Mechanistic studies of a peptidic GRP78 ligand for cancer cell-specific drug delivery

Authors
Liu, YingSteiniger, Sebastian C. J.Kim, YoungSooKaufmann, Gunnar F.Felding-Habermann, BrunhildeJanda, Kim D.
Issue Date
2007-05
Publisher
AMER CHEMICAL SOC
Citation
MOLECULAR PHARMACEUTICS, v.4, no.3, pp.435 - 447
Abstract
Major obstacles in the development of new therapeutic anticancer drugs are the low bioavailability of hydrophilic substances and the nonspecific toxicity toward healthy tissues. As such, cell-targeting oligopeptides have emerged as attractive drug delivery vehicles for a variety of different types of cargo. The recently identified peptide Pep42 binds to the glucose-regulated protein 78 (GRP78), which is overexpressed on the cell surface of human cancer cells and internalizes into these cells. Herein, we demonstrate how Pep42 can be utilized as a carrier for different types of cytotoxic drugs to specifically target human cancer cell lines in vitro in a strictly GRP78-dependent manner. Furthermore, the mechanism of internalization of Pep42 was elucidated and found to involve clathrin-mediated endocytosis. Pep42 subsequently colocalizes within the lysosomal compartment. Importantly, we also provide evidence that Pep42-conjugated quantum dots have the ability to selectively enrich in tumor tissue in a xenograft mouse model. Our results suggest that the highly specific GRP78-Pep42 interaction can be utilized for the generation of Pep42-drug conjugates as a powerful anticancer drug delivery system that could substantially enhance the efficacy of chemotherapy by increasing the drug-tumor specificity, thus minimizing the adverse side effects associated with conventional cancer therapeutics.
Keywords
PENETRATING PEPTIDES; ENDOPLASMIC-RETICULUM; CHAPERONE GRP78; LUNG-CANCER; PROTEINS; BINDING; EXPRESSION; SELECTION; INTERNALIZATION; ACTIVATION; PENETRATING PEPTIDES; ENDOPLASMIC-RETICULUM; CHAPERONE GRP78; LUNG-CANCER; PROTEINS; BINDING; EXPRESSION; SELECTION; INTERNALIZATION; ACTIVATION; drug delivery; tumor targeting; GRP78; heat shock protein; cyclic peptide
ISSN
1543-8384
URI
https://pubs.kist.re.kr/handle/201004/134437
DOI
10.1021/mp060122j
Appears in Collections:
KIST Article > 2007
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