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Published April 19, 2011 | Published + Supplemental Material
Journal Article Open

Targeting kidney mesangium by nanoparticles of defined size

Abstract

Nanoparticles are being investigated for numerous medical applications and are showing potential as an emerging class of carriers for drug delivery. Investigations on how the physicochemical properties (e.g., size, surface charge, shape, and density of targeting ligands) of nanoparticles enable their ability to overcome biological barriers and reach designated cellular destinations in sufficient amounts to elicit biological efficacy are of interest. Despite proven success in nanoparticle accumulation at cellular locations and occurrence of downstream therapeutic effects (e.g., target gene inhibition) in a selected few organs such as tumor and liver, reports on effective delivery of engineered nanoparticles to other organs still remain scarce. Here, we show that nanoparticles of ~75 ± 25-nm diameters target the mesangium of the kidney. These data show the effects of particle diameter on targeting the mesangium of the kidney. Because many diseases originate from this area of the kidney, our findings establish design criteria for constructing nanoparticle-based therapeutics for targeting diseases that involve the mesangium of the kidney.

Additional Information

© 2011 National Academy of Sciences. Freely available online through the PNAS open access option. Contributed by Mark E. Davis, March 7, 2011 (sent for review February 8, 2011). We thank Debbie Guerrero and Siva Wu from the House Ear Institute for advice in histology. This work was supported by National Cancer Institute Grant CA119347 and National Institutes of Health Grant NIH 2P30DC006272-06 and the Ahmanson Foundation.

Attached Files

Published - Choi2011p13718P_Natl_Acad_Sci_Usa.pdf

Supplemental Material - pnas.201103573SI.pdf

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