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单量子点追踪揭示了纳米颗粒表面对细胞内状态的影响。

Single quantum dot tracking reveals the impact of nanoparticle surface on intracellular state.

机构信息

Department of Bioengineering, University of Illinois at Urbana-Champaign, Urbana, IL, 61801, USA.

Micro and Nanotechnology Laboratory, University of Illinois at Urbana-Champaign, Urbana, IL, 61801, USA.

出版信息

Nat Commun. 2018 May 8;9(1):1830. doi: 10.1038/s41467-018-04185-w.

Abstract

Inefficient delivery of macromolecules and nanoparticles to intracellular targets is a major bottleneck in drug delivery, genetic engineering, and molecular imaging. Here we apply live-cell single-quantum-dot imaging and tracking to analyze and classify nanoparticle states after intracellular delivery. By merging trajectory diffusion parameters with brightness measurements, multidimensional analysis reveals distinct and heterogeneous populations that are indistinguishable using single parameters alone. We derive new quantitative metrics of particle loading, cluster distribution, and vesicular release in single cells, and evaluate intracellular nanoparticles with diverse surfaces following osmotic delivery. Surface properties have a major impact on cell uptake, but little impact on the absolute cytoplasmic numbers. A key outcome is that stable zwitterionic surfaces yield uniform cytosolic behavior, ideal for imaging agents. We anticipate that this combination of quantum dots and single-particle tracking can be widely applied to design and optimize next-generation imaging probes, nanoparticle therapeutics, and biologics.

摘要

大分子和纳米颗粒向细胞内靶标传递效率低下是药物输送、基因工程和分子成像的主要瓶颈。在这里,我们应用活细胞单量子点成像和跟踪技术来分析和分类细胞内递送至细胞内后的纳米颗粒状态。通过将轨迹扩散参数与亮度测量值合并,多维分析揭示了使用单一参数无法区分的不同且异质的群体。我们在单细胞中得出了粒子加载、簇分布和囊泡释放的新定量指标,并评估了不同表面的细胞内纳米颗粒在渗透递送后的情况。表面性质对细胞摄取有重大影响,但对细胞质内的绝对数量影响较小。一个关键的结果是,稳定的两性离子表面会产生均匀的细胞质行为,非常适合成像剂。我们预计,这种量子点和单粒子跟踪的结合可以广泛应用于设计和优化下一代成像探针、纳米颗粒治疗剂和生物制剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0424/5940692/c254f643688e/41467_2018_4185_Fig1_HTML.jpg

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