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Encapsulating Quantum Dots within HIV-1 Virions through Site-Specific Decoration of the Matrix Protein Enables Single Virus Tracking in Live Primary Macrophages

机译:通过基质蛋白的特定位点特异性装饰在HIV-1病毒中封装量子点,使单一病毒跟踪在活的主要巨噬细胞中

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摘要

Labeling and imaging with quantum dots (QDs) provides powerful tools to visualize viral infection in living cells. Encapsulating QDs within virions represents a novel strategy for virus labeling. Here, we developed infectious HIV-1 virions encapsulating QDs through site-specific decoration of the viral matrix protein (MA) and used them to visualize early infection events in human primary macrophages by single-particle imaging. The MA protein was fused to a biotin acceptor peptide (BAP) tag, biotinylated, complexed with streptavidin-conjugated QDs in live cells, and incorporated into virions during virus assembly. The QD-encapsulated virions were tracked during infection of macrophages at a single particle level. The dynamic dissociation of MA and Vpr was also tracked in real time, and the results demonstrated that MA has multiple dynamic behaviors and functions during virus entry. More importantly, we tracked the dynamic interplay of QD-encapsulated virions with cellular mitochondria in live primary macrophages. We also found that HIV-1 can induce fission of mitochondria during the early phases of infection. In summary, we have constructed a type of QD-encapsulated virus particle and used this technology to further our understanding of the early events of HIV-1 infection.
机译:用量子点(QDS)的标记和成像提供了可视化活细胞中病毒感染的强大工具。在病毒粒中封装QD表示病毒标记的新策略。在此,我们通过特定于毒性基质蛋白(mA)的特异性装饰,通过特异性装饰来开发传染性HIV-1病毒病毒虫,并通过单粒子成像使用它们来可视化人初级巨噬细胞的早期感染事件。将MA蛋白融合到生物素受体肽(BAP)标签,生物素化,与活细胞中的链霉抗生物素蛋白 - 缀合的QD络合,并在病毒组件期间掺入病毒粒中。在单一颗粒水平的巨噬细胞感染期间跟踪QD包封的病毒粒子。 MA和VPR的动态解离也实时跟踪,结果表明MA在病毒进入期间具有多种动态行为和功能。更重要的是,我们跟踪了QD封装病毒中的动态相互作用与活初级巨噬细胞的细胞线粒体。我们还发现HIV-1可以在感染的早期阶段诱导线粒体裂变。总之,我们构建了一种QD封装的病毒粒子,并利用了这种技术,以进一步了解HIV-1感染的早期事件。

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