Single Nanoparticle Imaging and Characterization of Different Phospholipid-Encapsulated Quantum Dot Micelles

Phospholipid quantum dot (QD) micelles have been extensively used as fluorescent tags in single nanoparticle imaging for biomedical imaging. In this work, the microscopic structures and photophysical properties of the phospholipid QD micelles were studied at the single nanoparticle level. Two common...

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Bibliographic Details
Published inLangmuir Vol. 28; no. 28; pp. 10602 - 10609
Main Authors Liu, Jianbo, Yang, Xiaohai, Wang, Kemin, He, Yan, Zhang, Pengfei, Ji, Haining, Jian, Lixin, Liu, Wei
Format Journal Article
LanguageEnglish
Published Washington, DC American Chemical Society 17.07.2012
Subjects
Chemistry
Colloidal state and disperse state
Exact sciences and technology
Fluorescence
Fluorescent Dyes - chemistry
General and physical chemistry
Micelles
Micelles. Thin films
Models, Molecular
Nanoparticles - chemistry
Particle Size
Phospholipids - chemistry
Physical and chemical studies. Granulometry. Electrokinetic phenomena
Quantum Dots
Quantum dot
Nanoparticle
Fluorescence
Micelle
Phospholipid
Liquid phase
Characterization
Ethylene oxide polymer
Total internal reflection
Amine
Imaging
Distribution
Solid phase
Trajectory
Diffusion coefficient
Diffusion
Structure
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Summary:Phospholipid quantum dot (QD) micelles have been extensively used as fluorescent tags in single nanoparticle imaging for biomedical imaging. In this work, the microscopic structures and photophysical properties of the phospholipid QD micelles were studied at the single nanoparticle level. Two commonly used types of phospholipid QD micelles were prepared and tested both on a solid-phase surface and in liquid phase, including 1,2-distearoyl-sn-glycero-3-phosphoethanolamine-encapsulated QD micelles (DSPE–QDMs) and 1,2-distearoyl-sn-glycero-3-phosphoethanolamine-N-[methoxy(polyethylene glycol)-2000]-encapsulated QD micelles (PEG–DSPE–QDMs). Their fluorescence intensities and diffusion trajectories were determined by a total internal reflection fluorescence-based single nanoparticle imaging platform and comparatively analyzed carefully. It was demonstrated that DSPE–QDMs possessed a comparably wider intensity distribution and lower diffusion coefficient than that of PEG–DSPE–QDMs. PEG–DSPE–QDMs exhibited an obvious fluorescent intermittence. The results suggested that for most of the DSPE–QDMs, more than one QD were encapsulated in a single micelle. On the other hand, only one QD was embedded in a single micelle of PEG–DSPE–QDMs for most of the cases. Such variances suggested that phospholipids play a key role in the fabrication of the QD micelles. This work provides a useful foundation for their further biomedical applications.
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ISSN:0743-7463
1520-5827
DOI:10.1021/la301873m