AI Article Synopsis

  • The development of functional nanostructures for bioimaging faces challenges such as achieving low-dose contrast, stability in biological conditions, non-toxicity, and efficient cell uptake.
  • Researchers created magnetofluorescent architectures by coating superparamagnetic iron oxide nanoparticles with fluorescent organic nanoparticles, modifying the outer layer using different polyelectrolytes to optimize imaging capabilities.
  • Results showed that certain polyelectrolyte coatings enhanced MRI contrast and facilitated safe internalization in cancer cells, demonstrating effective imaging without causing cell death over a 72-hour period.

Article Abstract

Controlling the interactions of functional nanostructures with water and biological media represents high challenges in the field of bioimaging applications. Large contrast at low doses, high colloidal stability in physiological conditions, the absence of cell cytotoxicity, and efficient cell internalization represent strong additional needs. To achieve such requirements, we report on high-payload magnetofluorescent architectures made of a shell of superparamagnetic iron oxide nanoparticles tightly anchored around fluorescent organic nanoparticles. Their external coating is simply modulated using anionic polyelectrolytes in a final step to provide efficient magnetic resonance imaging (MRI) and fluorescence imaging of live cells. Various structures of PEGylated polyelectrolytes have been synthesized and investigated, differing from their iron oxide complexing units (carboxylic vs phosphonic acid), their structure (block- or comblike), their hydrophobicity, and their fabrication process [conventional or reversible addition-fragmentation chain transfer (RAFT)-controlled radical polymerization] while keeping the central magnetofluorescent platforms the same. Combined photophysical, magnetic, NMRD, and structural investigations proved the superiority of RAFT polymer coatings containing carboxylate units and a hydrophobic tail to impart the magnetic nanoassemblies (NAs) with enhanced-MRI negative contrast, characterized by a high r/r ratio and a transverse relaxation r equal to 21 and 125 s mmol L, respectively, at 60 MHz clinical frequency (∼1.5 T). Thanks to their dual modality, cell internalization of the NAs in mesothelioma cancer cells could be evidenced by both confocal fluorescence microscopy and magnetophoresis. A 72 h follow-up showed efficient uptake after 24 h with no notable cell mortality. These studies again pointed out the distinct behavior of RAFT polyelectrolyte-coated bimodal NAs that internalize at a slower rate with no adverse cytotoxicity. Extension to multicellular tumor cell spheroids that mimic solid tumors revealed the successful internalization of the NAs in the periphery cells, which provides efficient deep-imaging labels thanks to their induced T* contrast, large emission Stokes shift, and bright dotlike signal, popping out of the strong spheroid autofluorescence.

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Source
http://dx.doi.org/10.1021/acsami.7b01737DOI Listing

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