 DNA 的级联组装步骤,随后是一个解组装步骤,在该步骤中,目标 microRNA 被置换并从 DNA-4WJ 中释放出来,从而催化更多分支结的自组装。结果,在血红素/K(+)存在下,G-四链体亚基序列和荧光素 amidite(FAM)被编码在 DNA-4WJ 中,形成一个接近的距离,刺激 CRET 过程,形成辣根过氧化物酶(HRP)模拟 DNA 酶,催化发光氨(Luminol)/H2O2 化学发光(CL)的生成,进一步转移到 FAM。通过磁分离去除未反应的物质,使用磁性氧化石墨烯(MGO)很容易减少背景信号,这有助于提高检测灵敏度,并实现低至 6.9 fM microRNA-let-7a(miR-let-7a)的检测限。此外,还成功地构建了具有自动复位功能的四输入级联逻辑电路,该电路依赖于所提出的 DNA-4WJ 结构。更重要的是,DNA 纳米水凝胶可以在离心后使用 DNA-4WJ 作为构建单元自组装,其驱动力来自于构建单元的液晶化和密集包装。此外,DNA 纳米水凝胶可以通过与适体、生物成像剂和药物加载位点的结合来进行功能化,因此它们可以作为高效的纳米载体,用于靶向药物输送和癌症治疗,具有高载药能力和优异的生物相容性。

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