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Data from: Capturing the start point of the virus-cell interaction with high-speed 3D single-particle tracking

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DataCite Commons2022-11-04 更新2024-07-13 收录
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https://idn.duke.edu/ark:/87924/r4bp07h15
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<strong>*Data will be embargoed until publication of related article, or up to no more than 1 year from data upload.*</strong> The early stages of the virus-cell interaction have long evaded observation by existing microscopy methods due to the rapid diffusion of virions in the extracellular space and the large 3D cellular structures involved. Here we present an active-feedback single-particle tracking method with simultaneous volumetric imaging of the live cell environment to address this knowledge gap to present unprecedented detail to the extracellular phase of the infectious cycle. We report previously unobserved phenomena in the early stages of the virus-cell interaction, including skimming contact events at the millisecond timescale, orders of magnitude change in diffusion coefficient upon binding, and cylindrical and linear diffusion modes along cellular protrusions. Finally, we demonstrate how this new method can move single-particle tracking from simple monolayer culture towards more tissue-like conditions by tracking single virions in tightly packed epithelial cells. This multi-resolution method presents new opportunities for capturing fast, 3D processes in biological systems.
提供机构:
Duke Research Data Repository
创建时间:
2022-11-03
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