The functionalization
of nanoparticles with functional moieties
is a key strategy to achieve cell targeting in nanomedicine. The interplay
between size and ligand number is crucial for the formulation performance
and needs to be properly characterized to understand nanoparticle
structure–activity relations. However, there is a lack of methods
able to measure both size and ligand number at the same time and at
the single particle level. Here, we address this issue by introducing
a correlative light and electron microscopy (CLEM) method combining
super-resolution microscopy (SRM) and transmission electron microscopy
(TEM) imaging. We apply our super-resCLEM method to characterize the
relationship between size and ligand number and density in PLGA–PEG
nanoparticles. We highlight how heterogeneity found in size can impact
ligand distribution and how a significant part of the nanoparticle
population goes completely undetected in the single-technique analysis.
Super-resCLEM holds great promise for the multiparametric analysis
of other parameters and nanomaterials.
The successful cytosolic delivery of nanoparticles is hampered by their endosomal entrapment and degradation. In order to push forward the smart development of nanoparticles we must reliably detect and quantify...
The characterization of newly synthesized materials is a cornerstone of all chemistry and nanotechnology laboratories. For this purpose, a wide array of analytical techniques have been standardized and are used...
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