AI Article Synopsis

  • Researchers recorded fluorescence spectra of the anti-cancer drug emodin loaded onto nanostructured porous silicon, finding an enhancement in fluorescence due to the use of colloidal silver nanoparticles.
  • The mean pore size of the silicon was 60 nm, and the silver nanoparticles were 50 nm in diameter, with conditions that allowed for effective drug infiltration and loading.
  • The best results, including a fluorescence enhancement factor of 24 and better drug penetration, occurred using methanol as a solvent, indicating potential for future medical applications in drug delivery systems.

Article Abstract

Fluorescence spectra of anti-tumoral drug emodin loaded on nanostructured porous silicon have been recorded. The use of colloidal nanoparticles allowed embedding of the drug without previous porous silicon functionalization and leads to the observation of an enhancement of fluorescence of the drug. Mean pore size of porous silicon matrices was 60 nm, while silver nanoparticles mean diameter was 50 nm. Atmospheric and vacuum conditions at room temperature were used to infiltrate emodin-silver nanoparticles complexes into porous silicon matrices. The drug was loaded after adsorption on metal surface, alone, and bound to bovine serum albumin. Methanol and water were used as solvents. Spectra with 1 μm spatial resolution of cross-section of porous silicon layers were recorded to observe the penetration of the drug. A maximum fluorescence enhancement factor of 24 was obtained when protein was loaded bound to albumin, and atmospheric conditions of inclusion were used. A better penetration was obtained using methanol as solvent when comparing with water. Complexes of emodin remain loaded for 30 days after preparation without an apparent degradation of the drug, although a decrease in the enhancement factor is observed. The study reported here constitutes the basis for designing a new drug delivery system with future applications in medicine and pharmacy.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3447710PMC
http://dx.doi.org/10.1186/1556-276X-7-364DOI Listing

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