4.8 Article

3-Dimensional Tracking of Non-blinking 'Giant' Quantum Dots in Live Cells

期刊

ADVANCED FUNCTIONAL MATERIALS
卷 24, 期 30, 页码 4796-4803

出版社

WILEY-V C H VERLAG GMBH
DOI: 10.1002/adfm.201400349

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资金

  1. National Institutes of Health [5R01AI097154-02]
  2. NIH-NIGMS Grant [1R01GM084702-01]
  3. Los Alamos National Laboratory Directed Research and Development Program
  4. National Nuclear Security Administration of the US Department of Energy [DE-AC52-06NA25396]
  5. New Mexico Spatiotemporal Modeling Center [P50GM0852673]
  6. NIH [R01GM100114]
  7. [P50 GM065794]
  8. [R01AI051575]

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While semiconductor quantum dots (QDs) have been used successfully in numerous single particle tracking (SPT) studies due to their high photoluminescence efficiency, photostability, and broad palette of emission colors, conventional QDs exhibit fluorescence intermittency or 'blinking,' which causes ambiguity in particle trajectory analysis and limits tracking duration. Here, non-blinking 'giant' quantum dots (gQDs) are exploited to study IgE-Fc epsilon RI receptor dynamics in live cells using a confocal-based 3D SPT microscope. There is a 7-fold increase in the probability of observing IgE-Fc epsilon RI for longer than 1 min using the gQDs compared to commercially available QDs. A time-gated photon-pair correlation analysis is implemented to verify that selected SPT trajectories are definitively from individual gQDs and not aggregates. The increase in tracking duration for the gQDs allows the observation of multiple changes in diffusion rates of individual IgE-Fc epsilon RI receptors occurring on long (>1 min) time scales, which are quantified using a time-dependent diffusion coefficient and hidden Markov modeling. Non-blinking gQDs should become an important tool in future live cell 2D and 3D SPT studies, especially in cases where changes in cellular dynamics are occurring on the time scale of several minutes.

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