Issue 21, 2013

Modulation of hydrogel nanoparticle intracellular trafficking by multivalent surface engineering with tumor targeting peptide

Abstract

Surface engineering of a hydrogel nanoparticle (NP) with the tumor-targeting ligand, F3 peptide, enhances both the NP's binding affinity for, and internalization by, nucleolin overexpressing tumor cells. Remarkably, the F3-functionalized NPs consistently exhibited significantly lower trafficking to the degradative lysosomes than the non-functionalized NPs, in the tumor cells, after internalization. This is attributed to the non-functionalized NPs, but not the F3-functionalized NPs, being co-internalized with Lysosome-associated Membrane Protein-1 (LAMP1) from the surface of the tumor cells. Furthermore, it is shown that the intracellular trafficking of the F3-functionalized NPs differs significantly from that of the molecular F3 peptides (untethered to NPs). This has important implications for designing effective, chemically-responsive, controlled-release and multifunctional nanodrugs for multi-drug-resistant cancers.

Graphical abstract: Modulation of hydrogel nanoparticle intracellular trafficking by multivalent surface engineering with tumor targeting peptide

Supplementary files

Article information

Article type
Paper
Submitted
20 Feb 2013
Accepted
18 Aug 2013
First published
22 Aug 2013

Nanoscale, 2013,5, 10327-10344

Modulation of hydrogel nanoparticle intracellular trafficking by multivalent surface engineering with tumor targeting peptide

L. Karamchand, G. Kim, S. Wang, H. J. Hah, A. Ray, R. Jiddou, Y. Koo Lee, M. A. Philbert and R. Kopelman, Nanoscale, 2013, 5, 10327 DOI: 10.1039/C3NR00908D

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